Microbiology- Antimicrobials (Micobacterium, HIV and Micosis)

Question 1

Antifungal therapy Imagen

Answer 1

pag 198

Question 2

Amphotericin B

• Mechanism
• Adverse effects

Answer 2

Binds ergosterol (unique to fungi); forms membrane pores that allow leakage of electrolytes.

Fever/chills (“shake and bake”), hypotension, nephrotoxicity, arrhythmias, anemia, IV phlebitis (“amphoterrible”). Hydration lowers nephrotoxicity. Liposomal amphotericin lowers toxicity.

Question 3

Amphotericin B

- Clinical Uses

Answer 3

Serious, systemic mycoses. Cryptococcus (amphotericin B with/without flucytosine for cryptococcal meningitis), Blastomyces, Coccidioides, Histoplasma, Candida,
Mucor. Intrathecally for fungal meningitis. Supplement K+ and Mg2+ because of altered renal tubule permeability.

Question 4

Nystatin

• Mechanism
• Clinical Uses

Answer 4

Same as amphotericin B. Topical use only as too toxic for systemic use.

“Swish and swallow” for oral candidiasis (thrush); topical for diaper rash or vaginal candidiasis.

Question 5

Flucytosine

• Mechanism
• Clinical Uses
• Adverse effects

Answer 5

Inhibits DNA and RNA biosynthesis by conversion to 5 fluorouracil by cytosine deaminase.

Systemic fungal infections (especially meningitis caused by Cryptococcus) in combination with amphotericin B.

Bone marrow suppression.

Question 6

Azoles

• Names
• Mechanism
• Adverse effects

Answer 6

Clotrimazole, fluconazole, isavuconazole, itraconazole, ketoconazole, miconazole, voriconazole.

Inhibit fungal sterol (ergosterol) synthesis by inhibiting the cytochrome P-450 enzyme that converts lanosterol to ergosterol.

Testosterone synthesis inhibition (gynecomastia, especially with ketoconazole), liver dysfunction (inhibits cytochrome P-450).

Question 7

Azoles

- Clinical use

Answer 7

Local and less serious systemic mycoses. Fluconazole for chronic suppression of cryptococcal meningitis in AIDS patients and candidal infections of all types.

Itraconazole for Blastomyces, Coccidioides, Histoplasma. Clotrimazole and miconazole for topical fungal infections.

Voriconazole for Aspergillus and some Candida. Isavuconazole for serious Aspergillus and Mucor
infections

Question 8

Terbinafine

• Mechanism
• Clinical Uses
• Adverse effects

Answer 8

Inhibits the fungal enzyme squalene epoxidase

Dermatophytoses (especially onychomycosis—fungal infection of finger or toe nails).

GI upset, headaches, hepatotoxicity, taste disturbance.

Question 9

Echinocandins

• Names
• Mechanism
• Clinical Uses
• Adverse effects

Answer 9

Anidulafungin, caspofungin, micafungin

Inhibit cell wall synthesis by inhibiting synthesis of β-glucan.

Invasive aspergillosis, Candida.

GI upset, flushing (by histamine release).

Question 10

Griseofulvin

• Mechanism
• Clinical Uses
• Adverse effects

Answer 10

Interferes with microtubule function; disrupts mitosis. Deposits in keratin-containing tissues (eg, nails).

Oral treatment of superficial infections; inhibits growth of dermatophytes (tinea, ringworm)

Teratogenic, carcinogenic, confusion, headaches, disulfiram-like reaction, High cytochrome P-450 and
warfarin metabolism.

Question 11

Antiprotozoal therapy

Answer 11

Pyrimethamine (toxoplasmosis), suramin and melarsoprol (Trypanosoma brucei), nifurtimox (T cruzi), sodium stibogluconate (leishmaniasis).

Question 12

Anti-mite/louse therapy

Answer 12

Permethrin (inhibits Na+ channel deactivation, neuronal membrane depolarization), malathion (acetylcholinesterase inhibitor), lindane (blocks GABA channels, neurotoxicity).

Used to treat scabies (Sarcoptes scabiei) and lice (Pediculus and Pthirus).

Question 13

Chloroquine

• Mechanism
• Clinical Uses
• Adverse effects

Answer 13

Blocks detoxification of heme into hemozoin. Heme accumulates and is toxic to plasmodia.

Treatment of plasmodial species other than P falciparum. Resistance due to membrane pump that lowers intracellular concentration of drug.

Treat P falciparum with artemether/lumefantrine or atovaquone/proguanil. For life-threatening malaria,
use quinidine in US (quinine elsewhere) or artesunate.

Retinopathy; pruritus (especially in dark-skinned individuals).

Question 14

Antihelminthic therapy

Answer 14

Pyrantel pamoate, Ivermectin, Mebendazole (microtubule inhibitor), Praziquantel, Diethylcarbamazine.

Helminths get PIMP’D.

Question 15

Oseltamivir, zanamivir

• Mechanism
• Clinical Uses

Answer 15

Inhibit influenza neuraminidase, lowers release of progeny virus.

Treatment and prevention of both influenza A and B. Beginning therapy within 48 hours of symptom onset may shorten duration of illness.

Question 16

Acyclovir, famciclovir, valacyclovir

• Mechanism
• Adverse effects
• Resistance

Answer 16

Guanosine analogs. Monophosphorylated by HSV/VZV thymidine kinase. Triphosphate formed by cellular enzymes. Preferentially inhibit viral DNA polymerase by chain termination.

Obstructive crystalline nephropathy and acute renal failure if not adequately hydrated.

Mutated viral thymidine kinase.

Question 17

Acyclovir, famciclovir, valacyclovir

- Clinical use

Answer 17

HSV and VZV. Weak activity against EBV. No activity against CMV.

Used for HSVinduced mucocutaneous and genital lesions as well as for encephalitis. Prophylaxis in
immunocompromised patients. No effect on latent forms of HSV and VZV.

Valacyclovir, a prodrug of acyclovir, has better oral bioavailability. For herpes zoster, use famciclovir.

Question 18

Ganciclovir

• Mechanism
• Adverse effects
• Resistance

Answer 18

5′-monophosphate formed by a CMV viral kinase. Guanosine analog. Triphosphate formed by cellular kinases. Preferentially inhibits viral DNA polymerase.

Bone marrow suppression, renal toxicity. More toxic
to host enzymes than acyclovir.

Mutated viral kinase.

Question 19

Ganciclovir

- Clinical use

Answer 19

CMV, especially in immunocompromised patients. Valganciclovir, a prodrug of ganciclovir, has better oral bioavailability.

Question 20

Foscarnet

• Mechanism
• Adverse effects
• Resistance

Answer 20

Viral DNA/RNA polymerase inhibitor and HIV reverse transcriptase inhibitor. Binds to pyrophosphate-binding site of enzyme. Does not require any kinase activation.

Nephrotoxicity, electrolyte abnormalities (hypo- or hypercalcemia, hypo- or hyperphosphatemia, hypokalemia, hypomagnesemia) can lead to seizures.

Mutated DNA polymerase.

Question 21

Foscarnet

- Clinical use

Answer 21

CMV retinitis in immunocompromised patients when ganciclovir fails; acyclovir-resistant HSV.

Question 22

Cidofovir

Answer 22

Preferentially inhibits viral DNA polymerase. Does not require phosphorylation by viral kinase.

CMV retinitis in immunocompromised patients; acyclovir-resistant HSV. Long half-life.

Nephrotoxicity (coadminister with probenecid and IV saline to reduce toxicity).

Question 23

HIV therapy

Answer 23

Highly active antiretroviral therapy (HAART): often initiated at the time of HIV diagnosis.

Strongest indication for patients presenting with AIDS-defining illness, low CD4+ cell counts (< 500 cells/mm3), or high viral load.

Regimen consists of 3 drugs to prevent resistance:
2 NRTIs and preferably an integrase inhibitor

Question 24

NRTIs

- Mechanism

Answer 24

Competitively inhibit nucleotide binding to reverse transcriptase and terminate the DNA chain (lack a 3′ OH group). All need to be phosphorylated to be active.

ZDV can be used for general prophylaxis and during pregnancy to reduce risk of fetal transmission.

Question 25

NRTIs

- Toxicity

Answer 25

Bone marrow suppression (can be reversed with
granulocyte colony-stimulating factor [G-CSF] and erythropoietin), peripheral neuropathy, lactic acidosis (nucleosides), anemia (ZDV), pancreatitis (didanosine).

Abacavir contraindicated if patient has HLA-B*5701 mutation due to risk of hypersensitivity.

Question 26

NRTIs

- Names

Answer 26

Abacavir (ABC)
Didanosine (ddI)
Emtricitabine (FTC)
Lamivudine (3TC)
Stavudine (d4T)
Tenofovir (TDF)
Zidovudine (ZDV,cformerly AZT)

Question 27

NNRTIs

• Names
• Mechanism

Answer 27

Delavirdine, Efavirenz, Nevirapine

Bind to reverse transcriptase at site different from NRTIs. Do not require phosphorylation to be active or compete with nucleotides.

Question 28

NNRTIs

- Toxicity

Answer 28

Rash and hepatotoxicity are common to all NNRTIs. Vivid dreams and CNS symptoms are common with efavirenz. Delavirdine and efavirenz are contraindicated in pregnancy.

Question 29

Protease inhibitors

- names

Answer 29

Atazanavir
Darunavir
Fosamprenavir
Indinavir
Lopinavir
Ritonavir
Saquinavir

Question 30

Protease inhibitors

- Mechanism

Answer 30

Assembly of virions depends on HIV-1 protease (pol gene), which cleaves the polypeptide products of HIV mRNA into their functional parts

Ritonavir can “boost” other drug concentrations by inhibiting cytochrome P-450.

Question 31

Protease inhibitors

- Toxicity

Answer 31

Hyperglycemia, GI intolerance (nausea, diarrhea), lipodystrophy (Cushing-like syndrome).

Nephropathy, hematuria, thrombocytopenia (indinavir).

Rifampin (potent CYP/UGT inducer) reduces protease inhibitor concentrations; use rifabutin instead

Question 32

Integrase inhibitors

• Names
• Mechanism
• Toxicity

Answer 32

Dolutegravir, Elvitegravir, Raltegravir

Inhibits HIV genome integration into host cell chromosome by reversibly inhibiting HIV integrase

High creatine kinase

Question 33

Fusion inhibitors

• Enfuvirtide
• Maraviroc

Answer 33

• Binds gp41, inhibiting viral entry. Skin reaction at injection sites.
• Binds CCR-5 on surface of T cells/monocytes, inhibiting interaction with gp120.

Question 34

Interferons

• Mechanism
• Adverse effects

Answer 34

exhibiting a wide range of antiviral and antitumoral properties.

Flu-like symptoms, depression, neutropenia, myopathy.

Question 35

Interferons

- Clinical use

Answer 35

Chronic HBV and HVC, Kaposi sarcoma, hairy cell leukemia, condyloma acuminatum, renal cell
carcinoma, malignant melanoma, multiple sclerosis, chronic granulomatous disease.

Question 36

Hepatitis C therapy

Answer 36

Chronic HCV infection is treated with different combinations of the following drugs; none is approved as monotherapy. Ribavirin also used to treat RSV (palivizumab preferred in children).

• Ledipasvir, Ribavirin, Simeprevir, Sofosbuvir

Question 37

Ledipasvir

Answer 37

Viral phosphoprotein (NS5A) inhibitor; NS5A plays important role in replication.

Question 38

Ribavirin

• Mechanism
• Adverse effects

Answer 38

Inhibits synthesis of guanine nucleotides by competitively inhibiting inosine monophosphate dehydrogenase.

Hemolytic anemia, severe teratogen.

Question 39

Simeprevir

• Mechanism
• Adverse effects

Answer 39

HCV protease (NS3/4A); prevents viral replication.

Photosensitivity reactions, rash

Question 40

Sofosbuvir

• Mechanism
• Adverse effects

Answer 40

Inhibits HCV RNA-dependent RNA polymerase (NS5B) acting as a chain terminator.

Fatigue, headache, nausea.

Question 41

Antimicrobials to avoid in pregnancy

Answer 41

SAFe Children Take Really Good Care.

Sulfonamides
Aminoglucosidos
Fluoroquinolone
Claritromicina
Tetraciclina
Ribavirin
Griseofulvin
Cloranfenicol

Question 42

Disinfection and

sterilization

Answer 42

Pag 204

Question 43

Antimycobacterial drugs

M tuberculosis

Answer 43

RIPE: Rifampin, Isoniazid, Pyrazinamide, Ethambutol

Profilaxis: Isoniazid

Question 44

Antimycobacterial drugs

M avium–intracellulare

Answer 44

More drug resistant than M tuberculosis. Azithromycin or clarithromycin + ethambutol. Can add rifabutin or ciprofloxacin.

Profilaxis: Azithromycin, rifabutin

Question 45

Antimycobacterial drugs

M leprae

Answer 45

Long-term treatment with dapsone and rifampin for tuberculoid form. Add clofazimine for lepromatous form.

Question 46

Rifamycins (Rifampin, rifabutin.)

• Mechanism
• Clinical use

Answer 46

Inhibit DNA-dependent RNA polymerase.

Mycobacterium tuberculosis; delay resistance to dapsone when used for leprosy. Used for meningococcal prophylaxis and chemoprophylaxis in contacts of children with H influenzae type b.

Question 47

Rifamycins (Rifampin, rifabutin)

• Adverse effects
• Resistance

Answer 47

Minor hepatotoxicity and drug interactions (Enhance cytochrome P-450); orange body fluids (nonhazardous side effect). Rifabutin favored over rifampin in patients with HIV infection due to less cytochrome P-450 stimulation.

Mutations reduce drug binding to RNA polymerase. Monotherapy rapidly leads to resistance.

Rifampin’s 4 R’s:
RNA polymerase inhibitor
Ramps up microsomal cytochrome P-450
Red/orange body fluids
Rapid resistance if used alone

Question 48

Isoniazid

• Mechanism
• Clinical use

Answer 48

Lowers synthesis of mycolic acids. Bacterial catalaseperoxidase (encoded by KatG) needed to convert INH to active metabolite.

Mycobacterium tuberculosis. The only agent used as solo prophylaxis against TB. Also used as monotherapy for latent TB.

Question 49

Isoniazid

• Adverse effects
• Resistance

Answer 49

Hepatotoxicity, P-450 inhibition, drug-induced SLE, anion gap metabolic acidosis, vitamin B6 deficiency (peripheral neuropathy, sideroblastic anemia). Administer with pyridoxine (B6).

INH Injures Neurons and Hepatocytes.

Mutations leading to underexpression of KatG.

Question 50

Pyrazinamide

• Mechanism
• Clinical use
• Adverse effects

Answer 50

Mechanism uncertain. Pyrazinamide is a prodrug that is converted to the active compound pyrazinoic acid. Works best at acidic pH.

Mycobacterium tuberculosis

Hyperuricemia, hepatotoxicity.

Question 51

Ethambutol

• Mechanism
• Clinical use
• Adverse effects

Answer 51

lowers carbohydrate polymerization of mycobacterium cell wall by blocking arabinosyltransferase.

Mycobacterium tuberculosis

Optic neuropathy (red-green color blindness). Pronounce “eyethambutol.”

Question 52

Streptomycin

• Mechanism
• Clinical use
• Adverse effects

Answer 52

Interferes with 30S component of ribosome

Mycobacterium tuberculosis (2nd line).

Tinnitus, vertigo, ataxia, nephrotoxicity