Difference between revisions of "Timeline of antibiotics"
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| 1997 || Resistance || {{w|Vancomycin}}-resistant {{w|staphyloccocus}} is reported.<ref name="Antibiotics armageddon?"/> || | | 1997 || Resistance || {{w|Vancomycin}}-resistant {{w|staphyloccocus}} is reported.<ref name="Antibiotics armageddon?"/> || | ||
|- | |- | ||
− | | 1999 || Introduction || Antibiotic {{w|quinupristin/dalfopristin}} is introduced.<ref name="Oxford Handbook of Infectious Diseases and Microbiology"/> || | + | | 1999 || Introduction || Antibiotic {{w|quinupristin/dalfopristin}} is introduced.<ref name="Oxford Handbook of Infectious Diseases and Microbiology"/> The combination is used to treat {{w|infection}}s by [[w:staphylococcus|staphylococci]] and by {{w|vancomycin}}-resistant ''[[w:Enterococcus|Enterococcus faecium]]''.|| |
|- | |- | ||
| 2000 || Introduction || {{w|Oxazolidinones}} are introduced.<ref name="Antibiotics armageddon?"/> These synthetic drugs are active against a large spectrum of Gram-positive bacteria, including methicillin- and vancomycin-resistant staphylococci, vancomycin-resistant enterococci, penicillin-resistant pneumococci and anaerobes.<ref>{{cite journal|last1=Bozdogan|first1=B|last2=Appelbaum|first2=PC.|title=Oxazolidinones: activity, mode of action, and mechanism of resistance.|doi=10.1016/j.ijantimicag.2003.11.003|pmid=15013035|url=https://www.ncbi.nlm.nih.gov/pubmed/15013035}}</ref> || | | 2000 || Introduction || {{w|Oxazolidinones}} are introduced.<ref name="Antibiotics armageddon?"/> These synthetic drugs are active against a large spectrum of Gram-positive bacteria, including methicillin- and vancomycin-resistant staphylococci, vancomycin-resistant enterococci, penicillin-resistant pneumococci and anaerobes.<ref>{{cite journal|last1=Bozdogan|first1=B|last2=Appelbaum|first2=PC.|title=Oxazolidinones: activity, mode of action, and mechanism of resistance.|doi=10.1016/j.ijantimicag.2003.11.003|pmid=15013035|url=https://www.ncbi.nlm.nih.gov/pubmed/15013035}}</ref> || |
Revision as of 09:16, 13 May 2018
This is a timeline of antibiotics, mainly focusing on both the introduction of drugs and first reported drug resistances. For historic events focusing on bacteria, visit Timeline of bacteriology.
Contents
Big picture
Time period | Development summary |
---|---|
<19th century | Although people did not know infections were caused by bacteria, antibiotics have been used for millennia to treat infections. Some of the earliest civilizations used various molds and plant extracts for treatment. The ancient Egyptians, for example, applied mouldy bread to infected wounds.[1] |
19th century | Scientists begin to observe antibacterial chemicals in action.[1] By the late century, a few notable breakthroughs occur. |
20th century | Antibiotics revolutionize medicine during the later half of the 20th century.[2] The major event in the history of antibiotics is the discovery of penicillin by Alexander Fleming in 1928. The first antibiotics are prescribed in the late 1930s.[3] The period between the 1950s and 1970s is considered the golden era of discovery of novel antibiotics classes, with no new classes discovered since then.[4] In fact, between 1944 and 1972 human life expectancy jumps by eight years, largely due to the introduction of antibiotics.[3] In the 1970s and 1980s synthetic versions of erythromycin, including clarithromycin and azithromycin, are developed.[5] After the 1970s, with the decline of the discovery rate, the mainstream approach for the development of new drugs to combat emerging and re-emerging resistance of pathogens to antibiotics would be the modification of existing antibiotics.[4] By the 1980s and 1990s, scientists only manage to make improvements within classes.[6] |
Full timeline
Year | Event type | Details | Geographical location |
---|---|---|---|
350 CE–550 CE | Traces of tetracycline are found in human skeletal remains from ancient Sudanese Nubia.[4][2] | ||
1877 | Scientific development | French microbiologist Louis Pasteur shows that the bacterial disease anthrax can be rendered harmless in animals with the injection of soil bacteria.[7][8] | France |
1887 | Scientific development | German bacteriologist Rudolf Emmerich shows that the intestinal infection cholera is prevented in animals that have been previously infected with the streptococcus bacterium and then injected with the cholera bacillus.[9] | |
1888 | Isolation | German scientist E. de Freudenreich manages to isolate an actual product from a bacterium that had antibacterial properties.[10] | |
1896 | Scientific development | French medical student Ernest Duchesne originally discovers the antibiotic properties of Penicillium.[11][12][13] | |
1907 | Scientific development | German chemist Alfred Bertheim and Paul Ehrlich discover arsenic-derived synthetic antibiotics. This marks the beginning of the era of antibacterial treatment.[14] | |
1909 | Introduction | Japanese bacteriologist Sahachiro Hata discovers the antisyphilitic activity of arsphenamine.[1][15] | |
1912 | Introduction | Paul Ehrlich discovers Neosalvarsan, a synthetic chemotherapeutic.[16] | |
1928 | Introduction | Scottish microbiologist Alexander Fleming, a Professor of Bacteriology at St Mary’s Hospital in London, discovers penicillin after sorting through some petri dishes containing a bacteria called staphylococcus, which causes boils, sore throats and abscesses. Flemming discovers killed baceria in one dish contaning a blob of mold on it.[10][5] | United Kingdom |
1930 | Isolation | French-born American microbiologist René Dubos isolates from a soil microorganism an enzyme that can decompose part of the bacillum that causes lobar pneumonia in humans.[17] | |
1932 | Introduction | German pathologist Gerhard Domagk develops prontosil, the first sulphonamide microbial.[18][19][20] | Germany |
1936 | Introduction | Sulfonamide antibacterial sulfanilamide is introduced in the United States and is immediately established as a powerful antiinfective agent.[21] | United States |
1937 | Introduction | The first effective antimicrobials (sulfonamides) are introduced.[22] | |
1938 | Introduction | Sulfapyridine is introduced for clinical use for the treatment of pneumococcic pneumonia.[23][24] Today it is used to help control dermatitis herpetiformis (Duhring's disease), a skin problem.[25] | |
1939 | Isolation | Microbiologist René Dubos manages to isolate an antibacterial substance and names it tyrothricin.[17] | |
1939 | Introduction | Gramicidin A is discovered from the soil bacterium bacillus brevis, and becomes the first clinically useful topical antibiotic.[26][27][28] | |
1939 | Scientific development | Australian pharmacologist Howard Florey and Ernst Boris Chain manage to elucidate the structure of penicillin G, the first penicillin used in therapy.[29][30][31] | |
1939 | Introduction | Sulfonamide antibiotic sulfacetamide is first reported in the treatment of diseases of the eye.[32][33] Today it is used to treat bacterial eye infections, such as conjunctivitis.[34] | |
1940 | Introduction | Sulfonamide antibiotic sulfamethizole is introduced and marketed as a single compound for the treatment of urinary tract infections.[35][36][37] | |
1941 | Introduction | β-lactam antibiotics enter initial clinical trials. In time, they would become the most widely produced and used antibacterial drugs in the world.[38][39] β-lactam antibiotics now the most economically important of all the groups of antimicrobials.[40] | |
1941 | Introduction | Penicillin is introduced for medical use.[41][20] Just before the introduction of penicillin, the mortality rate from Staphylococcus aureus infections that had reached the blood stream was reported to be 80%.[41] | |
1942 | Introduction | Sulfadimidine is introduced for the treatment of bacterial infections.[42][43][44][45] | |
1942 | Resistance | Penicillin resistant bacteria are first detected, about one year after the introduction of penicillin.[41] | |
1942 | Isolation | Gramicidin S, the first peptide antibiotic, is isolated by Gauze and Brazhnikova.[46][47][48] | |
1943 | Introduction | American biochemists Selman Waksman, Albert Schatz, and Elizabeth Bugie discover antibiotic streptomycin, the first aminoglycoside. It is the first antibiotic effective against tuberculosis.[5][49][50][51][20] | United States |
1943 | Introduction | Sulfamerazine is synthesized by American chemists.[52] The drug is today used as an antibacterial agent.[53][54][55][56] | United States |
1943 | Production | Penicillin is mass produced and used heavily to treat Allied troops fighting in Europe during World War II.[2] | |
1943 | Isolation | Bacitracin is first isolated.[57][58] The drug is used to prevent minor skin infections caused by small cuts, scrapes, or burns.[59] | |
1945 | Discovery | The cephalosporins are discovered from a fungus, Cephalosporium acremonium, in seawater samples near a sewage outfall in Sardinia.[20][60][61][62] | Italy |
1947 | Isolation | Chloramphenicol is isolated from the soil organism Streptomyces venezuelae. Merketed in 1949, its use would quickly become widespread due to its broad spectrum of antimicrobial activity.[63][64][65][66] | |
1947 | Isolation | American plant physiologist Benjamin Minge Duggar isolates chlortetracycline from a Missouri River mud sample. It is the first tetracycline introduced.[67][68][69][70] | United States |
1947 | Isolation | The polymyxin family of antibiotics is discovered, with polymyxin B being the first isolated from bacterium paenibacillus polymyxa.[5][71][72] | |
1947 | Introduction | Drug class Nitrofuran is introduced.[38] Nitrofurans are synthetic chemotherapeutic agents with a broad antimicrobial spectrum, active against both gram-positive and gram-negative bacteria, including salmonella and Giardia spp, trichomonads, amebae, and some coccidial species.[73] | |
1949 | Isolation | Jewish-American biochemist Selman Waksman and Hubert A. Lechevalier first isolates neomycin, as aminoglycoside antibiotic found in many topical medications such as creams, ointments, and eyedrops.[74][75][76] | United States |
1949 | Scientific development | British chemist Dorothy Hodgkin reveals the complete structure of molecular penicillin, using the X-ray crystallography.[22] | United Kingdom |
1950 | Introduction | Oxytetracycline comes into commercial use.[58][77][78] Since then, this antibiotic would be used widely in human and veterinary medicine.[79] | |
1950 | Resistance | Resistance against chloramphenicol is observed.[80] | |
1952 | Introduction | Lincosamides are introduced.[38] A small group of agents with a novel structure unlike that of any other antibiotic, lincosamides are widely active against Gram-positive bacteria and most anaerobes, with the exception of Gram-negative aerobes. Lincosamides are also active against some mycoplasmas and protozoa.[81] | |
1952 | Introduction | Antibiotic thiamphenicol is first synthesized.[82] It is a broad spectrum antibiotic with good activity against Gram negative and anaerobic bacteria.[83] | |
1952 | Introduction | Eli Lilly and Company introduces erythromycin, an antibiotic useful for the treatment of a number of bacterial infections, including respiratory tract infections, skin infections, chlamydia infections, pelvic inflammatory disease, and syphilis.[84][85][86] Erythromycin is the first macrolide antibiotic.[87] | United States |
1952 | Introduction | Streptogramins are introduced. Streptogramins are effective in the treatment of vancomycin-resistant Staphylococcus aureus (VRSA) and vancomycin-resistant Enterococcus (VRE), two of the most rapidly growing strains of multidrug-resistant bacteria.[38] | |
1953 | Introduction | Oxford University scientists discover antibiotic cephalosporin C, from which cephalosporins later develop. Like penicillins, cephalosporins inhibit cell wall synthesis by preventing cross-linking of peptidoglycan.[88][5] | United Kingdom |
1953 | Resistance | Macrolide resistance is observed.[38] | |
1954 | Introduction | Benzathine penicillin is established as a method for the treatment of syphilis.[89] | |
1955 | Introduction | Macrolide antibiotic spiramycin is first introduced into the French market.[90] Spiramycin is used to treat various infections.[91] | France |
1956 | Isolation | Research team at the Lilly Biological Laboratories in Indiana first isolates vancomycin from bacterium streplomyces orienlalis. Vancomycin is used as a treatment for complicated skin infections, bloodstream infections, endocarditis, bone and joint infections, and meningitis caused by methicillin-resistant staphylococcus aureus.[20][92][93][94] | United States |
1956 | Resistance | Resistance against erythromycin is observed.[80] | |
1957 | Introduction | Kanamycin is discovered. It is used to treat severe bacterial infections and tuberculosis.[58] | |
1957 | Introduction | Ansamycins are introduced. These bacterial secondary metabolites show antimicrobial activity against many Gram-positive and some Gram-negative bacteria.[38] | |
1959 | Introduction | Colistin becomes available for treating infections caused by gram-negative bacteria.[5] | |
1959 | Introduction | Nitroimidazoles are introduced. They are effective bactericidal agents against anaerobes and protozoa.[38] | |
1960 | Introduction | In an attempt to defeat penicillin-resistant strains, scientists develop methicillin, a different antibiotic in the penicillin class.[2][80] | |
1961 | Resistance | Methicillin resistance is first reported.[41][80][38] | |
1961 | Introduction | Antibiotic ampicillin is introduced. Within a short time it would become the drug of choice for treatment of Hemophilus influenzae meningitis.[95][96][97][20] | |
1961 | Resistance | Methicillin-resistant staphylococcus aureus is first reported in the United Kingdom, just a year after the antibiotic methicillin was introduced in the country.[5] | |
1961 | Discovery | Spectinomycin is first reported. Today it is used for the treatment of gonorrhea infections.[98][58] | |
1962 | Introduction | Quinolones are discovered accidentally, as a byproduct of some research on the antimalarial drug chloroquine.[5][38] | |
1963 | Isolation | Weinstein and his colleagues from the Schering Corporation describe the first isolation of the gentamicin complex.[20][99][100][101] | United States |
1963 | Introduction | Gentamicin is discovered. It is used to treat several types of bacterial infections.[58] | |
1963 | Resistance | Gram-negative bacterium acinetobacter baumannii becomes an antibiotic resistant pathogen.[41] | |
1965 | Introduction | Antibiotic Cloxacillin synthesized. Today it is useful for the treatment of a number of bacterial infections,[102] including impetigo, cellulitis, pneumonia, septic arthritis, and otitis externa.[102] It is used by mouth and by injection.[102].[103][104][105] | |
1966 | Resistance | Nalidixic acid resistance is observed.[38] | |
1966 | Synthesis | Antibiotic doxycycline is synthesized.[106][107][108] Today it is used for bacterial pneumonia, acne, {{w|chlamydia infection}s, early Lyme disease, cholera and syphilis.[109] | |
1966 | Resistance | Resistance against cephalotin is observed.[80] | |
1967 | Introduction | Clindamycin is first produced. Today it is used for the treatment of a number of bacterial infections.[58] | |
1968 | Introduction | Antibiotic rifampicin is introduced for clinical use.[110][111][112] The introduction of rifampicin would greatly shorten the duration of tuberculosis chemotherapy.[113] | Italy |
1968 | Resistance | Tetracycline resistance is observed.[38][38] | |
1968 | Introduction | Trimethoprim is introduced. It is used mainly in the treatment of bladder infections.[38] | |
1970 | Introduction | Non-toxic semi-synthetic acid-resistant isoxazolyl penicillin flucloxacillin is introduced into clinical practice.[105][114] | |
1971 | Introduction | Aminoglycoside antibiotic Tobramycin is discovered. It is used to treat various types of bacterial infections, particularly Gram-negative infections.[58] | |
1972 | Isolation | Extracellular broad spectrum beta-lactam antibiotic cephamycin C is first isolated.[115][58] | |
1972 | Introduction | Antibiotic minocycline is discovered.[106][107][108] It has both antibacterial and anti-inflammatory properties. Minocycline is used for a variety of infectious diseases and in acne.[116] | |
1973 | Introduction | Bactericidal antibiotic Carbenicillin is discovered. It belongs to the carboxypenicillin subgroup of the penicillins.[117] Carbenicillin has bactericidal and beta-lactamase resistant activity.[118] | |
1974 | Introduction | Antibiotic trimethoprim/sulfamethoxazole is commercially released.[119][20] | |
1974 | Introduction | Cotrimoxazole is introduced.[58] It is used to treat certain bacterial infections, such as pneumonia, bronchitis, and infections of the urinary tract, ears, and intestines. Cotrimoxazole also is used to treat 'travelers' diarrhea.[120] | |
1976 | Introduction | The Bristol-Banyu research institute in Japan publishes the discovery of antibiotic amikacin.[20][58][121] Amikacin is active against a broad spectrum of Gram-negative organisms, including pseudomonas, Escherichia coli and some Gram-positive organisms, like Staphylococcus aureus.[122] | Japan |
1976 | Resistance | Tufts University researcher Stuart B. Levy becomes one of the first to identify antibiotic resistance due to their use in animals.[2] | |
1978 | Introduction | Cefoxitin is introduced as an early cephamycin.[117][123] It is synthesized in order to create an antibiotic with a broader spectrum.[124] | |
1978 | Discovery | The teicoplanin family of glycopeptides is discovered.[125] Teicoplanin is used in the prophylaxis and treatment of serious infections caused by Gram-positive bacteria, including methicillin-resistant Staphylococcus aureus and Enterococcus faecalis.[126] | |
1979 | Introduction | Eli Lilly patents antibiotic cefaclor.[127][128][129] It is used to treat certain bacterial infections such as pneumonia and infections of the ear, lung, skin, throat, and urinary tract. | United States |
1981 | Resistance | AmpC beta-lactamase resistance is observed.[38] | |
1981 | Discovery | Researchers at Bayer discover ciprofloxacin, the first fluoroquinolone. Ciproloxacin is used to treat bone and joint infections, intra abdominal infections, certain type of infectious diarrhea, respiratory tract infections, skin infections, typhoid fever, and urinary tract infections, among others.[130] | |
1983 | Resistance | Extended-spectrum-beta-lactamase resistance is observed.[38] | |
1984 | Introduction | amoxicillin clavulanate is introduced.[58] It is specifically used for otitis media, strep throat, pneumonia, cellulitis, urinary tract infections, animal bites, and tuberculosis.[131] | |
1985 | Introduction | Researchers at Eli Lilly and Company discover antibiotic daptomycin.[132][133][134] | United States |
1985 | Introduction | Carbapenems are introduced.[80] These are commonly used for the treatment of severe or high-risk bacterial infections. | |
1986 | Resistance | Vancomycin-resistant enterococcus is reported.[80][38] | |
1987 | Introduction | Antibiotic imipenem/cilastin is introduced.[20] It is useful for the treatment of pneumonia, sepsis, endocarditis, joint infections, intra-abdominal infections, and urinary tract infections.[135] | |
1987 | Introduction | Highly potent fluoroquinolones are introduced.[22] These are used to treat a variety of illnesses such as respiratory and urinary tract infections.[136] | |
1987 | Resistance | Resistance against cephalosporins is observed.[80] | |
1987 | Resistance | Resistance against carbapenems is observed.[80] | |
1990s | Resistance | Fluorochinolone resistance is observed.[38] | |
1993 | Introduction | Antibiotic azithromycin is introduced.[20] It is used to treat certain bacterial infections, such as bronchitis, pneumonia, sexually transmitted diseases (STD), and infections of the ears, lungs, sinuses, skin, throat, and reproductive organs.[137] | |
1993 | Introduction | Antibiotic clarithromycin is introduced.[20] It is used to prevent and treat certain infections caused by bacteria.[138] | |
1997 | Resistance | Vancomycin-resistant staphyloccocus is reported.[38] | |
1999 | Introduction | Antibiotic quinupristin/dalfopristin is introduced.[20] The combination is used to treat infections by staphylococci and by vancomycin-resistant Enterococcus faecium. | |
2000 | Introduction | Oxazolidinones are introduced.[38] These synthetic drugs are active against a large spectrum of Gram-positive bacteria, including methicillin- and vancomycin-resistant staphylococci, vancomycin-resistant enterococci, penicillin-resistant pneumococci and anaerobes.[139] | |
2000 | Introduction | Antibiotic linezolid is introduced for the treatment of infections caused by gram-positive bacteria that are resistant to other antibiotics.[20][80] An oxazolidinone antibiotic, linezolid represents the first principally new antibiotic platform that has entered medical practice in more than 30 years.[140][38] | |
2001 | Introduction | Antibiotic telithromycin is introduced in the European Union.[141][142][143] It is used to treat certain types of pneumonia.[144] | |
2001 | Introduction | Broader-spectrum fluoroquinolones are introduced.[117] | |
2002 | Resistance | Resistance against linezolid is observed.[80] | |
2002 | Introduction | The United States Food and Drug Administration approves cefditoren, pivoxil and ertapenem. [145][58] | |
2002 | Resistance | Vancomycin-resistant staphylococcus aureus is reported.[38] | |
2003 | Introduction | Lipopeptides are introduced as antibiotics.[38] | |
2003 | Introduction | Daptomycin is introduced for treatment of systemic and life-threatening infections caused by Gram-positive organisms.[20] | |
2004 | Introduction | Telythromicin is introduced.[58] It is used to treat certain types of pneumonia.[146] | |
2005 | Introduction | Antibiotic tigecycline is introduced for the treatment of skin and skin structure infections and intraabdominal infections.[147][148][149] | |
2010 | Publication | Authors of a report on the evolution of resistance note that microbes have “extraordinary genetic capabilities” that benefit “from man’s overuse of antibiotics to exploit every source of resistance genes... to develop [resistance] for each and every antibiotic introduced into practice clinically, agriculturally, or otherwise.”[2] | |
2011 | Introduction | The United States Food and Drug Administration approves fidaxomicin for treatment of clostridium Difficile Infection.[150][151] | United States |
2012 | Study | A team of scientists propose adding the terms extensively drug-resistant (XDR) and pandrug-resistant (PDR) to multidrug-resistant (MDR) bacteria to better help them classify and potentially defeat superbugs.[2] | |
2012 | Introduction | The United States Food and Drug Administration approves bedaquiline for the treatment of multidrug-resistant tuberculosis.[152][153] | United States |
2013 | Introduction | The United States Food and Drug Administration approves telavancin for the treatment of hospital-acquired pneumonia caused by susceptible staphylococcus aureus.[154][155][156] | United States |
2014 | Declaration | The World Health Organization (WHO) releases a statement in response to major superbug outbreaks like lebsiella pneumoniae (which causes pneumonia and bloodstream infections in the hospital) and gonorrhea strains all over the world, noting that “this serious threat is no longer a prediction for the future, it is happening right now in every region of the world and has the potential to affect anyone, of any age, in any country.”[2] | |
2014 | Introduction | The United States Food and Drug Administration approves four new antibacterial agents, dalbavancin, oritavancin, tedizolid for skin infections, and ceftolozane/tazobactam for complicated intra‐abdominal and urinary tract infections.[157] | United States |
2015 | Policy | American fast food company McDonald's announces that it would phase out all meat sources that contain antibiotics.[2] | |
2015 | Introduction | Ceftazidime/avibactam is introduced for use in the United States.[158][159][160] The combination is used for treatment against certain multidrug-resistant Gram-negative infections. | United States |
2018 | Introduction | The discovery of malacidins is published.[161] The novel antibiotic can work against many of the multidrug-resistant bacterial strains.[162] |
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References
- ↑ 1.0 1.1 1.2 "THE HISTORY OF ANTIBIOTICS". microbiologysociety.org. Retrieved 29 March 2018.
- ↑ 2.0 2.1 2.2 2.3 2.4 2.5 2.6 2.7 2.8 "A Brief History Of Antibiotic Resistance: How A Medical Miracle Turned Into The Biggest Public Health Danger Of Our Time". medicaldaily.com. Retrieved 29 March 2018.
- ↑ 3.0 3.1 "antibiotics 1928-2000". abc.net.au. Retrieved 31 March 2018.
- ↑ 4.0 4.1 4.2 Aminov, Rustam I. "A Brief History of the Antibiotic Era: Lessons Learned and Challenges for the Future". PMC 3109405. PMID 21687759. doi:10.3389/fmicb.2010.00134.
- ↑ 5.0 5.1 5.2 5.3 5.4 5.5 5.6 5.7 "Ten important moments in the history of antibiotic discovery". correctiv.org. Retrieved 29 March 2018.
- ↑ "A brief history of antibiotics". news.bbc.co.uk. Retrieved 30 March 2018.
- ↑ Tierno, Philip M. The Secret Life of Germs: What They Are, Why We Need Them, and How We Can Protect Ourselves Against Them.
- ↑ Williams, Elizabeth S.; Barker, Ian K. Infectious Diseases of Wild Mammals.
- ↑ Newell-McGloughlin, Martina; Re, Edward. The Evolution of Biotechnology: From Natufians to Nanotechnology.
- ↑ 10.0 10.1 Newell-McGloughlin, Martina; Re, Edward. The Evolution of Biotechnology: From Natufians to Nanotechnology.
- ↑ Zhang, Yawei. Encyclopedia of Global Health, Volume 1.
- ↑ Myers, Richard L. The 100 Most Important Chemical Compounds: A Reference Guide.
- ↑ Manning, Shannon D.; Alcamo, I. Edward; Heymann, David L. Escherichia Coli Infections.
- ↑ SWATHY, S; ARYA, US. "ANTIBIOTIC USAGE IN PEDIATRICS" (PDF). INTERNATIONAL JOURNAL FOR INNOVATIVE RESEARCH IN MULTIDISCIPLINARY FIELD.
- ↑ Thomas, Gareth. Medicinal Chemistry: An Introduction.
- ↑ "Neosalvarsan". sciencedirect.com. Retrieved 1 April 2018.
- ↑ 17.0 17.1 "René Dubos". britannica.com. Retrieved 30 March 2018.
- ↑ Ravina, Enrique. The Evolution of Drug Discovery: From Traditional Medicines to Modern Drugs.
- ↑ Savona-Ventura, Charles. Contemporary Medicine in Malta [1798-1979].
- ↑ 20.00 20.01 20.02 20.03 20.04 20.05 20.06 20.07 20.08 20.09 20.10 20.11 20.12 20.13 20.14 Torok, Estee; Moran, Ed; Cooke, Fiona. Oxford Handbook of Infectious Diseases and Microbiology.
- ↑ HUGHES, RAYMOND P. "THE USE OF SULFANILAMIDE IN DERMATOLOGY". doi:10.1001/archderm.1940.01490130037006.
- ↑ 22.0 22.1 22.2 Davies, Julian; Davies, Dorothy. "Origins and Evolution of Antibiotic Resistance" (PDF). doi:10.1128/MMBR.00016-10.
- ↑ "Clinical Pharmacokinetics of Sulfonamides and Their Metabolites". karger.com. Retrieved 1 April 2018.
- ↑ DETWEILER, H. K.; KINSEY, H. I.; HURST, W. "TREATMENT OF PNEUMONIA WITH SULFAPYRIDINE".
- ↑ "Sulfapyridine (Oral Route)". mayoclinic.org. Retrieved 2 May 2018.
- ↑ Bhattacharjee, Mrinal K. Chemistry of Antibiotics and Related Drugs.
- ↑ Mouritsen, Ole G. Life - As a Matter of Fat: The Emerging Science of Lipidomics.
- ↑ Current Topics in Membranes and Transport, Volume 33.
- ↑ Stadler, Marc; Dersch, Petra. How to Overcome the Antibiotic Crisis: Facts, Challenges, Technologies and Future Perspectives.
- ↑ Persson, Sheryl. Smallpox, Syphilis and Salvation: Medical Breakthroughs that Changed the World.
- ↑ Smallman-Raynor,, Matthew; Cliff, Andrew. Atlas of Epidemic Britain: A Twentieth Century Picture.
- ↑ DUEMLING, WERNER W. "SODIUM SULFACETAMIDE IN TOPICAL THERAPY".
- ↑ DUEMLING, WERNER W. "SODIUM SULFACETAMIDE IN TOPICAL THERAPY". doi:10.1001/archderm.1954.01540130077007.
- ↑ "Sulfacetamide Sodium Drops". webmd.com. Retrieved 2 May 2018.
- ↑ Vree, T.B. "Clinical Pharmacokinetics of Sulfonamides and Their Metabolites". doi:10.1159/000414195.
- ↑ Vree, Tom B.; Aaron, Yechiel; Karger, Hekster S. Antibiotics and Chemotherapy, Volume 37.
- ↑ The New Yorker, Volume 45, Part 2.
- ↑ 38.00 38.01 38.02 38.03 38.04 38.05 38.06 38.07 38.08 38.09 38.10 38.11 38.12 38.13 38.14 38.15 38.16 38.17 38.18 38.19 38.20 38.21 "Antibiotics armageddon?". mega.online. Retrieved 31 March 2018.
- ↑ "Beta lactam antibiotics". slideshare.net. Retrieved 2 May 2018.
- ↑ "β-Lactam Antibiotics". sciencenutshell.com. Retrieved 2 May 2018.
- ↑ 41.0 41.1 41.2 41.3 41.4 Landecker, Hannah. "Antibiotic Resistance and the Biology of History".
- ↑ [Consolidated list of products whose consumption and/or sale have been banned, withdrawn, severely restricted or not approved by governments / Pharmaceuticals ] ; Consolidated list of products whose consumption and/or sale have been banned, withdrawn, severely restricted or not approved by governments. Pharmaceuticals. United Nations.
- ↑ "Clinical Pharmacokinetics of Sulfonamides and Their Metabolites". karger.com. Retrieved 1 April 2018.
- ↑ [Consolidated list of products whose consumption and/or sale have been banned, withdrawn, severely restricted or not approved by governments / Pharmaceuticals ] ; Consolidated list of products whose consumption and/or sale have been banned, withdrawn, severely restricted or not approved by governments. Pharmaceuticals. United Nations.
- ↑ Vree, Tom B.; Hekster, Yechiel Aaron. Antibiotics and Chemotherapy, Volume 37.
- ↑ Berditsch, Marina; Afonin, Sergii; Ulrich, Anne S. "The Ability of Aneurinibacillus migulanus (Bacillus brevis) To Produce the Antibiotic Gramicidin S Is Correlated with Phenotype Variation▿".
- ↑ GAUSE, G. F.; BRAZHNIKOVA, M. G. "Gramicidin S and its use in the Treatment of Infected Wounds". Nature. doi:10.1038/154703a0.
- ↑ Korzybski, Tadeusz; Kowszyk-Gindifer, Zuzanna; Kurylowicz, Wlodzimierz. Antibiotics: Origin, Nature and Properties.
- ↑ Lorian, Victor. Antibiotics in Laboratory Medicine.
- ↑ Morabia, Alfredo. Enigmas of Health and Disease: How Epidemiology Helps Unravel Scientific Mysteries.
- ↑ Cumo, Christopher Martin. The Ongoing Columbian Exchange: Stories of Biological and Economic Transfer in World History: Stories of Biological and Economic Transfer in World History.
- ↑ Boothe, Russell G. "Comparison of sulfathiazole with sulfamerazine in extraction and impaction".
- ↑ "Sulfamerazine". pubchem.ncbi.nlm.nih.gov. Retrieved 2 May 2018.
- ↑ Santo Tomas Journal of Medicine, Volume 3. University of Santo Tomas, College of Medicine.
- ↑ Biennial Report. North Dakota. State Dept. of Health.
- ↑ Nelson loose-leaf living medicine, Volume 8. T. Nelson & Sons.
- ↑ "Bacitracin A". pubchem.ncbi.nlm.nih.gov. Retrieved 2 May 2018.
- ↑ 58.00 58.01 58.02 58.03 58.04 58.05 58.06 58.07 58.08 58.09 58.10 58.11 58.12 "The Golden Age of Antibacterials". amrls.cvm.msu.edu. Retrieved 31 March 2018.
- ↑ "Bacitracin Ointment". webmd.com. Retrieved 2 May 2018.
- ↑ Stephanie Watts; Faingold, Carl; Dunaway, George; Crespo, Lynn. Brody's Human Pharmacology - E-Book.
- ↑ Riviere, Jim E.; Papich, Mark G. Veterinary Pharmacology and Therapeutics.
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- ↑ Kucers' The Use of Antibiotics: A Clinical Review of Antibacterial, Antifungal, Antiparasitic, and Antiviral Drugs, Seventh Edition - Three Volume Set (M. Lindsay Grayson, Sara E. Cosgrove, Suzanne Crowe, William Hope, James S. McCarthy, John Mills, Johan W. Mouton, David L. Paterson ed.).
- ↑ Alex, Alexander; Harris, C. John; Smith, Dennis A. Attrition in the Pharmaceutical Industry: Reasons, Implications, and Pathways Forward.
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