Lrp1 is Essential for Lethal Rift Valley Fever Hepatic Disease in Mice

Overview

Journal Sci Adv

Specialties Biology
Science

Date 2023 Jul 14

PMID 37450601

Authors

Madeline M Schwarz

Safder S Ganaie

Annie Feng

Griffin Brown

Tenzin Yangdon

J Michael White

Ryan M Hoehl

Cynthia M McMillen

Rachael E Rush

Kaleigh A Connors

Xiaoxia Cui

Daisy W Leung

Takeshi Egawa

Gaya K Amarasinghe

Amy L Hartman

Affiliations

Soon will be listed here.

Abstract

Rift Valley fever virus (RVFV) is an emerging arbovirus found in Africa. While RVFV is pantropic and infects many cells and tissues, viral replication and necrosis within the liver play a critical role in mediating severe disease. The low-density lipoprotein receptor-related protein 1 (Lrp1) is a recently identified host factor for cellular entry and infection by RVFV. The biological significance of Lrp1, including its role in hepatic disease in vivo, however, remains to be determined. Because Lrp1 has a high expression level in hepatocytes, we developed a mouse model in which Lrp1 is specifically deleted in hepatocytes to test how the absence of liver Lrp1 expression affects RVF pathogenesis. Mice lacking Lrp1 expression in hepatocytes showed minimal RVFV replication in the liver, longer time to death, and altered clinical signs toward neurological disease. In contrast, RVFV infection levels in other tissues showed no difference between the two genotypes. Therefore, Lrp1 is essential for RVF hepatic disease in mice.

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