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History of animal testing

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One ofPavlov's dogs with a saliva-catch container andtube surgically implanted in its muzzle, Pavlov Museum, 2005

Thehistory of animal testing goes back to the writings of theAncient Greeks in the 4th and 3rd centuries BCE, withAristotle (384–322 BCE) andErasistratus (304–258 BCE) one of the first documented to perform experiments on nonhuman animals.[1]Galen, a physician in 2nd-centuryRome, dissected pigs and goats, and is known as the "Father ofVivisection."[2]Avenzoar, anArabic physician in 12th-centuryMoorish Spain who also practiceddissection, introduced animal testing as anexperimental method of testing surgical procedures before applying them to human patients.[3][4] Although the exact purpose of the procedure was unclear, theNeolithic surgeon performedtrepanation on a cow in 3400-3000 BCE.[5] This is the earliest known surgery to have been performed on an animal, and it is possible that the procedure was done on a dead cow in order for the surgeon to practice their skills.

History of animal testing

[edit]
Themouse is a typical testing species.

In 1242,Ibn al-Nafis provided accurate descriptions of thecirculation of blood in mammals. A complete description of this circulation was later provided in the 17th century byWilliam Harvey.

In his unfinished 1627 utopian novel,New Atlantis, scientist and philosopherFrancis Bacon proposed a research center containing "parks and enclosures of all sorts of beasts and birds which we use ... for dissections and trials; that thereby we may take light what may be wrought upon the body of man."

In the 1660s, the physicist Robert Boyle conducted many experiments with a pump to investigate the effects of rarefied air. He listed two experiments on living nonhuman animals: "Experiment 40", which tested the ability of insects to fly under reduced air pressure, and the dramatic "Experiment 41," which demonstrated the reliance of living creatures on the air for their survival. Boyle conducted numerous trials during which he placed a large variety of different nonhuman animals, including birds, mice, eels, snails and flies, in the vessel of the pump and studied their reactions as the air was removed.[6] Here, he describes an injuredlark:

…the Bird for a while appear'd lively enough; but upon a greater Exsuction of the Air, she began manifestly to droop and appear sick, and very soon after was taken with as violent and irregular Convulsions, as are wont to be observ'd in Poultry, when their heads are wrung off: For the Bird threw her self over and over two or three times, and died with her Breast upward, her Head downwards, and her Neck awry.[7]

In the 18th century,Antoine Lavoisier decided to use aguinea pig in acalorimeter because he wanted to prove thatrespiration was a form ofcombustion. He had an impression that combustion and respiration are chemically identical. Lavoisier demonstrated this with the help ofPierre-Simon Laplace. They both carefully measured the amount of "carbon dioxide and heat given off by a guinea pig as (they) breathed".[8] Then they contrasted this to "the amount of heat produced when they burned carbon to produce the same amount of carbon dioxide as had been exhaled by the guinea pig".[8] Their conclusion made Lavoisier confident "that respiration is a form of combustion".[8] Also, the result showed that the heat mammals produce through respiration allowed their bodies to be above room temperature.

Stephen Hales measured blood pressure in thehorse. In the 1780s,Luigi Galvani demonstrated that electricity applied to a dead, dissected, frog's leg muscle caused it to twitch, which led to an appreciation for the relationship between electricity and animation. In the 1880s,Louis Pasteur convincingly demonstrated thegerm theory of medicine by givinganthrax to sheep. In the 1890s,Ivan Pavlov famously used dogs to describeclassical conditioning.

In 1921Otto Loewi provided the first substantial evidence thatneuronal communication with target cells occurred via chemical synapses. He extracted two hearts from frogs and left them beating in an ionic bath. He stimulated the attached Vagus nerve of the first heart and observed its beating slowed. When the second heart was placed in the ionic bath of the first, it also slowed.[9]

In the 1920s,Edgar Adrian formulated the theory of neural communication that the frequency of action potentials, and not the size of the action potentials, was the basis for communicating the magnitude of the signal. His work was performed in an isolated frog nerve-muscle preparation. Adrian was awarded a Nobel Prize for his work.[10]

In the 1960sDavid Hubel andTorsten Wiesel demonstrated the macro columnar organization of visual areas in cats and monkeys, and provided physiological evidence for thecritical period for the development of disparity sensitivity in vision (i.e.: the main cue for depth perception), and were awarded a Nobel Prize for their work.

In 1996Dolly the sheep was born, the first mammal to becloned from an adult cell.[11] The process by which Dolly the sheep was cloned utilized a process known asnuclear transfer applied by lead scientistIan Wilmut. Although other scientists were not immediately able to replicate the experiment, Wilmut argued that the experiment was indeed repeatable, given a timeframe of over a year.[12]

In 1997, innovations in frogs,Xenopus laevis, by developmental biologist Jonathan Slack of theUniversity of Bath, created headless tadpoles, which could allow future applications in donor organ transplantation.[13]

There has been growing concern about both the methodology and the care of animals in laboratories who are used in testing. There is increasing emphasis on more humane and compassionate treatment of other animals.[14] Methodological concerns include factors that make animal study results less reproducible than intended. For example, a 2014 study fromMcGill University inMontreal, Canada suggests that mice handled by men rather than women showed higher stress levels.[15][16][17]

In medicine

[edit]
Early depictions of vivisection using pigs

In the 1880s and 1890s,Emil von Behring isolated thediphtheria toxin and demonstrated its effects in guinea pigs. He went on to demonstrate immunity against diphtheria in other animals in 1898 by injecting a mix of toxin and antitoxin. This work constituted in part the rationale for awarding von Behring the 1901 Nobel Prize in Physiology or Medicine. Roughly 15 years later, Behring announced such a mix suitable for human immunity which largely banished diphtheria from the scourges of humankind.[18] The antitoxin is famously commemorated each year in the Iditarod race, which is modeled after the Nome in the1925 serum run to Nome. The success of the animal studies in producing the diphtheria antitoxin are attributed by some as a cause of the decline of the early 20th century antivivisectionist movement in the USA.[19]

In 1921,Frederick Banting tied up the pancreatic ducts of dogs and discovered that the isolates of pancreatic secretion could be used to keep dogs with diabetes alive. He followed up these experiments with the chemical isolation ofinsulin in 1922 withJohn Macleod. These experiments used bovine sources instead of dogs to improve the supply. The first person treated wasLeonard Thompson, a 14-year-old diabetic who only weighed 65 pounds and was about to slip into a coma and die. After the first dose, the formulation had to be re-worked, a process that took 12 days. The second dose was effective.[20] These two won theNobel Prize in Physiology or Medicine in 1923 for their discovery of insulin and its treatment ofdiabetes mellitus. Thompson lived 13 more years taking insulin. Before insulin's clinical use, a diagnosis ofdiabetes mellitus meant death; Thompson had been diagnosed in 1919.[21]

In 1943,Selman Waksman's laboratory discoveredstreptomycin using a series of screens to find antibacterial substances from the soil. Waksman coined the termantibiotic with regards to these substances. Waksman would win the Nobel Prize in Physiology or Medicine in 1952 for his discoveries in antibiotics. Corwin Hinshaw and William Feldman took the streptomycin samples and curedtuberculosis in four guinea pigs with it. Hinshaw followed these studies with human trials that provided a dramatic advance in the ability to stop and reverse the progression of tuberculosis.[22][23] Mortality from tuberculosis in the UK has diminished from the early 20th century due to better hygiene and improved living standards, but from the moment antibiotics were introduced, the fall became steep so that by the 1980s mortality in developed countries was effectively zero.[24]

In the 1940s,Jonas Salk used rhesus monkey cross-contamination studies to isolate the three forms of thepolio virus that affected hundreds of thousands yearly.[25] Salk's team created a vaccine against the strains of polio in cell cultures of rhesus monkey kidney cells. The vaccine was made publicly available in 1955 and reduced the incidence of polio 15-fold in the USA over the following five years.[26]Albert Sabin made a superior "live" vaccine by passing the polio virus through animal hosts, including monkeys. The vaccine was produced for mass consumption in 1963 and is still in use today. It had virtually eradicated polio in the US by 1965.[27] It has been estimated that 100,000 rhesus monkeys were killed in the course of developing the polio vaccines, and 65 doses of vaccine were produced from each monkey. Writing in the Winston-Salem Journal in 1992, Sabin said, "Without the use of nonhuman animals and human (animals), it would have been impossible to acquire the important knowledge needed to prevent much suffering and premature death not only among humans but (other) animals as well."[28]

Also in the 1940s,John Cade tested lithium salts in guinea pigs in a search for pharmaceuticals with anticonvulsant properties. The nonhuman animals seemed calmer in their mood. He then tested lithium on himself, before using it to treat recurrent mania.[29] The introduction of lithium revolutionized the treatment of manic-depressives by the 1970s. Prior to Cade's animal testing, manic-depressives were treated with a lobotomy or electro-convulsive therapy.

In the 1950s the first safer, volatile anaesthetichalothane was developed through studies on rodents, rabbits, dogs, cats and monkeys.[30] This paved the way for a whole new generation of modern general anaesthetics – also developed by animal studies – without which modern, complex surgical operations would be virtually impossible.[31]

In 1960,Albert Starr pioneered heart valve replacement surgery in humans after a series of surgical advances in dogs.[32] He received the Lasker Medical Award in 2007 for his efforts, along withAlain Carpentier. In 1968 Carpentier made heart valve replacements from the heart valves of pigs, which are pre-treated with glutaraldehyd to blunt immune response. Over 300,000 people receive heart valve replacements derived from Starr and Carpentier's designs annually. Carpentier said of Starr's initial advances "Before his prosthetic, patients with valvular disease would die."[33]

In the 1970s,leprosy multi-drug antibiotic treatments were refined using leprosy bacteria grown inarmadillos and were then tested in human clinical trials. Today, thenine-banded armadillo is still used to culture the bacteria that causes leprosy, for studies of the proteomics and genomics (the genome was completed in 1998) of the bacteria, for improving therapy and developing vaccines. Leprosy is still prevalent in Brazil, Madagascar, Mozambique, Tanzania, India, and Nepal, with over 400,000 cases at the beginning of 2004.[34] The bacteria has not yet been culturedin vitro with success necessary to develop drug treatments or vaccines, and mice and armadillos have been the sources of the bacteria for research.[35]

The non-human primate models of AIDS, using HIV-2, SHIV, and SIV in macaques, have been used as a complement to ongoing research efforts against the virus. The drugtenofovir has had its efficacy and toxicology evaluated in macaques and found long-term/high-dose treatments had adverse effects not found using short-term/high-dose treatment followed by long-term/low-dose treatment. This finding in macaques was translated into human dosing regimens. Prophylactic treatment with anti-virals has been evaluated in macaques because an introduction of the virus can only be controlled in an animal model. The finding that prophylaxis can be effective at blocking infection has altered the treatment for occupational exposures, such as needle exposures. Such exposures are now followed rapidly with anti-HIV drugs, and this practice has resulted in measurable transient virus infection similar to theNHP model. Similarly, the mother-to-fetus transmission, and its fetal prophylaxis with antivirals such as tenofovir and AZT, has been evaluated in controlled testing in macaques not possible in humans, and this knowledge has guided antiviral treatment in pregnant mothers with HIV. "The comparison and correlation of results obtained in monkey and human studies are leading to a growing validation and recognition of the relevance of the animal model. Although each animal model has its limitations, carefully designed drug studies in nonhuman primates can continue to advance our scientific knowledge and guide future clinical trials."[36][37][38]

Throughout the 20th century, research that used live nonhuman animals has led to many other medical advances and treatments for human diseases, such as:organ transplant techniques and anti-transplant rejection medications,[39][40][41][42] the heart-lung machine,[43] antibiotics likepenicillin,[44] andwhooping cough vaccine.[45]

Presently, animal experimentation continues to be used in research that aims to solve medical problems includingAlzheimer's disease,[46]multiple sclerosis[47]spinal cord injury,[48] and many more conditions in which there is no usefulin vitro model system available.Currently, several options are available for animal-friendly testing, i.e methods that avoid physical and psychological suffering in the tested animals.[49][50]

Veterinary advances

[edit]
A veterinary surgeon at work with acat

Animal testing for veterinary studies accounts for around five percent of research using other animals. Treatments to each of the following animal diseases have been derived from animal studies:rabies,[51]anthrax,[51]glanders,[51]Feline immunodeficiency virus (FIV),[52]tuberculosis,[51] Texas cattle fever,[51]Classical swine fever (hog cholera),[51]Heartworm and other parasitic infections.[53]

Testing other animals for rabies do require the animal to be dead, and it takes two hours to conduct the test.[54]

Basic and applied research inveterinary medicine continues in varied topics, such as searching for improved treatments and vaccines forfeline leukemia virus and improvingveterinary oncology.

Early debate

[edit]
The ethical implications of using animals for testing has been a heated debate in regards to the humane treatment that is used.
Further information:Animal rights
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In 1655, physiologistEdmund O'Meara was recorded as saying that "the miserable torture of vivisection places the body in an unnatural state."[55][56] O'Meara thus expressed one of the chief scientific objections to vivisection: that the pain that the individual endured would interfere with the accuracy of the results.

In 1822, the firstanimal protection law was enacted in the British parliament, followed by theCruelty to Animals Act (1876), the first law specifically aimed at regulating animal testing. The legislation was promoted byCharles Darwin, who wrote toRay Lankester in March 1871:

You ask about my opinion on vivisection. I quite agree that it is justifiable for real investigations on physiology; but not for mere damnable and detestable curiosity. It is a subject which makes me sick with horror, so I will not say another word about it, else I shall not sleep to-night."[57][58]

Opposition to the use of nonhuman animals in medical research arose in the United States during the 1860s, whenHenry Bergh founded theAmerican Society for the Prevention of Cruelty to Animals (ASPCA), with America's first specifically anti-vivisection organization being the American AntiVivisection Society (AAVS), founded in 1883.

In the UK, an article in theMedical Times and Gazette on April 28, 1877, indicates that anti-vivisectionist campaigners, mainly clergymen, had prepared a number of posters entitled, "This is vivisection," "This is a living dog," and "This is a living rabbit," depicting nonhuman animals in a poses that they said copied the work ofElias von Cyon in St. Petersburg, though the article says the images differ from the originals. It states that no more than 10 or a dozen men were actively involved in animal testing on living nonhuman animals in the UK at that time.[59]

Antivivisectionists of the era believed the spread of mercy was the great cause of civilization, and vivisection was cruel. However, in the U.S., the antivivisectionists' efforts were defeated in every legislature because of the widespread support of an informed public for the careful and judicious use of other animals. The early antivivisectionist movement in the U.S. dwindled greatly in the 1920s. Overall, this movement had no US legislative success. The passing of the Laboratory Animal Welfare Act, in 1999 was more focused on protecting the welfare of other animals who are used in all fields, including research, food production, consumer product development, etc.[60][61]

On the other side of the debate, those in favor of nonhuman-animal testing held that experiments on other animals were necessary to advance medical and biological knowledge and to ensure the safety of products intended for human and animal use. In 1831, the founders of theDublin Zoo—the fourth oldest zoo in Europe, after Vienna, Paris, and London—were members of the medical profession, interested in studying the individuals both while they were alive and when they were dead.[62]Claude Bernard, known as the "prince of vivisectors"[63] and the father of physiology—whose wife,Marie Françoise Martin, founded the first anti-vivisection society in France in 1883[64]—famously wrote in 1865 that "the science of life is a superb and dazzlingly lighted hall which may be reached only by passing through a long and ghastly kitchen."[65] Arguing that "experiments on (nonhuman) animals...are entirely conclusive for the toxicology and hygiene of man...the effects of these substances are the same on man as on (other) animals, save for differences in degree,"[66] Bernard established animal experimentation as part of the standardscientific method.[67] In 1896, the physiologist and physicianDr. Walter B. Cannon said "The antivivisectionists are the second of the two types Theodore Roosevelt described when he said, 'Common sense without conscience may lead to crime, but conscience without common sense may lead to folly, which is the handmaiden of crime.'"[60] These divisions between pro- and anti- animal testing groups first came to public attention during thebrown dog affair in the early 20th century, when hundreds of medical students clashed with anti-vivisectionists and police over a memorial to a vivisected dog.[68]

See also

[edit]

Notes

[edit]
  1. ^Cohen and Loew 1984.
  2. ^"History of nonhuman animal research"Archived 2006-10-13 at theWayback Machine, Laboratory Primate Advocacy Group.
  3. ^Abdel-Halim, Rabie E. (September 2005). "Contributions of Ibn Zuhr (Avenzoar) to the progress of surgery: a study and translations from his book Al-Taisir".Saudi Med J.26 (9):1333–9.PMID 16155644.
  4. ^Abdel-Halim, Rabie E. (2006). "Contributions of Muhadhdhab Al-Deen Al-Baghdadi to the progress of medicine and urology".Saudi Medical Journal.27 (11):161–1641.PMID 17106533.
  5. ^Ramirez Rozzi, Fernando; Froment, Alain (2018-04-19)."Earliest Animal Cranial Surgery: from Cow to Man in the Neolithic".Scientific Reports.8 (1): 5536.Bibcode:2018NatSR...8.5536R.doi:10.1038/s41598-018-23914-1.ISSN 2045-2322.PMC 5908843.PMID 29674628.
  6. ^West, J.B. (2005). "Robert Boyle's landmark book of 1660 with the first experiments on rarified air".Journal of Applied Physiology.98 (1):31–39.doi:10.1152/japplphysiol.00759.2004.PMID 15591301.S2CID 5837786.
  7. ^Boyle, Robert (2003) [1744].Works of the Honorable Robert Boyle. Kessinger Publishing. p. 740.ISBN 978-0-7661-6865-7.
  8. ^abc"Antoine Lavoisier – Biography, Facts and Pictures".www.famousscientists.org. Retrieved2016-08-07.
  9. ^[1][dead link] O. Loewi (1921) "Uber humorale Ubertragbarkeit der Herznervenwirkung. I."Pflügers Archiv, 189, pp. 239-242
  10. ^[2] Adrian Nobel Prize
  11. ^"Cloning Dolly the sheep | Animal Research". Archived fromthe original on 2013-06-07. Retrieved2012-11-21., AnimalResearch.Info Dolly the Sheep
  12. ^"Dolly the Sheep Was a Clone, Edinburgh Scientist Maintains".BMJ: British Medical Journal.316 (7131): 573. 1998.JSTOR 25178321.
  13. ^Morton, Oliver; Williams, Nigel (1997). "First Dolly, Now Headless Tadpoles".Science.278 (5339): 798.doi:10.1126/science.278.5339.798.JSTOR 2894431.PMID 9381189.S2CID 23144947.
  14. ^Mcmillan, Franklin D. (2012). "What Dictionary Are Animal Researchers Using?".Journal of Animal Ethics.2 (1):1–5.doi:10.5406/janimalethics.2.1.0001.JSTOR 10.5406/janimalethics.2.1.0001.
  15. ^"The world's favourite lab animal has been found wanting, but there are new twists in the mouse's tale".The Economist. 2016-12-24. Retrieved2017-01-10.
  16. ^Katsnelson, Alla (2014)."Male researchers stress out rodents".Nature.doi:10.1038/nature.2014.15106.S2CID 87534627.
  17. ^"Male Scent May Compromise Biomedical Research".Science | AAAS. 2014-04-28. Retrieved2017-01-10.
  18. ^"Emil von Behring – Biographical".
  19. ^Walter B. Cannon Papers, American Philosophical SocietyArchived 2009-08-14 at theWayback Machine
  20. ^Discovery of InsulinArchived 2009-09-30 at theWayback Machine
  21. ^"Leonard Thompson Bio Page". Archived fromthe original on 2009-02-10.
  22. ^[3] Hinshaw obituary
  23. ^[4] Streptomycin
  24. ^Is Science Necessary
    Author: Max Perutz
    Page: 37-41
    Published 1989
    Publisher E.P. Dutton/NAL Penguin Inc
    ISBN 0-525-24673-8
  25. ^[5] Virus-typing of polio by Salk
  26. ^[6] Salk polio virus
  27. ^[7]Archived 2011-06-04 at theWayback Machine History of polio vaccine
  28. ^""the work on [polio] prevention was long delayed by... misleading experimental models of the disease in monkeys" - ari.info".
  29. ^Ironside, Wallace (1993)."John Frederick Joseph Cade (1912–1980)".Australian Dictionary of Biography. Vol. 13. National Centre of Biography,Australian National University.ISBN 978-0-522-84459-7.ISSN 1833-7538.OCLC 70677943. Retrieved19 August 2025.
  30. ^Raventos J (1956)Br J Pharmacol 11, 394
  31. ^Whalen FX, Bacon DR & Smith HM (2005)Best Pract Res Clin Anaesthesiol 19, 323
  32. ^"Portland surgeon receives top medical prize".The Oregonian. 15 September 2007.
  33. ^"2007 Lasker Awards announced – The Scientist Magazine®". Archived fromthe original on 2011-01-21. Retrieved2007-09-16.
  34. ^"Home – spectroscopyNOW.com".
  35. ^"Armadillos in Research".
  36. ^AIDS Reviews 2005;7:67-83 Antiretroviral Drug Studies in Nonhuman Primates: a Valid Animal Model for Innovative Drug Efficacy and Pathogenesis ExperimentsArchived 2008-12-17 at theWayback Machine
  37. ^"PMPA: Experimental Drug That Completely Protects Monkeys Exposed To SIV".
  38. ^"Medical Roundup".
  39. ^Carrel A (1912)Surg. Gynec. Obst. 14: p. 246
  40. ^Williamson C (1926)J. Urol. 16: p. 231
  41. ^Woodruff H & Burg R (1986) inDiscoveries in Pharmacology vol 3, ed Parnham & Bruinvels, Elsevier, Amsterdam
  42. ^Moore F (1964)Give and Take: the Development of Tissue Transplantation. Saunders, New York
  43. ^Gibbon JH (1937)Arch. Surg. 34, 1105
  44. ^Fleming A (1929)Br J Exp Pathol 10, 226
  45. ^Medical Research Council (1956)Br. Med. J. 2: p. 454
  46. ^Geula, C; Wu C-K, Saroff D; Lorenzo, A; Yuan, M; Yankner, BA; Yankner, Bruce A. (1998). "Aging renders the brain vulnerable to amyloid β protein neurotoxicity".Nature Medicine.4 (7):827–31.doi:10.1038/nm0798-827.PMID 9662375.S2CID 45108486.
  47. ^Jameson, BA; McDonnell, JM; Marini, JC; Korngold, R (1994). "A rationally designed CD4 analogue inhibits experimental allergic encephalomyelitis".Nature.368 (6473):744–6.Bibcode:1994Natur.368..744J.doi:10.1038/368744a0.PMID 8152486.S2CID 4370797.
  48. ^Lyuksyutova, AL; Lu C-C, Milanesio N; Milanesio, N; King, LA; Guo, N; Wang, Y; Nathans, J; Tessier-Lavigne, M; et al. (2003). "Anterior-posterior guidance of commissural axons by Wnt-Frizzled signaling".Science.302 (5652):1984–8.Bibcode:2003Sci...302.1984L.doi:10.1126/science.1089610.PMID 14671310.S2CID 39309990.
  49. ^d'Isa R, Gerlai R (January 2023)."Designing animal-friendly behavioral tests for neuroscience research: The importance of an ethological approach".Frontiers in Behavioral Neuroscience.16 1090248.doi:10.3389/fnbeh.2022.1090248.PMC 9871504.PMID 36703720.
  50. ^d'Isa R, Fasano S, Brambilla R (June 2024)."Editorial: Animal-friendly methods for rodent behavioral testing in neuroscience research".Frontiers in Behavioral Neuroscience.18 1431310.doi:10.3389/fnbeh.2024.1431310.PMC 11232432.PMID 38983871.
  51. ^abcdefA reference handbook of the medical sciences. William Wood and Co., 1904, Edited by Albert H. Buck.
  52. ^Pu, R; Coleman, J; Coisman, J; Sato, E; Tanabe, T; Arai, M; Yamamoto, JK (2005)."Dual-subtype FIV vaccine (Fel-O-Vax FIV) protection against a heterologous subtype B FIV isolate".Journal of Feline Medicine and Surgery.7 (1):65–70.doi:10.1016/j.jfms.2004.08.005.PMC 10911555.PMID 15686976.S2CID 26525327.
  53. ^Dryden, MW; Payne, PA (2005). "Preventing parasites in cats".Veterinary Therapeutics: Research in Applied Veterinary Medicine.6 (3):260–7.PMID 16299672.
  54. ^"Diagnosis in Animals and Humans".Centers for Disease Control and Prevention. 2011-09-20. Retrieved2016-07-31.
  55. ^Ryder, Richard D.Animal Revolution: Changing Attitudes Towards Speciesism. Berg Publishers, 2000, p. 54.
  56. ^"Animal Experimentation: A Student Guide to Balancing the Issues"Archived 2009-03-27 at theWayback Machine, Australian and New Zealand Council for the Care of Animals in Research and Teaching (ANZCCART), retrieved December 12, 2007, cites original reference in Maehle, A-H. and Tr6hler, U. 1987. Animal experimentation from antiquity to the end of the eighteenth century: attitudes and arguments. In N. A. Rupke (ed.) Vivisection in Historical Perspective. Croom Helm, London, p. 22
  57. ^The Life and Letters of Charles Darwin, Volume II,fulltextarchive.com.
  58. ^Bowlby, John.Charles Darwin: A New Life, W. W. Norton & Company, 1991. p. 420.
  59. ^The Latest Phase of the Vivisection Question,Medical Times and Gazette, April 28, 1877, pp. 446–447.
  60. ^abThe Physiologist at the-aps.org A Physiologist's Views on the Animal Rights/Liberation MovementArchived 2008-05-30 at theWayback Machine by Charles S. NicollThe Physiologist 34(6): Dec 1991
  61. ^Buettinger, CraigAntivivisection and the charge of zoophil-psychosis in the early twentieth century.The Historian 1993
  62. ^Costello, John (9 June 2011)."The great zoo's who".Irish Independent.
  63. ^Croce, Pietro.Vivisection or Science? An Investigation into Testing Drugs and Safeguarding Health. Zed Books, 1999, p. 11.
  64. ^Rudacille, Deborah.The Scalpel and the Butterfly: The Conflict, Farrar Straus Giroux, 2000, p. 19.
  65. ^"In sickness and in health: vivisection's undoing",The Daily Telegraph, November 2003.
  66. ^Bernard, ClaudeAn Introduction to the Study of Experimental Medicine, 1865. First English translation by Henry Copley Greene, published by Macmillan & Co., Ltd., 1927; reprinted in 1949, p125
  67. ^LaFollette, H., Shanks, N., Animal Experimentation: the Legacy of Claude Bernard,International Studies in the Philosophy of Science (1994) pp. 195-210.
  68. ^Mason, Peter.The Brown Dog AffairArchived 2020-10-06 at theWayback Machine. Two Sevens Publishing, 1997.
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