Is Hepatitis C Virus (HCV) Elimination Achievable Among People Who Inject Drugs in Tijuana, Mexico? A Modeling Analysis

Overview

Journal Int J Drug Policy

Publisher Elsevier

Specialties Psychiatry
Public Health

Date 2020 Mar 14

PMID 32165050

Citations 7

Authors

Lara K Marquez

Javier A Cepeda

Annick Borquez

Steffanie A Strathdee

Patricia E Gonzalez-Zuniga

Clara Fleiz

Claudia Rafful

Richard S Garfein

Susan M Kiene

Stephanie Brodine

Natasha K Martin

Affiliations

Soon will be listed here.

Abstract

Background: In 2019, Mexico became the first Latin American country committed to hepatitis C virus (HCV) elimination, but the amount of intervention scale-up required is unclear. In Tijuana, HCV among people who inject drugs (PWID) is high; yet there is minimal and intermittent harm reduction, and involuntary exposure to compulsory abstinence programs (CAP) occurs which is associated with increased HCV risk. We determined what combination intervention scale-up can achieve HCV elimination among current and former PWID in Tijuana.

Methods: We constructed a dynamic, deterministic model of HCV transmission, disease progression, and harm reduction among current and former PWID parameterized to Tijuana (~10,000 current PWID, 90% HCV seropositive, minimal opiate agonist therapy [OAT] or high coverage needle/syringe programs [HCNSP]). We evaluated the number of direct-acting antiviral (DAA) treatments needed from 2019 to achieve elimination targets (80% incidence reduction, 65% mortality reduction by 2030) with: (a) DAAs alone, (b) DAAs plus scale-up of OAT+HCNSP (up to 50% coverage of OAT and HCNSP separately, producing 25% of PWID receiving both), (c) DAAs plus CAP scale-up to 50%. Scenarios examined the number of DAAs required if prioritized to current PWID or provided regardless of current injection status, and impact of harm reduction interruptions.

Results: Modeling suggests among ~30,000 current and former PWID in Tijuana, 16,160 (95%CI: 12,770-21,610) have chronic HCV. DAA scale-up can achieve the incidence target, requiring 770 treatments/year (95%CI: 640-970) if prioritized to current PWID. 40% fewer DAAs are required with OAT+HCNSP scale-up to 50% among PWID, whereas more are required with involuntary CAP scale-up. Both targets can only be achieved through treating both current and former PWID (1,710 treatments/year), and impact is reduced with harm reduction interruptions.

Conclusions: Elimination targets are achievable in Tijuana through scale-up of harm reduction and DAA therapy, whereas involuntary CAP and harm reduction interruptions hamper elimination.

Citing Articles

An Update on Viral Hepatitis B and C in Mexico: Advances and Pitfalls in Eradication Strategies.

Campos-Valdez M, Castro-Garcia M, Ramos-Marquez M, Gurrola-Diaz C, Salazar-Montes A, Sanchez-Orozco L Microorganisms. 2024; 12(7).

PMID: 39065136 PMC: 11279215. DOI: 10.3390/microorganisms12071368.

Estimating the impact of a police education program on hepatitis C virus transmission and disease burden among people who inject drugs in Tijuana, Mexico: A dynamic modeling analysis.

Rivera Saldana C, Abramovitz D, Beletsky L, Borquez A, Kiene S, Marquez L Addiction. 2023; 118(9):1763-1774.

PMID: 37039246 PMC: 10524658. DOI: 10.1111/add.16203.

Modelling the contribution of incarceration and public health oriented drug law reform to HCV transmission and elimination among PWID in Tijuana, Mexico.

Rivera Saldana C, Beletsky L, Borquez A, Kiene S, Marquez L, Strathdee S Int J Drug Policy. 2022; 110:103878.

PMID: 36242829 PMC: 9841890. DOI: 10.1016/j.drugpo.2022.103878.

Hepatitis C elimination among people who inject drugs in Mexico during the COVID-19 pandemic.

Marquez L, Borquez A, Fleiz C, Magis-Rodriguez C, Rangel G, Strathdee S Gac Med Mex. 2022; 158(2):110-113.

PMID: 35763823 PMC: 10589063. DOI: 10.24875/GMM.M22000650.

Methods and indicators to validate country reductions in incidence of hepatitis C virus infection to elimination levels set by WHO.

Artenie A, Luhmann N, Lim A, Fraser H, Ward Z, Stone J Lancet Gastroenterol Hepatol. 2022; 7(4):353-366.

PMID: 35122713 PMC: 10644895. DOI: 10.1016/S2468-1253(21)00311-3.

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