Proteome characterization of liver–kidney comorbidity after microbial sepsis-Reference-Cited by-同舟云学术

Proteome characterization of liver–kidney comorbidity after microbial sepsis

Published:2024-04-06 Issue:7 Volume:38 Page:
ISSN:0892-6638
Container-title:The FASEB Journal
language:en
Short-container-title:The FASEB Journal

Author:

Gui Yuan¹^ORCID,Yu Yanbao²^ORCID,Wang Wenjia³,Wang Yuanyuan¹^ORCID,Lu Hanyue¹,Mozdzierz Sarah¹,Eskander Kirollos¹,Lin Yi‐Han⁴^ORCID,Li Hanwen⁵,Tian Xiao‐Jun⁶^ORCID,Liu Silvia⁷⁸^ORCID,Zhou Dong¹^ORCID

Affiliation:

1. Division of Nephrology, Department of Medicine University of Connecticut School of Medicine Farmington Connecticut USA

2. Department of Chemistry & Biochemistry University of Delaware Newark Delaware USA

3. Department of Biostatistics, School of Public Health University of Pittsburgh Pittsburgh Pennsylvania USA

4. National Center for Advancing Translational Sciences Bethesda Maryland USA

5. Department of Statistics, Kenneth P. Dietrich School of Arts and Sciences University of Pittsburgh Pittsburgh Pennsylvania USA

6. School of Biological and Health Systems Engineering Arizona State University Tempe Arizona USA

7. Department of Pathology University of Pittsburgh School of Medicine Pittsburgh Pennsylvania USA

8. Pittsburgh Liver Research Center University of Pittsburgh Pittsburgh Pennsylvania USA

Abstract

AbstractSepsis is a life‐threatening condition that occurs when the body responds to an infection but subsequently triggers widespread inflammation and impaired blood flow. These pathologic responses can rapidly cause multiple organ dysfunction or failure either one by one or simultaneously. The fundamental common mechanisms involved in sepsis‐induced multiple organ dysfunction remain unclear. Here, employing quantitative global and phosphoproteomics, we examine the liver's temporal proteome and phosphoproteome changes after moderate sepsis induced by cecum ligation and puncture. In total, 4593 global proteins and 1186 phosphoproteins according to 3275 phosphosites were identified. To characterize the liver–kidney comorbidity after sepsis, we developed a mathematical model and performed cross‐analyses of liver and kidney proteome data obtained from the same set of mice. Beyond immune response, we showed the commonly disturbed pathways and key regulators of the liver–kidney comorbidity are linked to energy metabolism and consumption. Our data provide open resources to understand the communication between the liver and kidney as they work to fight infection and maintain homeostasis.

Funder

Division of Diabetes, Endocrinology, and Metabolic Diseases

Publisher

Wiley

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