A book of ideas collected from Medical Hypotheses: Death can be cured by Roger Dobson
Bruce G. Charlton
Medical Hypotheses. 2008; 70: 905-9.
Summary
A new collection of ideas from Medical Hypotheses by Roger Dobson is entitled Death can be cured and 99 other Medical Hypotheses. It consists of humorous summaries of Medical Hypotheses articles from the past 30 years. The book’s humour derives mainly from the subject matter, although sometimes also from the ‘unconventional’ approach of the authors with respect to matters such as evidence, argument or inference. Medical Hypotheses has generated such a lot of apparently- or actually-bizarre ideas because it aims to be open to potentially revolutionary science. The journal’s official stance is that more harm is done by a failure to publish one idea that might have been true, than by publishing a dozen ideas that turn out to be false. Bizarre ideas tend to catch attention, and may stimulate a valuable response – even when a paper is mostly-wrong. A paper may be flawed but still contain the germ of an idea that can be elaborated and developed. The journal review process is susceptible to both false positives and false negatives. False positives occur when we publish an idea that is wrong; false negatives occur when we fail to publish an important idea that is right, and a potential scientific breakthrough never happens. False positives are more obvious, since the paper will be ignored, refuted, or fail to be replicated – and often attracts criticism and controversy. Editors may therefore take the more cautious path of avoiding false positives more assiduously than false negatives; however, this policy progressively favours less-ambitious science. Consequently, in Medical Hypotheses the ‘set point’ of risk is nearer to the false positive end of the spectrum than for most journals – and the publication of many apparently-bizarre papers is a natural consequence of this policy.
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A new book of ideas from Medical Hypotheses
Roger Dobson’s collection of ideas from Medical Hypotheses is entitled Death can be cured and 99 other Medical Hypotheses [1], [2], [3], [4], [5], [6], [7], [8], [9], [10], [11], [12], [13], [14], [15], [16], [17], [18], [19], [20], [21], [22], [23], [24], [25], [26], [27], [28], [29], [30], [31], [32], [33], [34], [35], [36], [37], [38], [39], [40], [41], [42], [43], [44], [45], [46], [47], [48], [49], [50], [51], [52], [53], [54], [55], [56], [57], [58], [59], [60], [61], [62], [63], [64], [65], [66], [67], [68], [69], [70], [71], [72], [73], [74], [75], [76], [77], [78], [79], [80], [81], [82], [83], [84], [85], [86], [87], [88], [89], [90], [91], [92], [93], [94], [95], [96], [97], [98], [99] and [100].
This delightful volume consists of gently-humorous summaries of Medical Hypotheses articles published since the journal’s foundation by the late David Horrobin in 1975.
The book’s humour derives mainly from the subject matter, although sometimes also from the ‘unconventional’ approach of the authors with respect to matters such as evidence, argument or inference. The apparently-bizarre nature of the science is of many types. In most instances the subject matter and conclusions are quite mainstream and serious from a scientific perspective, but from the perspective of an outsider they may seem strange. In other instances the ideas really are bizarre, from almost any perspective. And there are theories from all points in-between.
Bizarre ideas tend to catch attention, and may stimulate a valuable response – even when a paper is mostly-wrong. When reading what I think is a mostly-wrong idea submitted to Medical Hypotheses, I sometimes find myself provoked into formulating exactly where and why the idea is wrong – which can be a valuable experience. A paper may be flawed but still contain the germ of an idea that can be elaborated and developed – the reader feels they can do a better job than the author, and might embark on a new line of investigation.
Bizarre or flawed papers that provoke the reader may therefore stimulate correspondence to the author or journal in response, may turn-up later as a citation, or may have an important but invisible effect on another scientist’s attitudes, teaching or direction of research. This is all a contribution to the dynamic process of science – and science should always be regarded as a dynamic process, not a fixed body of facts and laws.
False positives and negatives in reviewing
The reason that Medical Hypotheses has generated such a lot of apparently- or actually-bizarre ideas is that it aims to be open to potentially revolutionary science. The journal’s official stance is that more harm is done by a failure to publish one idea that might have been true, than by publishing a dozen ideas that turn out to be false.
It may easily be forgotten that the review processes of science are susceptible both false positives and false negatives. False positives occur when we publish an idea that is wrong; false negatives occur when the journal fails to publish an idea that is right. False positives are more obvious, since the paper will be ignored, refuted, or fail to be replicated. This attracts criticism because it may waste the time and resources of other scientists.
But false negatives – when we fail to publish an idea which would (in an imaginary alternative universe) have led to some kind of breakthrough – are a more devastating mistake. But the false negative problem is seldom acknowledged, because the consequences may be invisible. Failure to publish might lead to an idea being lost altogether, or being published somewhere less appropriate (increasing the possibility that it would be unnoticed or ignored).
The fact that false positives attract more rapid and certain criticism and controversy than false negatives exerts a constant drip–drip of pressure on editors to take the more cautious and less controversy-generating path of avoiding false positives more assiduously than false negatives. This is prudent, but constitutes a sinister trade-off in the long term because it progressively favours less ambitious and more conservative science.
Consequently, in Medical Hypotheses the ‘set point’ of risk is nearer to the false positive end of the spectrum than it is for most journals. This is why the journal deploys editorial review (where journal contents are chose mainly by the editor) rather than the commoner but more cautious and negative peer review system.
On top of this, the Medical Hypotheses editorial policy constitutes an implicit contention concerning the style in which science should be conducted. Our idea is that it is sometimes (but not always) better to be interestingly wrong than boringly right; sometimes better to err on the side of tolerance rather than exclusion, sometimes better to stimulate than to reinforce closure.
It takes many personality types to make the world of science, and the same applies to journals. Science would not work efficiently if all journals were like Medical Hypotheses: there would be too much ‘noise’ in the system. But science does not work properly when journals will only publish papers that are regarded as completely correct by a panel of peers – because such papers cannot be bold and speculative, and because gems of insight may come from bizarre or flawed research.
Currently, the pendulum has probably swung too far in the direction of excess caution in mainstream medical science; such that the imperative to exclude noise has slipped-over into a too-rigid exclusion of diversity and dissent. The majority of journals publish only ultra-cautious papers that report dependable but cringingly-modest, incremental extrapolations of solidly-established knowledge.
One consequence is that although medical science has expanded hugely in funding and production over recent decades, there has probably been a declining frequency of major breakthroughs which seems to have slowed the rate of medical progress.
The future of bizarre ideas
These are some of the reasons why Medical Hypotheses publishes (apparently) bizarre papers, and how it was possible for Roger Dobson to collect 100 such ideas into an entertaining volume.
However, in the internet era of open-access to international publication, the role of Medical Hypotheses has inevitably become more specialised: it is now more like a place where bold scientific speculation meets the mainstream.
Since Medical Hypotheses has recently entered the realms of respectability with its 2006 impact factor of 1.29, monthly internet downloads running at about 32,000, and the rejection rate currently hovering around 80% or 90% – my challenge as editor will be to build on this success while maintaining the traditional open-ness and genial eccentricity of the journal which have characterized its first three decades.
This goal of avoiding false negatives more assiduously than false positives will almost-inevitably mean that Medical Hypotheses shall need to continue rejecting some probably-correct papers that are worthy-but-somewhat-dull, in favour of publishing some bizarre or flawed papers that just might (but – it must be admitted – probably will not) stimulate a break-though of some sort.
By holding to this principle, I hope to ensure that in another thirty years, a future science writer can produce an equally entertaining and edifying volume as Roger Dobson’s Death can be cured.
References
What follows are the 100 papers from Medical Hypotheses featured in Death can be cured and 99 other Medical Hypotheses, by Roger Dobson – Cyan Books, 32–38 Saffron Hill, London, EC1N 8FH, UK, 2007. ISBN 978-1-905736-31-7. Chapter titles are appended in italics.
[1] Mak MWM, Kwan TS, Cheng KH, Chan RTF, Ho SL. Myopia as a latent phenotype of a pleiotropic gene positively selected for facilitating neurocognitive development, and the effects of environmental factors in its expression. 2006;66:1209–15 [Short-sighted people are more intelligent].
[2] Arzy S, Idel M, Landis T, Blanke O. Why revelations have occurred on mountains. Linking mystical experiences and cognitive neuroscience. 2005;65:841–5 [Revelations always happen on mountains].
[3] Oinonen KA, Mazmanian D. Does body fat protect against negative moods in women? 2001;57:387–8 [Fat people really are more jolly].
[4] Melles RB, Katz B. Night terrors and sudden unexplained nocturnal death. 1988;26:149–54 [Nightmares can kill you].
[5] Stevenson I. The phenomenon of claimed memories of previous lives: possible interpretations and importance. 2000;54:652–9 [Birthmarks are proof of reincarnation].
[6] Fisch H, Andrews HF, Fisch KS, Golden R, Liberson G, Olsson CA. The relationship of long-term global temperature change and human fertility. 2003;61:21–8 [Global warming reduces fertility].
[7] Elsner RJF, Spangler JG. Neurotoxicity of inhaled manganese: public health danger in the shower? 2005;65:607–16 [Showers are bad for the brain].
[8] Samaras TT, Storms LH. Secular growth and its harmful ramifi cations. 2002;58:93–112 [Small people can save the world].
[9] Sri Kantha S. Total immediate ancestral longevity (TIAL) score as a longevity indicator: an analysis on Einstein and three of his scientist peers. 2001;56:519–22 [The date you will die can be calculated].
[10] Katz G, Durst R, Zislin Y, Barel Y, Knobler HY. Psychiatric aspects of jet lag: review and hypothesis. 2001;56:20–3 [Jet lag triggers mental illness].
[11] Harris JR. Parental selection: a third selection process in the evolution of human hairlessness and skin colour. 2006;66:1053–9 [Why humans are not furry].
[12] Verhaegen MJB. The aquatic ape theory and some common diseases. 1987;24:293–9 [The purpose of ear wax].
[13] Bobrow RS. Paranormal phenomena in the medical literature sufficient smoke to warrant a search for fire. 2003;60:864–8 [Hearing voices could save your life].
[14] Ichim I, Kieser J, Swain M. Tongue contractions during speech may have led to the development of the bony geometry of the chin following the evolution of human language? A mechanobiological hypothesis for the development of the human chin. 2007;69:20–24 [The reason for chins].
[15] Howe NE. The origin of humour. 2002;59:252–4 [Humour increases survival].
[16] Fessler DMT, Abrams ET. Infant mouthing behaviour: the immunocalibration hypothesis. 2004;63:925–32 [Babies suck to avoid asthma].
[17] Vardi P, Pinhas-Hamiel O. The young hunter hypothesis: age-related weight gain – a tribute to the thrifty theories. 2000;55:521–3 [Beer bellies protect men in old age].
[18] Kolettis TM, Kolettis MT. Winter swimming: healthy or hazardous? Evidence and hypotheses. 2003;61:654–6 [Why winter swimmers don’t shiver].
[19] Manning JT, Bundred PE. The ratio of 2nd to 4th digit length: a new predictor of disease predisposition? 2000;54:855–7 [Finger lengths predict disease].
[20] Mobley JL. Is rheumatoid arthritis a consequence of natural selection for enhanced tuberculosis resistance? 2004;62:839–43 [Arthritis is the price of having healthy ancestors].
[21] Rubio-Godoy M, Aunger R, Curtis V. Serotonin – a link between disgust and immunity? 2007;68:61–6 [Feeling disgusted is healthy].
[22] Miric D, Hallet-Mathieu A-M, Amar G. Aetiology of antisocial personality disorder: benefits for society from an evolutionary standpoint. 2005;65:665–70 [Psychopaths are a necessary evil].
[23] Cassano WF. Cystic fibrosis and the plague. 1985;18:51–2 [Cystic fibrosis is a legacy of the Black Death].
[24] Sontag SJ, Wanner JN. The cause of leg cramps and knee pains: a hypothesis and effective treatment. 1988;25:35–41 [Modern toilets ruin legs].
[25] Bakan R. Queen Elizabeth I: a case of testicular feminization? 1985;17:277–84 [Queen Elizabeth I was part man].
[26] Bark N. Did schizophrenia change the course of English history? The mental illness of Henry VI 2002;59:416–21 [Schizophrenia changed the course of English history].
[27] Clarkson JDB. A possible origin for the Turin shroud image. 1983;12:11–16 [Jesus, the Turin Shroud and spontaneous combustion].
[28] Størmer FC, Mysterud I. Cave smoke: air pollution poisoning involved in Neanderthal extinction? 2007;68:723–4 [Smoke made Neanderthals extinct].
[29] McSweegan E. Anthrax and the aetiology of the English Sweating Sickness. 2004;62:155–7 [English Sweating Disease was really anthrax].
[30] Walsh GP. The history of the herring and with its decline the significance to health. 1986;20:133–7 [Herrings saved us from heart disease].
[31] Hollander DH. Beef allergy and the Persian Gulf syndrome. Med Hypothesis 1995;45:221–2 [Gulf War Syndrome is an allergy to burgers].
[32] Platek SM, Gallup GG, Fryer BD. The fi reside hypothesis: Was there differential selection to tolerate air pollution during human evolution? 2002;58:1–5 [Prehistoric fires protected man from lung cancer].
[33] Sri Kantha S. Could nitroglycerine poisoning be the cause of Alfred Nobel’s anginal pains and premature death? 1997;49:303–6 [Alfred Nobel was killed by dynamite].
[34] Passie T, Hartmann U, Schneider U, Emrich HM. On the function of groaning and hyperventilation during sexual intercourse: intensification of sexual experience by altering brain metabolism through hippomania. 2003;60:660–3 [Why women groan during sex].
[35] Gofrit ON. The evolutionary role of erectile dysfunction. 2006;67:1245–9 [The importance of being impotent].
[36] Marx GF, Naushaba SH, Schulman H. Is pre-eclampsia a disease of the sexually active gravida? 1981;7:1397–9 [Sex causes high blood pressure in pregnancy].
[37] Sheth R, Panse GT. Can vasectomy reduce the incidence of prostatic tumour? 1982;8:237–41 [Vasectomy lowers the risk of prostate cancer].
[38] Shoja MM, Tubbs RS, Ansarin K. A cure for infatuation? The potential ‘therapeutic’ role of pineal gland products such as melatonin and vasotocin in attenuating romantic love. 2007;68:1172–3 [A cure for infatuation].
[39] Eagles JM. Seasonal affective disorder: a vestigial evolutionary advantage? 2004;63:767–72 [Winter depression stops sex].
[40] Ramachandran VS. Why do gentlemen prefer blondes? 1997;48:19–20 [Gentlemen prefer blondes].
[41] Burger J, Gochfeld M. A hypothesis on the role of pheromones on age of menarche. 1985;17:39–46 [House smells turn teenage girls into women].
[42] Ney PG. The intravaginal absorption of male generated hormones and their possible effect on female behaviour. 1986;20:221–31 [Baby blues are caused by lack of sex].
[43] Xiong X, Buekens P, Vastardis S, Wu T. Periodontal disease as one possible explanation for the Mexican paradox. 2006;67:1348–54 [Gum disease causes small babies].
[44] Gjorgov N. Barrier contraceptive practice and male infertility as related factors to breast cancer in married women. 1978;4:79–88 [Condoms increase the risk of breast cancer].
[45] Schreiber G, Avissar S, Tzahor Z, Barak-glantz I, Grisaru N. Photoperiodicity and annual rhythms of wars and violent crimes. 1997;48:89–96 [Sunny days make men violent].
[46] Richardson-Andrews RC. Sunspots and the recency theory of schizophrenia. 1995;44:16–19 [The sun causes schizophrenia].
[47] Davis GE, Lowell WE. Solar cycles and their relationship to human disease and adaptability. 2006;67:447–61 [The sun fixes lifespan].
[48] Yeung JWK. A hypothesis: sunspot cycles may detect pandemic influenza A in 1700–2000 ad. 2006;67:1016–22 [Flu epidemics are affected by the sun].
[49] Mikulecky M, Rovensky J. Gout attacks and lunar cycle. 2000;55:24–5 [Gout attacks are caused by the moon].
[50] Sok M, Mikulecky M, Erzen J. Onset of spontaneous pneumothorax and the synodic lunar cycle. 2001;57:638–41 [Chest pains are caused by the moon].
[51] Sher L. Effects of the weather conditions on mood and behaviour: the role of acupuncture points. 1996;46:19–20 [How weather affects mood].
[52] Erren TC, Piekarski C. Does winter darkness in the Arctic protect against cancer? The melatonin hypothesis revisited. 1999;53:1–5 [Why Greenlanders have less cancer].
[53] Pauley SM. Lighting for the human circadian clock: recent research indicates that lighting has become a public health issue. 2004;63:588–96 [Lights at night cause cancer].
[54] Laumbacher B, Fellerhoff B, Herzberger B, Wank R. Do dogs harbour risk factors for human breast cancer? 2006;67:21–6 [Dogs give women breast cancer].
[55] Milham S, Ossiander E. Electric typewriter exposure and increased female breast cancer mortality in typists. 2007;68:450–1 [Electric typewriters cause breast cancer].
[56] Komarova SV. A moat around castle walls: the role of axillary and facial hair in lymph node protection from mutagenic factors. 2006;67:698–701 [Hairy people have less cancer].
[57] Kumar A, Mallya K, Kumar J. Are lung cancers triggered by stopping smoking? 2007;68:1176–7 [Quitting smoking too fast triggers lung cancer].
[58] Steindal Hykkerud, Porojnicu AC, Moan J. Is the seasonal variation in cancer prognosis caused by sun-induced folate degradation? 2007;69:182–5 [Cancer is best diagnosed in the summer].
[59] Donovan M, Tiwary CM, Axelrod D, Sasco AJ, Jones L, Hajek R, et al. Personal care products that contain estrogens or xenoestrogens may increase breast cancer risk. 2007;68:756–66 [Hairsprays cause cancer].
[60] Manning JT, Caswell N. Constitutive skin pigmentation: a marker of breast cancer risk? 2004;63:787–9 [Skin colour and breast cancer].
[61] Hoseini SS, Gharibzadeh S. Squeezing the glans penis: a possible manoeuvre for improving the defecation process and preventing constipation. 2007;68:925–6 [A cure for constipation].
[62] Weber C. Eliminate infection (abscess) in teeth with cashew nuts. 2005;65:1200 [Nuts cure toothache].
[63] Robinson A. Electrolysis between the feet and the ground and its probable health effects. 1979;5:1071–7 [Leather shoes cure diseases].
[64] Kumar A. Gag reflex for arrest of hiccups. 2005;65:1206 [A cure for hiccups].
[65] Eby GA. Strong humming for one hour daily to terminate chronic rhinosinusitis in four days: a case report and hypothesis for action by stimulation of endogenous nasal nitric oxide production. 2006;66:851–4 [Humming 120 times a day cures blocked noses].
[66] Kolettis J, Kumar A. Sustained repulsive magnetic force for bone lengthening. 2005;65:630 [Magnets can make you taller].
[67] Mathur RK. The role of hypersomolal food in the development of atherosclerosis. 2005;64:579–81 [Drinking water lowers the risk of heart disease].
[68] Dehmelt H. Healthiest diet hypothesis: How to cure most diseases? 2005;64:882 [A cure for most diseases].
[69] Olson CB. A possible cure for death. 1988;26:77–84 [A cure for death].
[70] Patronek GJ, Glickman LT. Pet ownership protects against the risks and consequences of coronary heart disease. 1993;40:245–9 [Pets prevent heart attacks].
[71] Sabayan B, Zolghadrasli A, Mahmoudian N. Could taking an up-elevator on the way to the delivery room be a potential novel therapy for dystocia? 2007;68:227 [Taking the elevator for a natural birth].
[72] Teas J, Hebert JR, Helen Fitton J, Zimba PV. Algae – a poor man’s HAART? 2004;62:507–10 [Seaweed may prevent AIDS].
[73] Magen E, Borkow G, Bentwich Z, Mishal J, Scharf S. Can worms defend our hearts? Chronic helminthic infections may attenuate the development of cardiovascular diseases. 2005;64:904–9 [Worms prevent heart disease].
[74] Smith W, Skilling DE, Castello JD, Rogers SO. Ice as a reservoir for pathogenic human viruses: specifically, caliciviruses, influenza viruses, and enteroviruses. 2004;63:560–6 [Killer viruses are hiding in the ice].
[75] Robinson A. Heart disease, cancer and vehicle travel. 1979;5:323–8 [Car travel causes heart disease].
[76] Seely S. The recession of gastric cancer and its possible causes. 1978;4:50–7 [How soft drinks prevent stomach cancer].
[77] Fischer KM. Hypothesis: tobacco use is a risk factor in rheumatoid arthritis. 1991;34:116–7 [Smoking caused rheumatoid arthritis].
[78] van Woerden H. Dust mites living in human lungs – the cause of asthma? 2004;63:193–7 [Tiny bugs living in the lungs cause asthma].
[79] Blondell JM. Pesticides and breast cancer, popcorn and colorectal cancer: innovation versus fashion in dietary epidemiology. 1983;12:191–4 [Killer popcorn].
[80] Lim ECH. RCS Seet, Botulinum toxin injections to reduce adiposity: possibility, or fat chance? 2006;67:1086–9 [Botox makes you thinner].
[81] Ahmad Aziz N, Ibrahim Aziz M. Losing weight by defecating at night. 2006;67:989 [Defecate at night to lose weight].
[82] Johnson JB, Laub DR, John S. The effect on health of alternate day calorie restriction: eating less and more than needed on alternate days prolongs life. 2006;67:209–11 [Diet every other day to lose weight and live longer].
[83] Tekol Y. Salt addiction: a different kind of drug addiction. 2006;67:1233–4 [Salt, the cocaine of the kitchen?].
[84] Moishezon-Blank N. Commentary on the possible effect of hormones in food on human growth. 1992;38:273–7 [Why American heads are getting smaller (and the French bigger)].
[85] Nanji A, Narod S. Multiple sclerosis, latitude and dietary fat: Is pork the missing link? 1986;20:279–82 [Eating pork causes multiple sclerosis].
[86] Shaw CA, Bains JS. Did consumption of flour bleached by the agene process contribute to the incidence of neurological disease? 1998;51:477–81 [Mad flour disease].
[87] Ganmaa D, Li XM, Qin LQ, Wang PY, Takeda M, Sato A. The experience of Japan as a clue to the aetiology of testicular and prostatic cancers. 2003;60:724–30 [Milk causes cancer].
[88] Concepcion GP, Padlan EA. Are humans getting ‘mad-cow disease’ from eating beef, or something else? 2003;60:699–701 [Rats spread mad cow disease to humans].
[89] Surja Agus S, El-Mallakh RS. Fertility and childhood bipolar disorder. 2007;69:587–9 [How a prescription drug increased depression in children].
[90] Cook RD. Multiple sclerosis: Is the domestic cat involved? 1981;7:147–54 [MS and the domestic cat].
[91] Cane RH. The role of soap and nutrition in producing human diseases. 1983;11:251–4 [Soap causes heart disease].
[92] Previc FH. Prenatal influences on brain dopamine and their relevance to the rising incidence of autism. 2007;68:46–60 [Autism and city life].
[93] Henshaw DL. Does our electricity distribution system pose a serious risk to public health? 2002;59:39–51 [Power lines cause depression].
[94] Flensmark J. Is there an association between the use of heeled footwear and schizophrenia? 2004;63:740–7 [Heeled shoes cause schizophrenia].
[95] Sutton PRN. Can water fluoridation increase orthodontic problems? 1988;26:63–4 [Fluoride makes teeth crooked].
[96] Clauss R, Mayes J, Hilton P, Lawrenson R. The influence of weather and environment on pulmonary embolism: pollutants and fossil fuels. 2005;64:1198–1201 [Rain causes blood clots].
[97] Moalem S, Storey KB, Percy ME, Peros MC, Perl DP. The sweet thing about type 1 diabetes: a cryoprotective evolutionary adaptation. 2005;65:8–16 [Climate change caused diabetes].
[98] Aronson M. Does excessive television viewing contribute to the development of dementia? 1993;41:465–6 [TV shows cause dementia].
[99] Sutton PRN. Psychosomatic dental disease: Is mental stress in adults followed by acute dental caries in all racial groups? 1993;41:279–81 [Stress can seriously damage your teeth].
[100] Worth J. Neonatal sensitization to latex. 2000;54:29–33 [Gloves cause asthma].
Sunday, 23 March 2008
Wednesday, 5 March 2008
Mega-cash prizes for revolutionary science
Editorial
Stimulating revolutionary science with mega-cash prizes
Bruce G. Charlton (a) and Peter Andras (b)
Medical Hypotheses - Volume 70, Issue 4, 2008, Pages 709-713
(a) Editor-in-Chief – Medical Hypotheses, Newcastle University, NE1 7RU, UK and (b) Editorial Advisory Board – Medical Hypotheses, Newcastle University, NE1 7RU, UK
Available online 5 March 2008.
Summary
We argue that the most ambitious science is intrinsically riskier science, more likely to fail. It is almost always a safer career strategy for the best scientists to seek to extend knowledge more modestly and to build incrementally on existing ideas and methods. Therefore, higher rewards for success are a necessary incentive to encourage top scientists to work on the most important scientific problems, ones where the solution has potentially revolutionary implications. We suggest that mega-cash prizes (measured in tens of millions of dollars) are a suitable reward for those individuals (or institutions) whose work has triggered radically new directions in science.
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Rewards for successful revolutionary science
Revolutionary science may be distinguished from ‘normal’ science in that revolutionary science aims at generating qualitative advances on established science while normal science aims at incremental progress [1]. While there is a grey borderline, there is a clear distinction between research that aims at transformation of a scientific discipline and that which aims at extension of that discipline [2].
Naturally, since revolutionary science is more ambitious, it is more likely to fail. For every successful instance of revolutionary science there are likely to be manifold examples of failure [3]. By contrast, ‘normal’ incremental science is much more likely to succeed, especially when it is performed by able and well-trained scientists working in well-resourced institutions.
Given that revolutionary science is a high risk endeavour which usually fails; it is likely to thrive only when the incentives rewarding the rare instances of success are greater than for normal science. Therefore we would argue that it is insufficient for successful revolutionary scientists merely to get the usual rewards of prestigious professorships, respect from within the scientific profession, and a modestly high level of reasonably secure income. Something more is needed: lots of money.
The money incentive in science
To compensate for the intrinsically greater risk of failure, successful revolutionary science requires greater rewards than normal science; rewards such as higher prestige, better jobs and/or more money. We suggest that more money is the most promising incentive to encourage revolutionary science, because it is the factor which is most-controllable.
Historically, the main reward for scientific success was high prestige. It was possible for a successful genius to transform a whole science – as Darwin transformed biology and Newton transformed physics. After such success these scientists became public figures so there was an incentive of ‘immortality’ (e.g. Darwin and Newton have appeared on UK banknotes). But now that science is divided into numerous sub-specialties there is less prospect of general public esteem and the rewards of high status are confined to recognition within what may be a relatively small and specific scientific discipline.
Nor is revolutionary science likely to be rewarded with better jobs, except at the very top stratum of eminence such as Nobel laureates. The prospect of rewarding successful revolutionary scientists with better jobs than successful normal scientists is unlikely to happen. Economists usually suggest that the basis of the salary and conditions of a job are the (probable) marginal effects that an individual has on future productivity of an organization [4]. This implies that salaries are not given for past achievement, except when this enhances future prospects for the organization. For example, the top research universities in the USA seem to compete to have Nobel laureates on their faculty as a symbol of their scientific eminence. This signal is apparently effective even when the laureates are semi-retired and unproductive.
But this is due to the extreme rarity of Nobel laureates [5], and at lower levels of eminence there is little advantage for an institution to employ people who were, in the past, successful at revolutionary science – and to employ them at the enhanced rates of pay and privileged conditions of service which are necessary to compensate them for having chosen the high-risk path of revolutionary science.
A scientist of high ability who chooses revolutionary science as a career will probably and on average attain lower outputs, lower numbers of citations, lower-impact publications and less professional prestige than if they put the same efforts and abilities into normal science. (To put in another way, a scientist would probably gain a higher rate of science production by aiming directly at attaining high science production, than by aiming to solve a major problem.)
An able and committed scientist choosing a normal science path would therefore usually be able to out-perform himself as a revolutionary scientist, in terms of immediate and measurable performance measures. A longer term strategy will tend to generate results and produce rewards later. Even if everything goes perfectly and a successful revolutionary scientist ends-up with a Nobel prize, the chances are that this will come near or after the end of their professional career.
But the prospect of a major prize such as a Nobel is surely too unlikely, too remote and too uncertain to be a widespread or realistic motivation in the career paths of young scientists in their twenties or thirties. And it is at this age when scientists must decide whether or not to pursue revolutionary science [6].
Incentives for the best young scientists to pursue revolutionary science
The critical decision to embark on a high-risk strategy of revolutionary science would typically come not much later than a scientist’s late-twenties – just after they have finished their PhD or equivalent research training [6]. Of course, some young scientists will be so idealistic (or so unrealistic) that they ignore the potential rewards or costs of their career choices. Nonetheless, incentives usually make a difference to human behaviour, and if there were more powerful incentives, then presumably more scientists would opt to practice revolutionary science. So, what are the incentives which might affect a young and gifted scientist’s career selection?
Let us imagine an outstanding young scientist who has the potential to be first rate. He or she is faced by a choice between a high risk strategy of trying to make a revolutionary contribution to their branch of science, or else to ‘down-shift’ to a less ambitious but lower-risk path of doing a large volume of high-quality normal science. The best scientists are, in other words, in a position to choose between a small chance of success at the goal of making a first rate qualitative breakthrough, and a much better chance of success as a second rank scientist – perhaps making numerous incremental and quantitative advances in the most prestigious areas of existing science.
As argued above, at this age the small chance of a Nobel prize at (say) 65 years old would strike most objective people as hopelessly unlikely, and vastly remote compared with the much more immediate prospect of generating high-impact, highly-cited, well-funded normal science leading reliably to a job at a prestigious institution within the decade. Our feeling is that the only effective incentive to encourage this young scientist into the high-risk strategy of revolutionary science is the prospect of becoming fabulously rich at a stroke – in other words the prospect of winning a mega-prize for revolutionary science.
The prospect of vast riches in the near-ish future is an important motivation to encourage high achievement in creative areas of popular culture in fields such as music, acting and sports. The competition in these areas is intense, and the percentage chance of success is very low – but ‘the mass market’ rewards success very highly and the reward comes while the person is still young – so the incentive is that much more powerful. Music, acting and sports are among the few fields in which young people can become fabulously rich while still young, and there is therefore no shortage (indeed, a huge surplus) of young people competing in these areas of endeavour while eschewing safer and more secure careers [7].
Our point is not that it is necessarily socially beneficial to have so many young people chasing so few niches in music, sports and acting – rather to emphasize that a large and not-too-distant financial reward seems to be a powerful incentive in creative activities. If it works in the arts, we believe the motivating effect of riches would also work in the sciences. We see no reason why revolutionary science would be an exception.
Why mega-cash prizes for revolutionary science?
Traditional science prizes gain their prestige from their extreme rarity – for example, Nobel prizes are awarded to a maximum of three people per year in each discipline (and this rarity would still apply even if the number of Nobel prizes were expanded, as we have advocated [2] and [5]). So, Nobel prizes are essentially prestige rewards. The financial reward attached to Nobel prizes (although it is fairly generous – over one million US dollars shared among the recipients) is of such little motivational significance that media reports often neglect to mention the sum of money.
But in the early days of Nobel prizes, the large amount of money attached to each award was a major reason for the prestige of the prize. If mega-cash prizes became used as an incentive to promote revolutionary science, then the intrinsic status of the prize would again be dependent mainly on the amount of money (rather than the sheer status of winning the prize) because the intention of using mega-cash prizes is that there be many such prizes without the large numbers diluting the motivational effect of the prize.
Traditional science prizes (such as Nobels) therefore constitute a zero sum game in which the more prizes are awarded the less prestige attaches to each prize – because there is only a fixed amount of status to be shared. But this does not apply to monetary rewards – a prize of one hundred million dollars remains well-worth winning whether it is unique or whether 10 or 100 other people also get a 100 million dollar prize. This is important because there need to be enough prizes for revolutionary science that competitors should feel they have a realistic chance of winning one of these prizes so long as their research succeeds in its aims. This would enable there to be a significant incentive to do revolutionary science across as many scientific disciplines as there are mega-cash prizes.
Our feeling is that mega-prizes to stimulate revolutionary science would need to be of the order of magnitude of tens of millions of US dollars in order to replicate the kind of incentives seen in popular creative activities such as music and sports.
Potential problems with mega-cash prizes
There are (at least) two major problems in using mega-prizes to stimulate revolutionary science. However both problems are potentially soluble.
The first problem is that the prizes must have a basis in objective fact, to guard against the prizes being awarded for subjective reasons (for example for political reasons – as has arguably been the case for the MacArthur ‘genius’ fellowships (www.macfound.org) – where significant numbers of recipients seem to have been chosen for their symbolic value rather than their measurable achievement).
To guard against this possibility, our proposal is that mega-prizes should be awarded only to those who have objective evidence of having performed successful revolutionary science. This could be accomplished by specifying objective scientometric criteria which must be satisfied before a person or group can be considered eligible for a prize.
A second difficulty is that mega-prizes must be awarded early enough in a person’s lifespan to act as an incentive to aspiring scientists who are planning their career strategy in their mid-twenties. We think this implies that these prizes should usually be awarded before the age of fifty.
The paradox is that revolutionary science prizes are intended to promote ambitious long term strategic research. Yet to be an effective incentive the prize must be awarded in the medium term (and not the long term). In other words, a compromise is necessary.
In practice, a mega-cash prize before fifty would encourage the brightest 25–35 year old scientists to adopt a time horizon of about ten years for research coming to fruition – on the assumption that a decade-level of long-termism is worthwhile in a context of normal science which typically rewards achievement in units of more like 3–5 years.
A prize awarded before fifty would allow post-doctoral scientists to work on a problem for about a decade, then would allow approximately another decade for the importance of this work to become apparent and for a revolutionary breakthrough measurably to influence the research practices of other scientists.
Scientometrics as a basis for revolutionary science prizes
To be an effective incentive, a prize needs to be relatively transparent and objective, so that the aspiring scientist can be reasonably confident that if they do in fact achieve success in revolutionary science, then this will probably be noticed and they will in likelihood be considered for a prize.
The necessary level of transparency and objectivity can best be achieved by having a first stage selection process based on objective scientometric criteria. This, in turn, requires the development of scientometric instruments for measuring revolutionary science [2] and [8]. Such scientometric instruments are not currently available, and the development and testing of scientometric methods for measuring revolutionary science would – we hope – be a very valuable by product or spin-off benefit of using mega-prizes to reward revolutionary science.
A proper consideration of the topic of scientometric methods for detecting and measuring revolutionary science requires separate treatment, but for the present is may suffice to say that the basis of objective recognition of successful revolutionary science is that the success of revolutionary science can be defined by the fact that revolutionary science affects the direction of normal science. In other words, what makes revolutionary science a success is that is changes normal science then becomes normal science.
In terms of scientometrics, this means that revolutionary science can (in principle) be identified retrospectively from the fact that a small set of revolutionary science communications generate a much larger set of normal science communications which are referenced-back to that originating revolutionary science. In a nutshell, successful revolutionary science can be defined as the work that leads to the evolution of a new scientific specialty.
A new scientific specialty is typically either a sub-specialty of a previous science or a hybrid science. A sub-specialty example is when new branch of medical science develops around a class of disease – e.g. lung disease or liver disease; further new sub-specialty sciences may then arise from sub-classes of these disease classes – e.g. asthma sub-specializing from lung diseases, or hepatitis from liver diseases; and then the process may continue. An example of a hybrid science would be biochemistry – when a new specialty was created by the simultaneous application of theories, techniques and other forms of knowledge from both sub-sets of biology and chemistry knowledge.
This means that some revolutionary science (although not all of it) should be identifiable from a sophisticated analysis of citations within the scientific literature. For example, there may be an observation that over a specified period of time (between, say, 5–10 years) a new cluster of inter-referenced science communications has emerged. This could be detected by the emergence of a new set of specialized conferences, journals and papers – detected using specific terms and methods. More sophisticated methods could include the analysis of emerging citation clusters representing new foci of scientific activity [e.g. [9] and [10]].
The main difficulty is that not all scientific communications are accessible to analysis. For example, as well as formal scientific papers and other public communications there are many un-recorded informal interactions between scientists occurring verbally and by ephemeral or inaccessible media such as notes, letters and private e-mails – not to mention the thoughts inside each scientists head! So scientometrics will only sample from a sub-set of science communications, and it is inevitable that some examples of revolutionary science will remained undetected or under-estimated.
Nonetheless, given the advantages of objective quantification, we would advocate that the field of possible recipients of revolutionary science mega prizes should initially be defined by scientometric methods. After this potential field has been defined, then expert peer review methods could be used to determine whether the identified potential examples of successful revolutionary science were primarily the work of a small number of individual scientists (potential prize recipients); or alternatively the work of teams within a small number of research institutions (in which case the prize could be awarded to the institutions).
Prizes instead of program grants
In conclusion, we suggest that revolutionary science could be encouraged by increasing the monetary incentives for successful revolutionary science – especially the incentives as they operate on the best young scientists as they choose their career paths in their mid twenties to early thirties.
This could be accomplished by a change in behaviour of the large grant awarding bodies – a shift from funding research programs with grants and towards rewarding successful revolutionary science with prizes. For example, a research foundation working in a specific scientific field might at present spend 100 million dollars per year – and might spread this money among ten 10 million dollar program grants. In all likelihood, this money will at present be spent on normal science, and will produce modest incremental progress.
We are suggesting that such a research foundation might instead spend 100 million dollars in a single prize, awarded to a relatively young scientist or a few scientists in recognition of a significant success in revolutionary science.
In the short term, this kind of prize would serve merely as a retrospective recognition of research which had been done anyway – but after a few years the mega-cash prize would begin to work as a prospective incentive; shaping the behaviour of young scientists towards more ambitious scientific problems which (if successfully solved) would be eligible for such prizes.
There is a previous literature on the use of prizes to stimulate scientific research [11], [12], [13] and [14] – however, these types of prizes have either implicitly or explicitly been orientated towards problem solving as quickly as possible and therefore using the simplest possible methods – since this ‘research and development’ approach is most likely to win the prize.
What is novel about our argument here, is that we are suggesting that prizes may also be set-up such that they encourage revolutionary science. Furthermore, we advocate the use of scientometrics as a screening mechanism before peer review as a method of preventing corruption and ensuring that the research being rewarded has had an objectively verifiable consequence of revolutionizing (i.e. changing the direction of, or opening-up new fields for) the practice of science.
In other words, mega-cash prizes might encourage some of the very best young scientists to make more long-term and high risk career choices. The real winner of this would be society as a whole; since normal science can successfully be done by second rate scientists – but if the first rate scientists do not make the decision to tackle the toughest scientific problems, then solutions to these tough problems may be delayed, or they may never be solved.
References
[1] T.S. Kuhn, The structure of scientific revolutions, Chicago University Press, Chicago (1970).
[2] B.G. Charlton and P. Andras, Evaluating universities using simple scientometric research output metrics, Sci Publ Policy 34 (2007), pp. 555–563.
[3] D.L. Hull, Science as a process, Chicago University Press, Chicago (1988).
[4] Caplan B. George Mason University – Econ 103: Labour markets and labour regulation. [accessed 02.01.08].
[5] B.G. Charlton, Why there should be more science Nobel prizes and laureates, Med Hypotheses 68 (2007), pp. 471–473.
[6] F.L. Holmes, Investigative pathways, Yale University Press, New Haven (USA) (2004).
[7] R.H. Frank and P. Cook, The winner take all society, The Free Press, New York (1995).
[8] Charlton B, Andras P. The ‘down-shifting’ of UK science? – The decline of ‘revolutionary science’ and the rise of ‘normal science’ in the UK compared with the USA. Med Hypotheses, in press. doi:10.1016/j.mehy.2007.12.004.
[9] A.F.J. Van Raan, Reference-based publication networks with episodic memories, Scientometrics 6393 (2005), pp. 549–566.
[10] Van Raan AFJ. Scaling rules in the science system: influence of field-specific citation characteristics on the impact of research groups.; 2007.
[11] D.F. Horrobin, Glittering prizes for research support, Nature 324 (1986), p. 221. Full Text via CrossRef
[12] Davis LN. Should we consider alternative incentives for basic research? Patents vs. prizes. Presented at DRUID summer conference 2002.; 2002 [accessed 02.01.08].
[13] B.G. Charlton, Mega-prizes in medicine: big cash awards may stimulate useful and rapid therapeutic innovation, Medi Hypotheses 68 (2006), pp. 1–3.
[14] J.E. Stiglitz, Scrooge and intellectual property rights: a medical prize fund could improve the financing of drug innovations, BMJ 333 (2006), pp. 1279–1280.
Stimulating revolutionary science with mega-cash prizes
Bruce G. Charlton (a) and Peter Andras (b)
Medical Hypotheses - Volume 70, Issue 4, 2008, Pages 709-713
(a) Editor-in-Chief – Medical Hypotheses, Newcastle University, NE1 7RU, UK and (b) Editorial Advisory Board – Medical Hypotheses, Newcastle University, NE1 7RU, UK
Available online 5 March 2008.
Summary
We argue that the most ambitious science is intrinsically riskier science, more likely to fail. It is almost always a safer career strategy for the best scientists to seek to extend knowledge more modestly and to build incrementally on existing ideas and methods. Therefore, higher rewards for success are a necessary incentive to encourage top scientists to work on the most important scientific problems, ones where the solution has potentially revolutionary implications. We suggest that mega-cash prizes (measured in tens of millions of dollars) are a suitable reward for those individuals (or institutions) whose work has triggered radically new directions in science.
***
Rewards for successful revolutionary science
Revolutionary science may be distinguished from ‘normal’ science in that revolutionary science aims at generating qualitative advances on established science while normal science aims at incremental progress [1]. While there is a grey borderline, there is a clear distinction between research that aims at transformation of a scientific discipline and that which aims at extension of that discipline [2].
Naturally, since revolutionary science is more ambitious, it is more likely to fail. For every successful instance of revolutionary science there are likely to be manifold examples of failure [3]. By contrast, ‘normal’ incremental science is much more likely to succeed, especially when it is performed by able and well-trained scientists working in well-resourced institutions.
Given that revolutionary science is a high risk endeavour which usually fails; it is likely to thrive only when the incentives rewarding the rare instances of success are greater than for normal science. Therefore we would argue that it is insufficient for successful revolutionary scientists merely to get the usual rewards of prestigious professorships, respect from within the scientific profession, and a modestly high level of reasonably secure income. Something more is needed: lots of money.
The money incentive in science
To compensate for the intrinsically greater risk of failure, successful revolutionary science requires greater rewards than normal science; rewards such as higher prestige, better jobs and/or more money. We suggest that more money is the most promising incentive to encourage revolutionary science, because it is the factor which is most-controllable.
Historically, the main reward for scientific success was high prestige. It was possible for a successful genius to transform a whole science – as Darwin transformed biology and Newton transformed physics. After such success these scientists became public figures so there was an incentive of ‘immortality’ (e.g. Darwin and Newton have appeared on UK banknotes). But now that science is divided into numerous sub-specialties there is less prospect of general public esteem and the rewards of high status are confined to recognition within what may be a relatively small and specific scientific discipline.
Nor is revolutionary science likely to be rewarded with better jobs, except at the very top stratum of eminence such as Nobel laureates. The prospect of rewarding successful revolutionary scientists with better jobs than successful normal scientists is unlikely to happen. Economists usually suggest that the basis of the salary and conditions of a job are the (probable) marginal effects that an individual has on future productivity of an organization [4]. This implies that salaries are not given for past achievement, except when this enhances future prospects for the organization. For example, the top research universities in the USA seem to compete to have Nobel laureates on their faculty as a symbol of their scientific eminence. This signal is apparently effective even when the laureates are semi-retired and unproductive.
But this is due to the extreme rarity of Nobel laureates [5], and at lower levels of eminence there is little advantage for an institution to employ people who were, in the past, successful at revolutionary science – and to employ them at the enhanced rates of pay and privileged conditions of service which are necessary to compensate them for having chosen the high-risk path of revolutionary science.
A scientist of high ability who chooses revolutionary science as a career will probably and on average attain lower outputs, lower numbers of citations, lower-impact publications and less professional prestige than if they put the same efforts and abilities into normal science. (To put in another way, a scientist would probably gain a higher rate of science production by aiming directly at attaining high science production, than by aiming to solve a major problem.)
An able and committed scientist choosing a normal science path would therefore usually be able to out-perform himself as a revolutionary scientist, in terms of immediate and measurable performance measures. A longer term strategy will tend to generate results and produce rewards later. Even if everything goes perfectly and a successful revolutionary scientist ends-up with a Nobel prize, the chances are that this will come near or after the end of their professional career.
But the prospect of a major prize such as a Nobel is surely too unlikely, too remote and too uncertain to be a widespread or realistic motivation in the career paths of young scientists in their twenties or thirties. And it is at this age when scientists must decide whether or not to pursue revolutionary science [6].
Incentives for the best young scientists to pursue revolutionary science
The critical decision to embark on a high-risk strategy of revolutionary science would typically come not much later than a scientist’s late-twenties – just after they have finished their PhD or equivalent research training [6]. Of course, some young scientists will be so idealistic (or so unrealistic) that they ignore the potential rewards or costs of their career choices. Nonetheless, incentives usually make a difference to human behaviour, and if there were more powerful incentives, then presumably more scientists would opt to practice revolutionary science. So, what are the incentives which might affect a young and gifted scientist’s career selection?
Let us imagine an outstanding young scientist who has the potential to be first rate. He or she is faced by a choice between a high risk strategy of trying to make a revolutionary contribution to their branch of science, or else to ‘down-shift’ to a less ambitious but lower-risk path of doing a large volume of high-quality normal science. The best scientists are, in other words, in a position to choose between a small chance of success at the goal of making a first rate qualitative breakthrough, and a much better chance of success as a second rank scientist – perhaps making numerous incremental and quantitative advances in the most prestigious areas of existing science.
As argued above, at this age the small chance of a Nobel prize at (say) 65 years old would strike most objective people as hopelessly unlikely, and vastly remote compared with the much more immediate prospect of generating high-impact, highly-cited, well-funded normal science leading reliably to a job at a prestigious institution within the decade. Our feeling is that the only effective incentive to encourage this young scientist into the high-risk strategy of revolutionary science is the prospect of becoming fabulously rich at a stroke – in other words the prospect of winning a mega-prize for revolutionary science.
The prospect of vast riches in the near-ish future is an important motivation to encourage high achievement in creative areas of popular culture in fields such as music, acting and sports. The competition in these areas is intense, and the percentage chance of success is very low – but ‘the mass market’ rewards success very highly and the reward comes while the person is still young – so the incentive is that much more powerful. Music, acting and sports are among the few fields in which young people can become fabulously rich while still young, and there is therefore no shortage (indeed, a huge surplus) of young people competing in these areas of endeavour while eschewing safer and more secure careers [7].
Our point is not that it is necessarily socially beneficial to have so many young people chasing so few niches in music, sports and acting – rather to emphasize that a large and not-too-distant financial reward seems to be a powerful incentive in creative activities. If it works in the arts, we believe the motivating effect of riches would also work in the sciences. We see no reason why revolutionary science would be an exception.
Why mega-cash prizes for revolutionary science?
Traditional science prizes gain their prestige from their extreme rarity – for example, Nobel prizes are awarded to a maximum of three people per year in each discipline (and this rarity would still apply even if the number of Nobel prizes were expanded, as we have advocated [2] and [5]). So, Nobel prizes are essentially prestige rewards. The financial reward attached to Nobel prizes (although it is fairly generous – over one million US dollars shared among the recipients) is of such little motivational significance that media reports often neglect to mention the sum of money.
But in the early days of Nobel prizes, the large amount of money attached to each award was a major reason for the prestige of the prize. If mega-cash prizes became used as an incentive to promote revolutionary science, then the intrinsic status of the prize would again be dependent mainly on the amount of money (rather than the sheer status of winning the prize) because the intention of using mega-cash prizes is that there be many such prizes without the large numbers diluting the motivational effect of the prize.
Traditional science prizes (such as Nobels) therefore constitute a zero sum game in which the more prizes are awarded the less prestige attaches to each prize – because there is only a fixed amount of status to be shared. But this does not apply to monetary rewards – a prize of one hundred million dollars remains well-worth winning whether it is unique or whether 10 or 100 other people also get a 100 million dollar prize. This is important because there need to be enough prizes for revolutionary science that competitors should feel they have a realistic chance of winning one of these prizes so long as their research succeeds in its aims. This would enable there to be a significant incentive to do revolutionary science across as many scientific disciplines as there are mega-cash prizes.
Our feeling is that mega-prizes to stimulate revolutionary science would need to be of the order of magnitude of tens of millions of US dollars in order to replicate the kind of incentives seen in popular creative activities such as music and sports.
Potential problems with mega-cash prizes
There are (at least) two major problems in using mega-prizes to stimulate revolutionary science. However both problems are potentially soluble.
The first problem is that the prizes must have a basis in objective fact, to guard against the prizes being awarded for subjective reasons (for example for political reasons – as has arguably been the case for the MacArthur ‘genius’ fellowships (www.macfound.org) – where significant numbers of recipients seem to have been chosen for their symbolic value rather than their measurable achievement).
To guard against this possibility, our proposal is that mega-prizes should be awarded only to those who have objective evidence of having performed successful revolutionary science. This could be accomplished by specifying objective scientometric criteria which must be satisfied before a person or group can be considered eligible for a prize.
A second difficulty is that mega-prizes must be awarded early enough in a person’s lifespan to act as an incentive to aspiring scientists who are planning their career strategy in their mid-twenties. We think this implies that these prizes should usually be awarded before the age of fifty.
The paradox is that revolutionary science prizes are intended to promote ambitious long term strategic research. Yet to be an effective incentive the prize must be awarded in the medium term (and not the long term). In other words, a compromise is necessary.
In practice, a mega-cash prize before fifty would encourage the brightest 25–35 year old scientists to adopt a time horizon of about ten years for research coming to fruition – on the assumption that a decade-level of long-termism is worthwhile in a context of normal science which typically rewards achievement in units of more like 3–5 years.
A prize awarded before fifty would allow post-doctoral scientists to work on a problem for about a decade, then would allow approximately another decade for the importance of this work to become apparent and for a revolutionary breakthrough measurably to influence the research practices of other scientists.
Scientometrics as a basis for revolutionary science prizes
To be an effective incentive, a prize needs to be relatively transparent and objective, so that the aspiring scientist can be reasonably confident that if they do in fact achieve success in revolutionary science, then this will probably be noticed and they will in likelihood be considered for a prize.
The necessary level of transparency and objectivity can best be achieved by having a first stage selection process based on objective scientometric criteria. This, in turn, requires the development of scientometric instruments for measuring revolutionary science [2] and [8]. Such scientometric instruments are not currently available, and the development and testing of scientometric methods for measuring revolutionary science would – we hope – be a very valuable by product or spin-off benefit of using mega-prizes to reward revolutionary science.
A proper consideration of the topic of scientometric methods for detecting and measuring revolutionary science requires separate treatment, but for the present is may suffice to say that the basis of objective recognition of successful revolutionary science is that the success of revolutionary science can be defined by the fact that revolutionary science affects the direction of normal science. In other words, what makes revolutionary science a success is that is changes normal science then becomes normal science.
In terms of scientometrics, this means that revolutionary science can (in principle) be identified retrospectively from the fact that a small set of revolutionary science communications generate a much larger set of normal science communications which are referenced-back to that originating revolutionary science. In a nutshell, successful revolutionary science can be defined as the work that leads to the evolution of a new scientific specialty.
A new scientific specialty is typically either a sub-specialty of a previous science or a hybrid science. A sub-specialty example is when new branch of medical science develops around a class of disease – e.g. lung disease or liver disease; further new sub-specialty sciences may then arise from sub-classes of these disease classes – e.g. asthma sub-specializing from lung diseases, or hepatitis from liver diseases; and then the process may continue. An example of a hybrid science would be biochemistry – when a new specialty was created by the simultaneous application of theories, techniques and other forms of knowledge from both sub-sets of biology and chemistry knowledge.
This means that some revolutionary science (although not all of it) should be identifiable from a sophisticated analysis of citations within the scientific literature. For example, there may be an observation that over a specified period of time (between, say, 5–10 years) a new cluster of inter-referenced science communications has emerged. This could be detected by the emergence of a new set of specialized conferences, journals and papers – detected using specific terms and methods. More sophisticated methods could include the analysis of emerging citation clusters representing new foci of scientific activity [e.g. [9] and [10]].
The main difficulty is that not all scientific communications are accessible to analysis. For example, as well as formal scientific papers and other public communications there are many un-recorded informal interactions between scientists occurring verbally and by ephemeral or inaccessible media such as notes, letters and private e-mails – not to mention the thoughts inside each scientists head! So scientometrics will only sample from a sub-set of science communications, and it is inevitable that some examples of revolutionary science will remained undetected or under-estimated.
Nonetheless, given the advantages of objective quantification, we would advocate that the field of possible recipients of revolutionary science mega prizes should initially be defined by scientometric methods. After this potential field has been defined, then expert peer review methods could be used to determine whether the identified potential examples of successful revolutionary science were primarily the work of a small number of individual scientists (potential prize recipients); or alternatively the work of teams within a small number of research institutions (in which case the prize could be awarded to the institutions).
Prizes instead of program grants
In conclusion, we suggest that revolutionary science could be encouraged by increasing the monetary incentives for successful revolutionary science – especially the incentives as they operate on the best young scientists as they choose their career paths in their mid twenties to early thirties.
This could be accomplished by a change in behaviour of the large grant awarding bodies – a shift from funding research programs with grants and towards rewarding successful revolutionary science with prizes. For example, a research foundation working in a specific scientific field might at present spend 100 million dollars per year – and might spread this money among ten 10 million dollar program grants. In all likelihood, this money will at present be spent on normal science, and will produce modest incremental progress.
We are suggesting that such a research foundation might instead spend 100 million dollars in a single prize, awarded to a relatively young scientist or a few scientists in recognition of a significant success in revolutionary science.
In the short term, this kind of prize would serve merely as a retrospective recognition of research which had been done anyway – but after a few years the mega-cash prize would begin to work as a prospective incentive; shaping the behaviour of young scientists towards more ambitious scientific problems which (if successfully solved) would be eligible for such prizes.
There is a previous literature on the use of prizes to stimulate scientific research [11], [12], [13] and [14] – however, these types of prizes have either implicitly or explicitly been orientated towards problem solving as quickly as possible and therefore using the simplest possible methods – since this ‘research and development’ approach is most likely to win the prize.
What is novel about our argument here, is that we are suggesting that prizes may also be set-up such that they encourage revolutionary science. Furthermore, we advocate the use of scientometrics as a screening mechanism before peer review as a method of preventing corruption and ensuring that the research being rewarded has had an objectively verifiable consequence of revolutionizing (i.e. changing the direction of, or opening-up new fields for) the practice of science.
In other words, mega-cash prizes might encourage some of the very best young scientists to make more long-term and high risk career choices. The real winner of this would be society as a whole; since normal science can successfully be done by second rate scientists – but if the first rate scientists do not make the decision to tackle the toughest scientific problems, then solutions to these tough problems may be delayed, or they may never be solved.
References
[1] T.S. Kuhn, The structure of scientific revolutions, Chicago University Press, Chicago (1970).
[2] B.G. Charlton and P. Andras, Evaluating universities using simple scientometric research output metrics, Sci Publ Policy 34 (2007), pp. 555–563.
[3] D.L. Hull, Science as a process, Chicago University Press, Chicago (1988).
[4] Caplan B. George Mason University – Econ 103: Labour markets and labour regulation.
[5] B.G. Charlton, Why there should be more science Nobel prizes and laureates, Med Hypotheses 68 (2007), pp. 471–473.
[6] F.L. Holmes, Investigative pathways, Yale University Press, New Haven (USA) (2004).
[7] R.H. Frank and P. Cook, The winner take all society, The Free Press, New York (1995).
[8] Charlton B, Andras P. The ‘down-shifting’ of UK science? – The decline of ‘revolutionary science’ and the rise of ‘normal science’ in the UK compared with the USA. Med Hypotheses, in press. doi:10.1016/j.mehy.2007.12.004.
[9] A.F.J. Van Raan, Reference-based publication networks with episodic memories, Scientometrics 6393 (2005), pp. 549–566.
[10] Van Raan AFJ. Scaling rules in the science system: influence of field-specific citation characteristics on the impact of research groups.
[11] D.F. Horrobin, Glittering prizes for research support, Nature 324 (1986), p. 221. Full Text via CrossRef
[12] Davis LN. Should we consider alternative incentives for basic research? Patents vs. prizes. Presented at DRUID summer conference 2002.
[13] B.G. Charlton, Mega-prizes in medicine: big cash awards may stimulate useful and rapid therapeutic innovation, Medi Hypotheses 68 (2006), pp. 1–3.
[14] J.E. Stiglitz, Scrooge and intellectual property rights: a medical prize fund could improve the financing of drug innovations, BMJ 333 (2006), pp. 1279–1280.