Hepatitis + HIV Treatment PDF

Summary

This document presents information on hepatitis B (HBV) and hepatitis C (HVC) treatment, including details on various drugs, their mechanisms of action (MOA), metabolism, and potential side effects. It also covers treatment for HIV. The information is organized in tabular format for easy comparison.

Full Transcript

Hepatitis B (HBV) Treatment

Drug Classification MOA Metabolism & Excretion Side Effects

Lamivudine (DOC) Cytosine analogue Turns into an active Metabolism: minimal, Nausea
metabolite when it’s mainly intracellular by
- 100 mg PO QD Nucleoside reverse phosphorylated by the sulfotransferase Vomiting
transcriptase and host cell using L-TP
polymerase inhibitor Excretion: urinary HA
This active form is then (mainly unchanged)
Also used in HIV incorporated into viral Nephrotoxicity
treatment DNA which disrupts the ½ life = 7 hrs
process of viral
replication CYP450 minimal

The fraudulent viral
DNA terminates chain
elongation by
interfering w/ HBV’s
DNA polymerase and
HIV reverse
transcriptase

Adefovir dipivoxil Adenosine nucleotide Same as ^ Metabolism:
analog which leads to phosphorylation;
- Oral termination of HBV prodrug converted to
administration of DNA adefovir active form
10 mg once a day
Excretion: urine (45%
unchanged)

½ life = 7 hrs

CYP450 none, prodrug
converted to adefovir
active form

Entecavir (Baraclude) Deoxyguanosine analog Inhibits reverse Metabolism: Minimal HA
transcriptase, DNA
- Oral admin 1 mg Effective in replication, and Excreted by glomerular Fatigue
daily Lamivudine-resistant transcription filtration and tubular
HBV secretion Nausea, dizziness
Hepatitis C (HVC) Treatment

Drug Classification MOA Metabolism & Excretion Side Effects

Mavyret A fixed-dose An inhibitor of the HCV Metabolism: Liver failure
(Pibrentasivir/Glecaprev combination product NS3/4A protease which Glecaprevir: liver,
ir) containing Glecaprevir is necessary for the partially CYP3A4 Angioedema
(HCV NS3/4A protease proteolytic cleavage of
Indicated for the tx of inhibitor) and the HCV-encoded Metabolism: HVB reactivation
patients w/ chronic HCV Pibrentasivir (HCV NS5A polyprotein and for viral Pibrentasivir: none (patients with a hx)
genotype 1, 2, 3, 4, 5, or 6 inhibitor) replication
infection without HA
cirrhosis and with Pibrentasivr is an Excretion: Glecaprevir is
compensated cirrhosis inhibitor of HCV NS5A, in the feces versus Nausea
(Child-Pugh A) which is essential for Pibrentasivir is in the
viral RNA replication urine Diarrhea
and virion assembly
Rash

Epclusa Combination of NS5A polymerase Metabolism: Sofosbuvir: Bradycardia HBV (past
Sofosbuvir, an inhibitor inhibitors: interacts w/ liver extensively CYP450 hx)
Indicated for genotypes of the HCV NS5B, and viral and host proteins none, a prodrug
1-6; patients with Velpatasvir, an inhibitor converted to active Reactivation
decompensated of the HCV NS5A NS5B polymerase metabolite angioedema
cirrhosis (Child-Pugh B protein inhibitors: interferes w/
or C) should be the viral RNA Metabolism: Velpatasvir: HA
administered with polymerase liver CTYP 2B6, 2C8, 3A4
weigh-based ribavirin Diarrhea
dosing
Excretion: Sofosbuvir is Rash
in the urine (80%)
versus Velpatsavir is in Nausea
the feces/bile (94%)
Vomiting
HIV Treatment

Class MOA Adverse Reactions Drugs Notes

Viral fusion inhibitors Inhibits entry of the viral Enfuvirtide HAART (Highly Active
RNA into the host cell Antiretroviral Therapy)
by inhibiting GP41
binding to CD4 2 NRTI’s + NNRTI

Attachment Inhibits entry of the viral Maraviroc 2 NRTI’s +
coreceptor inhibitor RNA into the host cell Integrase
by inhibiting GP120 inhibitor
binding to CCR5
2 NRTI’s +
NRTI’s (ZALES TD) Inhibit the reverse Mitochondrial toxicity* Zidovudine Protease
transcriptase from Myopathy inhibitor
taking RNA and making Peripheral Abacavir
neuropathy Adjuvant therapy
DNA by stopping the
Hepatic steatosis Lamivudine
growing DNA template Lactic acidosis Enfuvirtide
By acting like a Emtricitabine Maraviroc
nucleotide even Others
though it’s not Pancreatitis Stavudine
It will terminate Nephrotoxicity
the actual Hypersensitivity Tenofovir
reaction
formation of DNA
Didanosine
off of this RNA
template strain

NNRTI’s (-vir) Allosteric inhibitors Hepatotoxicity Nevirapine
Binds onto a particular
site CNS toxicity (dizziness Efavirenz
or mood changes)
Inhibiting the
Etravirine
reverse Rash
transcriptase Delaviridine
enzyme from Teratogenic effect
being able to Rilpivirine
function properly
Protease Inhibitors Inhibit protease → won’t Crystal-induced Atazanavir
(-navir) be able to cleave the nephropathy
polyproteins that were Darunavir
CYP450 inhibitor
translated
Indinavir
They won’t be
able to make any Lopinavir
structural and
functional Nelfinavir
proteins
Essentially then Saquinavir
can’t make new
Tipranavir
virus
Ritonavir

Integrase Inhibitors Inhibit integrase → not Rhabdomyolysis Dolutegravir
(-tegravir) allowing for the
incorporation of viral Raltegravir
DNA with host DNA
Elvitegravir
Respiratory Syncytial Virus (RSV)

Drug MOA Admin Adverse Effects Metabolism & Excretion

Amantadine Dopaminergic drug 100 mg PO BID x 3-5 d, Ataxia Metabolism: liver
start within 48 hrs of conjugation
Tx of Parkinson’s symptoms Seizures
Excretion: urine (50-90%
disease
DOES cross BBB Insomnia unchanged)

Dizziness

GI intolerance

Prolonged QT interval

Rimantadine ^ Same dose and admin Fewer SE but seizures, Metabolism: liver
as ^ insomnia, dizziness and extensive
ataxia can occur
Less lipophilic and does Excretion: urine (