Refinement of the HIVAN1 Susceptibility Locus on Chr. 3A1-A3 Via Generation of Sub-Congenic Strains

Overview

Journal PLoS One

Specialties General Medicine
Science

Date 2016 Oct 14

PMID 27736906

Citations 2

Authors

Natalia Papeta

Ami Patel

Vivette D DAgati

Ali G Gharavi

Affiliations

Soon will be listed here.

Abstract

HIV-1 transgenic mice on the FVB/NJ background (TgFVB) represent a validated model of HIV-associated nephropathy (HIVAN). A major susceptibility locus, HIVAN1, was previously mapped to chromosome 3A1-A3 in a cross between TgFVB and CAST/EiJ (CAST) strains, and introgression of a 51.9 Mb segment encompassing HIVAN1 from CAST into TgFVB resulted in accelerated development of nephropathy. We generated three sub-congenic strains carrying CAST alleles in the proximal or distal regions of the HIVAN1 locus (Sub-II, 3.02-38.93 Mb; Sub-III, 38.45-55.1 Mb and Sub-IV, 47.7-55.1 Mb, build 38). At 5-10 weeks of age, histologic injury and proteinuria did not differ between HIV-1 transgenic Sub-II and TgFVB mice. In contrast, HIV-1 transgenic Sub-III and Sub-IV mice displayed up to 4.4 fold more histopathologic injury and 6-fold more albuminuria compared to TgFVB mice, similar in severity to the full-length congenic mice. The Sub-IV segment defines a maximal 7.4 Mb interval for HIVAN1, and encodes 31 protein coding genes: 15 genes have missense variants differentiating CAST from FVB, and 14 genes show differential renal expression. Of these, Frem1, Foxo1, and Setd7 have been implicated in the pathogenesis of nephropathy. HIVAN1 congenic kidneys are histologically normal without the HIV-1 transgene, yet their global transcriptome is enriched for molecular signatures of apoptosis, adenoviral infection, as well as genes repressed by histone H3 lysine 27 trimethylation, a histone modification associated with HIV-1 life cycle. These data refine HIVAN1to 7.4 Mb and identify latent molecular derangements that may predispose to nephropathy upon exposure to HIV-1.

Citing Articles

GWAS in Mice Maps Susceptibility to HIV-Associated Nephropathy to the Locus.

Steers N, Gupta Y, DAgati V, Lim T, DeMaria N, Mo A J Am Soc Nephrol. 2021; 33(1):108-120.

PMID: 34893534 PMC: 8763192. DOI: 10.1681/ASN.2021040543.

HIV-Associated Nephropathy in Africa: Pathology, Clinical Presentation and Strategy for Prevention.

Husain N, Ahmed M, Almobarak A, Noor S, Elmadhoun W, Awadalla H J Clin Med Res. 2017; 10(1):1-8.

PMID: 29238427 PMC: 5722038. DOI: 10.14740/jocmr3235w.

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