Binds Human Serum Amyloid A, and the Interaction Modulates the Colonization of Human Macrophages and the Transcriptional Response of the Pathogen

Overview

Journal Cells

Publisher MDPI

Specialties Biochemistry
Biophysics
Cell Biology
Molecular Biology

Date 2021 Jun 2

PMID 34065319

Citations 9

Authors

Malwina Kawka

Anna Brzostek

Katarzyna Dzitko

Jakub Kryczka

Radoslaw Bednarek

Renata Plocinska

Przemyslaw Plocinski

Dominik Strapagiel

Justyna Gatkowska

Jaroslaw Dziadek

Bozena Dziadek

Affiliations

Soon will be listed here.

Abstract

As a very successful pathogen with outstanding adaptive properties, () has developed a plethora of sophisticated mechanisms to subvert host defenses and effectively enter and replicate in the harmful environment inside professional phagocytes, namely, macrophages. Here, we demonstrated the binding interaction of with a major human acute phase protein, namely, serum amyloid A (SAA1), and identified AtpA (Rv1308), ABC (Rv2477c), EspB (Rv3881c), TB 18.6 (Rv2140c), and ThiC (Rv0423c) membrane proteins as mycobacterial effectors responsible for the pathogen-host protein interplay. SAA1-opsonization of prior to the infection of human macrophages favored bacterial entry into target phagocytes accompanied by a substantial increase in the load of intracellularly multiplying and surviving bacteria. Furthermore, binding of human SAA1 by resulted in the up- or downregulation of the transcriptional response of tubercle bacilli. The most substantial changes were related to the increased expression level of the genes of two operons encoding mycobacterial transporter systems, namely, (), and , . Therefore, we postulate that during infection, -SAA1 binding promotes the infection of host macrophages by tubercle bacilli and modulates the functional response of the pathogen.

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