antimicrobials- Flashcards

1
Q

Chemical substances produced by microorganisms with the capacity to inhibit
(bacteriostatic) or kill (bactericidal) other microorganisms.

A

antibiotics/antimicrobials

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2
Q

produce amphotericin B

A

streptomyces nodosus

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3
Q

produce Nystatin

A

Streptomyces noursei

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4
Q

produce Chloramphenicol

A

Streptomyces venezuelae

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5
Q

produce Bacitracin

A

Bacillus subtilis

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6
Q

produce Polymyxin

A

Bacillus polymyxa

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7
Q

produce Cephalosporins

A

Cephalosporium

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8
Q

produce Gentamicin

A

Micromonospora purpurea

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9
Q

produce Penicillin

A

Penicillium notatum

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10
Q

produce Erythromycin

A

Streptomyces erythraeus

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11
Q

produce Neomycin

A

Streptomyces fradiae

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12
Q

effective against a limited number of pathogens.

A

narrow spectrum

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13
Q

example of narrow-spectrum

A

Bacitracin, clindamycin, erythromycin, gentamicin, penicillin and
Vancomycin

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14
Q

destroy different kinds of organisms.

A

broad spectrum

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15
Q

example of broad spectrum

A

Ampicillin, cephalosporins, chloramphenicol, ciprofloxacin, rifampicin,
trimethoprim and tetracycline.

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16
Q

drugs produced by bacteria or fungi.

A

natural drugs such as Erythromycin, amphotericin B, vancomycin, tetracycline, penicillin

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17
Q

modified drugs with added chemical groups.

A

semi-synthetic drugs such as Ampicillin, carbenicillin and methicillin.

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18
Q

a chemically-produced drugs

A

synthetic drugs such as Sulfonamides, trimethoprim, ciprofloxacin, isoniazid.

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19
Q

inhibit the bacterial growth but generally they do not kill the microorganisms.

A

Bacteriostatic agents such as Chloramphenicol, erythromycin, clindamycin

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20
Q

usually kill or destroy organisms and are used for the treatment of life-threatening infections.

A

bactericidal agents such as:
Aminoglycosides ( gentamicin,amikacin & streptomycin)
β-lactams ( ceftriaxone, imepenem, penicillin & cefotaxime)
Glycopeptides ( isoniazid, quinolones, bacitracin and metronidazole)

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21
Q

Characteristics of Antimicrobial agents

A
  1. Must be in an active form.
  2. Must able to achieve concentration at the site of infection that is higher than the
    pathogen’s MIC to be effective.
  3. Must have “selective toxicity”.
22
Q

are genetic elements that are capable of integrating genes(cassettes) by an integrin
encoded site-specific recombinase.

A

integrons

23
Q

lowest concentration of a drug that can still
inhibit bacterial growth.

A

Minimal-inhibitory concentration (MIC)

24
Q

the lowest concentration of a drug that can kill bacteria.

A

Minimal lethal concentration

25
Q

are enzymes (transpeptidase or transglycolase) that mediate
peptidoglycan cross-linking with reduced affinity for B-lactam antibiotics.

A

Penicillin-binding proteins

26
Q

the ratio of the toxic dose to the therapeutic dose and as such, the higher the
therapeutic index, the more effective the chemotherapeutic agent.

A

therapeutic index

27
Q

DNA elements that encode transposition and excision functions and which are also
able to carry antibiotic resistance genes among plasmids and chromosomes

A

transposons

28
Q

most selective antibiotics with a high therapeutic index. Inhibits the transpeptidase enzymes in which cell growth stops and the death of the cells occurs.

A

cell wall inhibitors

29
Q

inhibits the synthesis of peptidoglycan precursors

A

bacitracin

30
Q

inhibits transpeptidation

A

β-lactams

31
Q

acts on growing cells & can either be a bactericidal or bacteriostatic agent

A

isoniazid

32
Q

inhibits the translocation and elongation of peptidoglycan.

A

vancomycin

33
Q

binds with a 30S subunit that result in the misreading
of mRNA and 50S subunit that results in the inhibition of peptidyl transferase and peptide
chain elongation.

A

protein synthesis inhibitors such as

Tetracycline, aminoglycosides (30S)
Erythromycin,chloramphenicol & clindamycin ( 50S)
Linezolid – blocks the initial step in protein synthesis.

34
Q

nucleic acid inhibitors

A

rifampicin, quinolones, metronidazole

35
Q

inhibits RNA polymerase

A

Rifampicin

36
Q

interferes with DNA gyrase and topoisomerase IV and highly effective for enteric bacteria.

A

Quinolones

37
Q

disrupts DNA and is effective against anaerobic bacteria.

A

Metronidazole

38
Q

cell membrane inhibitors

A

Polymyxin B and E – Gram- negative bacteria (P.aeuruginosa) also used as a topical
antibiotic.

39
Q

Essential metabolite inhibitors

A

SMZ, Dapsone, Trimethoprin

40
Q

inhibits folic acid and metabolism and has a higher
therapeutic index.

A

Sulfamethoxazole (SMZ)

41
Q

interferes with folic acid synthesis

A

Dapsone

42
Q

blocks the tetrahydrofale synthesis

A

Trimethoprim

43
Q

Result of both the use and overuse of antimicrobial agents and may arise within antibiotic-producing microorganism (autotoxicity)

A

Antibiotic Resistance

44
Q

2 types of A.R

A

Intrinsic Resistance and Acquired Resistance

45
Q

Result of the biochemical make up of wild type of organism.

Depends on the hydrophobic or hydrophilic nature of the antibiotic and on the
impermeability of the cell wall to the antibiotic

Passed vertically into new cell.

A

Intrinsic Resistance

46
Q

All Gram-negative bacteria mediate this type of resistance through the inactivation of
penicillin

A

intrinsic resistance

47
Q

enzymes that chemically inactivate β-lactam drugs by disrupting β-lactam ring component of the molecule.

A

B-lactamases

48
Q

clinically important B-lactamases

A

Class A enzymes - plasmids found
Class C enzymes - chromosomally localed and inducible by exposure to β-lactams.

49
Q

structurally similar with the β-lactam antibiotics and functions as
a substrate, thus reducing their harmful effects on the β-lactam antibiotics.

A

Β-lactamase Inhibitors

50
Q

Present only on a certain isolates that are different from the parental strains and usually expressed as a modification of target sites or enzymatic modification of antibiotics.

A

Acquired Resistance

51
Q

ex. of Acquired Resistance

A

Chromosomal mutations (transformation and recombination)