fbpx
Wikipedia

Me-too drug

January 01, 1970

The term "me-too drug" or "follow-on drug" refers to a medication that is similar to a pre-existing drug, usually by making minor modifications to the prototype, reflected in slight changes in the profiles of side effects or activity, and used to treat conditions for which drugs already exist.[1][2] While pharmaceutical companies have justified the development of me-toos as offering incremental improvements in efficacy, side-effects, compliance and cost, critics have questioned the increasing marketing of me-toos, their absorption of research and development resources and their impact on the innovation of new treatments.[3][4][5]

In 1956, Louis S. Goodman, co‐editor of Goodman and Gilman, referred to “the problem of the introduction of ‘me too’ drugs, that is, drugs without signal advantage of any sort”.[1] However, me-too drugs can be novel compounds themselves.[3][6] They are commonly used and include several beta blockers, antidepressants and stomach acid reducing and cholesterol lowering drugs.[1]

History edit

 
Louis Goodman, who coined the phrase "me-too"

The term "me‐too drugs" was coined in the 1950s. In 1956, Louis S. Goodman, co‐editor of Goodman and Gilman, referred to “the problem of the introduction of ‘me too’ drugs, that is, drugs without signal advantage of any sort”.[1] Once a new drug class was discovered, other major drug companies made efforts to produce their own similar versions. Pharmacologist Milton Silverman and physician Philip R. Lee noted "the great drug therapy era was marked not only by the introduction of new drugs in great profusion and by the launching of large promotional campaigns but also by the introduction of what are known as 'duplicative' or 'me-too' products".[7]

Between 1960 and 1962, Estes Kefauver, then Senator of Tennessee, led a series of hearings enquiring about the pharmaceutical industry's motive to produce me-too drugs after it was noted that much of their time and resources were spent producing them. Subsequently, the FDA required drug companies to prove their drugs were safe and effective.[7] In 1964, Louis Lasagna described me-too drugs as being “hard to justify putting into man at all, let alone on the market”.[1] Three years later, the term appeared in the Oxford English Dictionary.[1] In the early 1970s, Silverman and Lee reported that there were almost 100 tranquillisers, 130 antihistamines, greater than 270 antibiotics and more than 200 sulfonamides.[7]

In 1994, Desmond Laurence's textbook Clinical Pharmacology referred to me-too as "me-again".[1]

Definition edit

There is no agreed definition, however, several have been proposed,[1] including:

  • "multiple drugs within the same therapeutic class"
  • "drugs that are chemically related to the prototype, or other chemical compounds which have an identical mechanism of action"
  • "drugs which have more or less identical clinical outcomes to pre‐existing drugs"
  • "a drug with a similar chemical structure or the same mechanism of action as a drug that is already marketed".[1]

Biosimilars are compared with other biosimilars and are therefore not me-toos.[8][9]

Examples edit

Me-too drugs include diazepam, ranitidine and esketamine.[1]

Beta blockers edit

The first-in-class β-blocker pronethalol was developed by James Black at ICI Pharmaceuticals. It was followed by propranolol, sotalol, practolol, metoprolol, labetalol, acebutolol and bisoprolol. Successive differences between β-blockers have had a combined cumulative effect and are seen as "innovative".[1]

Benzodiazepines edit

15 benzodiazepines were marketed in the UK between 1960 and 1982, of which seven were produced by Roche.[1]

Proton pump inhibitors edit

The proton-pump inhibitor Nexium by AstraZeneca is a me-too which was granted its patent by showing that it was effective for heartburn, not that it was better than its precursor, Prilosec.[10] It was shown to preserve revenues of Prilosec, whose U.S. patent expired in 2001. Considered a new drug by the FDA, Nexium was patented separately, sold for eight times the cost of its generic esomeprazole and advertised as significantly better than its predecessor, a move the company received much criticism for, with a subsequent class action lawsuit filed against them.[11]

H2 antagonists edit

Both Tagamet's and Zantac's prices increased following the arrival of further me-too drugs Pepcid and Axid.[4][12]

ACE inhibitors edit

Several me-toos followed the prototype of the ace inhibitor, captopril, with enalapril being its first me-too.[1] Most were as efficient as each other and had similar adverse effect profiles.[11]

Statins edit

When Merck's cholesterol-lowering statin Mevacor (lovastatin) was approved by the U.S. Food and Drug Administration (FDA) in 1987, the understanding of the link between cholesterol and heart disease was improving, and the potential market for the drug became significant. Subsequently, several other companies developed similar drugs: Merck developed Zocor (simvastatin) and Crestor (rosuvastatin), Pfizer developed Lipitor (atorvastatin), Bristol-Myers Squibb developed Pravachol (pravastatin), and Novartis developed Lescol (fluvastatin).[13][14][15] Others include pitavastatin (Livalo).[1]

Antidepressants edit

Imipramine was the first-in-class of the tricyclic antidepressants. Amitriptyline, Nortriptyline, Dosulepin and Doxepin are some of the me-toos that followed.[1] Several me-too Selective serotonin reuptake inhibitors have been developed for maintenance treatment in chronic depression. These include Paxil (paroxetine), Celexa (citalopram), Zoloft (sertraline), Lexapro (escitalopram) and Prozac (fluoxetine).[16]

For example, Celexa is a mixture of a left-handed and right-handed version of the same compound ("citalopram"), but only the left-handed version ("es-citalopram") is biologically active. Lexapro, the "me too" drug released several years after Celexa thus extending the patent life, is a purified form of just the left-handed version (the "es" in "es-citalopram").[17]

Antivirals edit

Gilead Science's Descovy is a me-too drug of Truvada, a popular Antiretroviral also used to prevent HIV infection in healthy people. Both versions are prodrugs that metabolize into the same active compound. Gilead has been accused in lawsuits of "slow walking" the development of the me-too drug;[18] however, such lawsuits further a market perception the me-too drug is "safer." This drives sales of the more expensive me-too drug when both drugs have virtually identical safety profiles. Similarly, Valtrex, first FDA approved in 2001 to treat persistent herpes outbreaks is a prodrug of acyclovir, first FDA approved in the mid 1980's. Valtrex metabolizes into acyclovir in the liver,[19] but when it first entered the market, it cost many times than the generic.

Debate edit

In 2005, a report by the International Policy Network defended me-toos, describing their development as "incremental improvements on already existing drugs".[20] The report stated:

... this often represent(s) advances in safety and efficacy, along with providing new formulations and dosing options that significantly increase patient compliance. From an economic standpoint, expanding drug classes represent the possibility of lower drug prices as competition between manufacturers is increased. Additionally, pharmaceutical companies depend on incremental innovations to provide the revenue that will support the development of more risky “block-buster” drugs. Policies aimed at curbing incremental innovation will ultimately lead to a reduction in the overall quality of existing drug classes and may ultimately curb the creation of novel drugs.[20]

This incremental innovation has led to some referring to me-toos as "me-betters".[14][21]

Many physicians are unaware that me-toos are compared to placebos rather than pre-existing drugs.[22] Me-toos are seen as patentable new drugs and therefore substantial profit makers, where innovative drugs may be more risky to develop.[13][23][24]

Statistics edit

Between 1998 and 2003, the U.S. Food and Drug Administration (FDA) approved 487 drugs, of which 78 per cent appeared to have similar characteristics to pre-existing marketed drugs.[25]

More than 60% of medicines listed on the World Health Organization's essential list are me‐too drugs.[1]

In September 2019, half of antibiotics under clinical development were “me-too” drugs. At the beginning of 2020, the WHO stated that only two of the 50 antibiotics in clinical development are active against serious drug resistant gram-negative bacteria, and most are not significant "upgrades" of drugs.[26][27]

See also edit

References edit

  1. ^ a b c d e f g h i j k l m n o p Aronson, Jeffrey K.; Green, A. Richard (13 May 2020). "Me‐too pharmaceutical products: History, definitions, examples, and relevance to drug shortages and essential medicines lists". British Journal of Clinical Pharmacology. 86 (11): 2114–2122. doi:10.1111/bcp.14327. PMC 7576625. PMID 32358800.
  2. ^ Vincent Rajkumar, S. (23 June 2020). "The high cost of prescription drugs: causes and solutions". Blood Cancer Journal. 10 (6): 71. doi:10.1038/s41408-020-0338-x. PMC 7311400. PMID 32576816.
  3. ^ a b Garattini, Silvio (1997). "Are me-too drugs justified?". Journal of Nephrology. 10 (6): 283–94. PMID 9442441. S2CID 7039484.
  4. ^ a b Hollis, Aidan (13 December 2004). "Me-too drugs: is there a problem" (PDF). World Health Organization. S2CID 3142385.
  5. ^ Mazzucato, Mariana; Li, Henry Lishi; Darzi, Ara (4 March 2020). "Is it time to nationalise the pharmaceutical industry?". BMJ. 368: m769. doi:10.1136/bmj.m769. hdl:10044/1/86122. PMID 32132003. S2CID 212416521. ProQuest 2371182316.
  6. ^ Patterson, Julie A.; Carroll, Norman V. (May 2020). "Should the United States government regulate prescription prices? A critical review". Research in Social and Administrative Pharmacy. 16 (5): 717–723. doi:10.1016/j.sapharm.2019.06.010. PMID 31248779. S2CID 195761512.
  7. ^ a b c Goozner, Merrill (2005). "Me Too!". The $800 Million Pill: The Truth Behind the Cost of New Drugs. University of California Press. pp. 209–230. ISBN 978-0-520-24670-6.
  8. ^ Gutka, Hiten J.; Yang, Harry; Kakar, Shefali (2018). Biosimilars: Regulatory, Clinical, and Biopharmaceutical Development. Springer. p. 129. ISBN 978-3-319-99679-0.
  9. ^ Mason, Jonathan (5 October 2013). "Introduction of biosimilars: not to be confused with generics". Prescriber. 24 (19): 7. doi:10.1002/psb.1108. S2CID 56581328.
  10. ^ Menzel, Paul T. (2012). "Just Access to Health Care and Pharmaceuticals". In Brenkert, George G.; Beauchamp, Tom L. (eds.). The Oxford Handbook of Business Ethics. OUP USA. pp. 202–232. doi:10.1093/oxfordhb/9780195307955.003.0008. hdl:10822/1025918. ISBN 978-0-19-991622-1.
  11. ^ a b Hanekamp, Gerd (2007). Business Ethics of Innovation. Springer. p. 44. ISBN 978-3-540-72309-7.
  12. ^ Jena, Anupam B.; Calfee, John E.; Mansley, Edward C.; Philipson, Tomas J. (2009). "'Me-Too' Innovation in Pharmaceutical Markets". Forum for Health Economics & Policy. 12 (1): 5. doi:10.2202/1558-9544.1138. PMC 5659838. PMID 29081727.
  13. ^ a b Angell, Marcia (2004). The Truth About the Drug Companies: How They Deceive Us and What to Do About It. Random House Publishing Group. p. 80. ISBN 978-1-58836-211-7.
  14. ^ a b Patrick, Graham L. (2013). An Introduction to Medicinal Chemistry. OUP Oxford. p. 181. ISBN 978-0-19-969739-7.
  15. ^ Greene, Jeremy A. (1 October 2010). "'For Me There Is No Substitute'—Authenticity, Uniqueness, and the Lessons of Lipitor". AMA Journal of Ethics. 12 (10): 818–823. doi:10.1001/virtualmentor.2010.12.10.msoc2-1010. PMID 23186743.
  16. ^ Oldani, Michael (2009). "Understanding the 'Therapeutic Embrace' between Big Pharma and Modern Medicine". Pharmacy in History. 51 (2): 75–86. JSTOR 41112425.
  17. ^ Burke, William (2002). "Stereoisomers in Psychiatry: The Case of Escitalopram". Prim Care Companion J Clin Psychiatry. 4 (1): 20–24. doi:10.4088/pcc.v04n0107. PMC 314378. PMID 15014731.
  18. ^ "How a Drugmaker Profited by Slow-Walking a Promising H.I.V. Therapy". New York Times. No. July 23, 2023.
  19. ^ Smith, James (2010). "Pharmacokinetics of acyclovir and its metabolites in cerebrospinal fluid and systemic circulation after administration of high-dose valacyclovir in subjects with normal and impaired renal function". Antimicrob Agents Chemother. 54 (3): 1146–1151. doi:10.1128/AAC.00729-09. PMC 2825963. PMID 20038622.
  20. ^ a b Wertheimer, Albert I.; Santella, Thomas M. (2005). Pharmacoevolution: the advantages of incremental innovation (PDF). International Policy Network; Working Papers on Intellectual Property, Innovation and Health. ISBN 1-905041-05-5.
  21. ^ Nefissa Chakroun (2016). "6.4. Transferring patent information by means of imitation". Patents for Development: Improved Patent Information Disclosure and Access for Incremental Innovation. Cheltenham: Edward Elgar Publishing. p. 150. ISBN 978-1-78536-860-8.
  22. ^ Great Britain: Parliament: House of Commons: Health Committee (2005). The Influence of the Pharmaceutical Industry: Fourth Report of Session 2004-05. The Stationery Office. p. 204. ISBN 978-0-215-02457-2.
  23. ^ "Memorandum by Professor Patrick Vallance (PI 106)". House of Commons, Select Committee on Health Minutes of Evidence. Retrieved 2020-07-21.
  24. ^ Buccafusco, Christopher; Masur, Jonathan S. (31 March 2020). "Drugs, Patents, and Well-Being". Washington University Law Review. SSRN 3565320.
  25. ^ Angell, M. (7 December 2004). "Excess in the pharmaceutical industry". Canadian Medical Association Journal. 171 (12): 1451–1453. doi:10.1503/cmaj.1041594. PMC 534578. PMID 15583183.
  26. ^ O'Brien, Michael K.; Chu, Philip (8 July 2020). "A Market Failure for Antimicrobial Resistant Medicines". Applied Clinical Trials Online.
  27. ^ Price, W. Nicholson (2020). "The Cost of Novelty" (PDF). Columbia Law Review. 120 (3): 769–835. JSTOR 26910477. SSRN 3350477.

January 01, 1970
drug, term, drug, follow, drug, refers, medication, that, similar, existing, drug, usually, making, minor, modifications, prototype, reflected, slight, changes, profiles, side, effects, activity, used, treat, conditions, which, drugs, already, exist, while, ph. The term me too drug or follow on drug refers to a medication that is similar to a pre existing drug usually by making minor modifications to the prototype reflected in slight changes in the profiles of side effects or activity and used to treat conditions for which drugs already exist 1 2 While pharmaceutical companies have justified the development of me toos as offering incremental improvements in efficacy side effects compliance and cost critics have questioned the increasing marketing of me toos their absorption of research and development resources and their impact on the innovation of new treatments 3 4 5 In 1956 Louis S Goodman co editor of Goodman and Gilman referred to the problem of the introduction of me too drugs that is drugs without signal advantage of any sort 1 However me too drugs can be novel compounds themselves 3 6 They are commonly used and include several beta blockers antidepressants and stomach acid reducing and cholesterol lowering drugs 1 Contents 1 History 2 Definition 3 Examples 3 1 Beta blockers 3 2 Benzodiazepines 3 3 Proton pump inhibitors 3 4 H2 antagonists 3 5 ACE inhibitors 3 6 Statins 3 7 Antidepressants 3 8 Antivirals 4 Debate 5 Statistics 6 See also 7 ReferencesHistory edit nbsp Louis Goodman who coined the phrase me too The term me too drugs was coined in the 1950s In 1956 Louis S Goodman co editor of Goodman and Gilman referred to the problem of the introduction of me too drugs that is drugs without signal advantage of any sort 1 Once a new drug class was discovered other major drug companies made efforts to produce their own similar versions Pharmacologist Milton Silverman and physician Philip R Lee noted the great drug therapy era was marked not only by the introduction of new drugs in great profusion and by the launching of large promotional campaigns but also by the introduction of what are known as duplicative or me too products 7 Between 1960 and 1962 Estes Kefauver then Senator of Tennessee led a series of hearings enquiring about the pharmaceutical industry s motive to produce me too drugs after it was noted that much of their time and resources were spent producing them Subsequently the FDA required drug companies to prove their drugs were safe and effective 7 In 1964 Louis Lasagna described me too drugs as being hard to justify putting into man at all let alone on the market 1 Three years later the term appeared in the Oxford English Dictionary 1 In the early 1970s Silverman and Lee reported that there were almost 100 tranquillisers 130 antihistamines greater than 270 antibiotics and more than 200 sulfonamides 7 In 1994 Desmond Laurence s textbook Clinical Pharmacology referred to me too as me again 1 Definition editThere is no agreed definition however several have been proposed 1 including multiple drugs within the same therapeutic class drugs that are chemically related to the prototype or other chemical compounds which have an identical mechanism of action drugs which have more or less identical clinical outcomes to pre existing drugs a drug with a similar chemical structure or the same mechanism of action as a drug that is already marketed 1 Biosimilars are compared with other biosimilars and are therefore not me toos 8 9 Examples editMe too drugs include diazepam ranitidine and esketamine 1 Beta blockers edit The first in class b blocker pronethalol was developed by James Black at ICI Pharmaceuticals It was followed by propranolol sotalol practolol metoprolol labetalol acebutolol and bisoprolol Successive differences between b blockers have had a combined cumulative effect and are seen as innovative 1 Benzodiazepines edit 15 benzodiazepines were marketed in the UK between 1960 and 1982 of which seven were produced by Roche 1 Proton pump inhibitors edit The proton pump inhibitor Nexium by AstraZeneca is a me too which was granted its patent by showing that it was effective for heartburn not that it was better than its precursor Prilosec 10 It was shown to preserve revenues of Prilosec whose U S patent expired in 2001 Considered a new drug by the FDA Nexium was patented separately sold for eight times the cost of its generic esomeprazole and advertised as significantly better than its predecessor a move the company received much criticism for with a subsequent class action lawsuit filed against them 11 H2 antagonists edit Both Tagamet s and Zantac s prices increased following the arrival of further me too drugs Pepcid and Axid 4 12 ACE inhibitors edit Several me toos followed the prototype of the ace inhibitor captopril with enalapril being its first me too 1 Most were as efficient as each other and had similar adverse effect profiles 11 Statins edit When Merck s cholesterol lowering statin Mevacor lovastatin was approved by the U S Food and Drug Administration FDA in 1987 the understanding of the link between cholesterol and heart disease was improving and the potential market for the drug became significant Subsequently several other companies developed similar drugs Merck developed Zocor simvastatin and Crestor rosuvastatin Pfizer developed Lipitor atorvastatin Bristol Myers Squibb developed Pravachol pravastatin and Novartis developed Lescol fluvastatin 13 14 15 Others include pitavastatin Livalo 1 Antidepressants edit Imipramine was the first in class of the tricyclic antidepressants Amitriptyline Nortriptyline Dosulepin and Doxepin are some of the me toos that followed 1 Several me too Selective serotonin reuptake inhibitors have been developed for maintenance treatment in chronic depression These include Paxil paroxetine Celexa citalopram Zoloft sertraline Lexapro escitalopram and Prozac fluoxetine 16 For example Celexa is a mixture of a left handed and right handed version of the same compound citalopram but only the left handed version es citalopram is biologically active Lexapro the me too drug released several years after Celexa thus extending the patent life is a purified form of just the left handed version the es in es citalopram 17 Antivirals edit Gilead Science s Descovy is a me too drug of Truvada a popular Antiretroviral also used to prevent HIV infection in healthy people Both versions are prodrugs that metabolize into the same active compound Gilead has been accused in lawsuits of slow walking the development of the me too drug 18 however such lawsuits further a market perception the me too drug is safer This drives sales of the more expensive me too drug when both drugs have virtually identical safety profiles Similarly Valtrex first FDA approved in 2001 to treat persistent herpes outbreaks is a prodrug of acyclovir first FDA approved in the mid 1980 s Valtrex metabolizes into acyclovir in the liver 19 but when it first entered the market it cost many times than the generic Debate editIn 2005 a report by the International Policy Network defended me toos describing their development as incremental improvements on already existing drugs 20 The report stated this often represent s advances in safety and efficacy along with providing new formulations and dosing options that significantly increase patient compliance From an economic standpoint expanding drug classes represent the possibility of lower drug prices as competition between manufacturers is increased Additionally pharmaceutical companies depend on incremental innovations to provide the revenue that will support the development of more risky block buster drugs Policies aimed at curbing incremental innovation will ultimately lead to a reduction in the overall quality of existing drug classes and may ultimately curb the creation of novel drugs 20 This incremental innovation has led to some referring to me toos as me betters 14 21 Many physicians are unaware that me toos are compared to placebos rather than pre existing drugs 22 Me toos are seen as patentable new drugs and therefore substantial profit makers where innovative drugs may be more risky to develop 13 23 24 Statistics editBetween 1998 and 2003 the U S Food and Drug Administration FDA approved 487 drugs of which 78 per cent appeared to have similar characteristics to pre existing marketed drugs 25 More than 60 of medicines listed on the World Health Organization s essential list are me too drugs 1 In September 2019 half of antibiotics under clinical development were me too drugs At the beginning of 2020 the WHO stated that only two of the 50 antibiotics in clinical development are active against serious drug resistant gram negative bacteria and most are not significant upgrades of drugs 26 27 See also editUnique selling pointReferences edit a b c d e f g h i j k l m n o p Aronson Jeffrey K Green A Richard 13 May 2020 Me too pharmaceutical products History definitions examples and relevance to drug shortages and essential medicines lists British Journal of Clinical Pharmacology 86 11 2114 2122 doi 10 1111 bcp 14327 PMC 7576625 PMID 32358800 Vincent Rajkumar S 23 June 2020 The high cost of prescription drugs causes and solutions Blood Cancer Journal 10 6 71 doi 10 1038 s41408 020 0338 x PMC 7311400 PMID 32576816 a b Garattini Silvio 1997 Are me too drugs justified Journal of Nephrology 10 6 283 94 PMID 9442441 S2CID 7039484 a b Hollis Aidan 13 December 2004 Me too drugs is there a problem PDF World Health Organization S2CID 3142385 Mazzucato Mariana Li Henry Lishi Darzi Ara 4 March 2020 Is it time to nationalise the pharmaceutical industry BMJ 368 m769 doi 10 1136 bmj m769 hdl 10044 1 86122 PMID 32132003 S2CID 212416521 ProQuest 2371182316 Patterson Julie A Carroll Norman V May 2020 Should the United States government regulate prescription prices A critical review Research in Social and Administrative Pharmacy 16 5 717 723 doi 10 1016 j sapharm 2019 06 010 PMID 31248779 S2CID 195761512 a b c Goozner Merrill 2005 Me Too The 800 Million Pill The Truth Behind the Cost of New Drugs University of California Press pp 209 230 ISBN 978 0 520 24670 6 Gutka Hiten J Yang Harry Kakar Shefali 2018 Biosimilars Regulatory Clinical and Biopharmaceutical Development Springer p 129 ISBN 978 3 319 99679 0 Mason Jonathan 5 October 2013 Introduction of biosimilars not to be confused with generics Prescriber 24 19 7 doi 10 1002 psb 1108 S2CID 56581328 Menzel Paul T 2012 Just Access to Health Care and Pharmaceuticals In Brenkert George G Beauchamp Tom L eds The Oxford Handbook of Business Ethics OUP USA pp 202 232 doi 10 1093 oxfordhb 9780195307955 003 0008 hdl 10822 1025918 ISBN 978 0 19 991622 1 a b Hanekamp Gerd 2007 Business Ethics of Innovation Springer p 44 ISBN 978 3 540 72309 7 Jena Anupam B Calfee John E Mansley Edward C Philipson Tomas J 2009 Me Too Innovation in Pharmaceutical Markets Forum for Health Economics amp Policy 12 1 5 doi 10 2202 1558 9544 1138 PMC 5659838 PMID 29081727 a b Angell Marcia 2004 The Truth About the Drug Companies How They Deceive Us and What to Do About It Random House Publishing Group p 80 ISBN 978 1 58836 211 7 a b Patrick Graham L 2013 An Introduction to Medicinal Chemistry OUP Oxford p 181 ISBN 978 0 19 969739 7 Greene Jeremy A 1 October 2010 For Me There Is No Substitute Authenticity Uniqueness and the Lessons of Lipitor AMA Journal of Ethics 12 10 818 823 doi 10 1001 virtualmentor 2010 12 10 msoc2 1010 PMID 23186743 Oldani Michael 2009 Understanding the Therapeutic Embrace between Big Pharma and Modern Medicine Pharmacy in History 51 2 75 86 JSTOR 41112425 Burke William 2002 Stereoisomers in Psychiatry The Case of Escitalopram Prim Care Companion J Clin Psychiatry 4 1 20 24 doi 10 4088 pcc v04n0107 PMC 314378 PMID 15014731 How a Drugmaker Profited by Slow Walking a Promising H I V Therapy New York Times No July 23 2023 Smith James 2010 Pharmacokinetics of acyclovir and its metabolites in cerebrospinal fluid and systemic circulation after administration of high dose valacyclovir in subjects with normal and impaired renal function Antimicrob Agents Chemother 54 3 1146 1151 doi 10 1128 AAC 00729 09 PMC 2825963 PMID 20038622 a b Wertheimer Albert I Santella Thomas M 2005 Pharmacoevolution the advantages of incremental innovation PDF International Policy Network Working Papers on Intellectual Property Innovation and Health ISBN 1 905041 05 5 Nefissa Chakroun 2016 6 4 Transferring patent information by means of imitation Patents for Development Improved Patent Information Disclosure and Access for Incremental Innovation Cheltenham Edward Elgar Publishing p 150 ISBN 978 1 78536 860 8 Great Britain Parliament House of Commons Health Committee 2005 The Influence of the Pharmaceutical Industry Fourth Report of Session 2004 05 The Stationery Office p 204 ISBN 978 0 215 02457 2 Memorandum by Professor Patrick Vallance PI 106 House of Commons Select Committee on Health Minutes of Evidence Retrieved 2020 07 21 Buccafusco Christopher Masur Jonathan S 31 March 2020 Drugs Patents and Well Being Washington University Law Review SSRN 3565320 Angell M 7 December 2004 Excess in the pharmaceutical industry Canadian Medical Association Journal 171 12 1451 1453 doi 10 1503 cmaj 1041594 PMC 534578 PMID 15583183 O Brien Michael K Chu Philip 8 July 2020 A Market Failure for Antimicrobial Resistant Medicines Applied Clinical Trials Online Price W Nicholson 2020 The Cost of Novelty PDF Columbia Law Review 120 3 769 835 JSTOR 26910477 SSRN 3350477 Retrieved from https en wikipedia org w index php title Me too drug amp oldid 1216780325, wikipedia, wiki, book, books, library,

article

, read, download, free, free download, mp3, video, mp4, 3gp, jpg, jpeg, gif, png, picture, music, song, movie, book, game, games.