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Dreams of a “Magic Bullet”

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Presentation on theme: "Dreams of a “Magic Bullet”"— Presentation transcript:

1 Dreams of a “Magic Bullet”
Birth of Chemotherapy Presentation was developed by Hugh Fackrell Dreams of a “Magic Bullet”

2 Presentation Outline History “Sulfas” Ideal properties Sources
Salvorsan Sulfa Penicillin “Sulfas” Antimetabolites antibiotic synergism Ideal properties Sources Filename: Chemotheraphy.ppt

3 Semmelweiss Jena, Austria “Laying in” hospitals Peurperal fever
Cleanliness in surgery

4 Joseph Lister Developed antiseptic surgery

5 Early Antibiotics Salvarsan 606- failure
Prontosil- developed by careful research Penicillin- discovered accidently

6 Paul Ehrlich Noble Prize Chemotherapy Theory of immunity

7 Salvarsan 606 Paul Ehrlich early 1900’s syphilis
arsenic + organic compound Aniline dyes - wasn't able to find the "magic bullet”

8 Prontosil 1930's, Gerhard Domagk 1935, Jacques and Therese Trefoncel
discovered that the active compound in Prontosil was Sulfanilamide sulfanilamide “ Sulfas”

9 Sulfa Drugs

10 Sulfa vs PABA Sulfanilamide NH2 NH2SO2 PABA NH2 HOOC

11 Effectiveness of Sulfas
Organism must synthesis folic acid eg E coli no effect if folic acid is required eg man and many microbes BACTERIOSTATIC

12 Structure of Sulfa Drugs
Sulfanilamide Sulfisoxazole Prontosil

13 Folic Acid Metabolism PABA + pteridine Dihydrofolic Acid
Pteridine synthetase Dihydropteroic acid [GTP] Sulfonamide Dihydrofolic Acid Dihydrofolate Synthetase L- Glutamine Tetrahydrofolic Acid Dihydrofolate synthetase 2 NADPH 2 NADP+ Trimethoprim Thymidine DNA Purines DNA, RNA Methionine tRNa, Proteins

14 Folic Acid Inhibition PABA + pteridine Dihydrofolic Acid
Sulfonamide Dihydropteroic acid Dihydrofolic Acid Trimethoprim Tetrahydrofolic Acid Thymidine DNA Purines DNA, RNA Methionine tRNa, Proteins

15 Antibiotic Synergism Sulfisoxazole Trimethoprim

16 Antibiotic Synergism Sulfonamide + trimethoprim
Effective dosage 10% of two separately Broader spectrum of action Reduce emergence of resistant strains

17 Alexander Flemming Discovered penicillin

18 Penicillin 1928, Alexander Fleming 1938, Howard Florey and Ernst Chain
antibacterial activity in Penicillium mold (called it Penicillin) 1938, Howard Florey and Ernst Chain developed Penicillin as an effective antibiotic

19 Inhibition of Staphylococcus by Penicillium
Staphylococcus Colony Inhibition Penicillium mould

20 Penicillin prevents Assembly of Bacterial Cell Walls

21 Penicillium Growing in Broth

22 Mass Production Used Many Flasks

23 Penicillium in Vats

24 Antimicrobial Therapy
Antimicrobics substances produced by microbes that inhibit other microbes Semi-synthetic antibiotics naturally produced but altered Synthetic antibiotics: derived from chemicals

25 Ideal Properties of an Antibiotic
Low toxicity for patient kills the invading microorganism without damaging the host no adverse side reactions non allergenic High toxicity for microbe bactericidal not bacteriostatic broad spectrum Low risk of other infections

26 More Characteristics drug can be administered orally or parenterally (by injection) Soluble in tissue fluids absorbed by and dissolved in tissues or body fluids levels of active drug sustained long enough to kill the invading agent Long “Shelf” life

27 Still More Characteristics
Low probability of resistance Microbial drug resistance develops slowly microbicidal rather than microbistatic Not inactivated by organic material Assists the host in eliminating the infecting microbe Not a powerful allergen

28 Sources of Antibiotics
Most spore-forming microorganisms Fungi Penicillium penicillin, Cephalosporium griseofulvin Bacteria Bacillus bacitracin, polymyxin, tyrothricin, colimycin, gramicidin Streptomycetes Aminoglycosides, chloramphenicol, erythromycin, tetracylcine, nystatin...


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