A naturally occurring 22-amino acid fragment of human hemoglobin A inhibits autophagy and HIV-1

A naturally occurring 22-amino acid fragment of human hemoglobin A inhibits autophagy and HIV-1

Autophagy is an evolutionarily ancient catabolic pathway and has recently emerged as an integral part of the innate immune system. While the core machinery of autophagy is well defined, the physiological regulation of autophagy is less understood. Here, we identify a C-terminal fragment of human hem...

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Veröffentlicht in:CELLULAR AND MOLECULAR LIFE SCIENCES 2024-12, Vol.81 (1)
Hauptverfasser: Freisem, Dennis, Rodriguez-Alfonso, Armando A, Lawrenz, Jan, Zhou, Zhixuan, Monecke, Thomas, Preising, Nico, Endres, Sascha, Wiese, Sebastian, Staendker, Ludger, Kuan, Seah-Ling, Thal, Dietmar R, Weil, Tanja, Niessing, Dierk, Barth, Holger, Kirchhoff, Frank, Harms, Mirja, Muench, Jan, Sparrer, Konstantin M.J
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container_title CELLULAR AND MOLECULAR LIFE SCIENCES
container_volume 81
creator Freisem, Dennis
Rodriguez-Alfonso, Armando A
Lawrenz, Jan
Zhou, Zhixuan
Monecke, Thomas
Preising, Nico
Endres, Sascha
Wiese, Sebastian
Staendker, Ludger
Kuan, Seah-Ling
Thal, Dietmar R
Weil, Tanja
Niessing, Dierk
Barth, Holger
Kirchhoff, Frank
Harms, Mirja
Muench, Jan
Sparrer, Konstantin M.J
description Autophagy is an evolutionarily ancient catabolic pathway and has recently emerged as an integral part of the innate immune system. While the core machinery of autophagy is well defined, the physiological regulation of autophagy is less understood. Here, we identify a C-terminal fragment of human hemoglobin A (HBA1, amino acids 111-132) in human bone marrow as a fast-acting non-inflammatory inhibitor of autophagy initiation. It is proteolytically released from full-length HBA1 by cathepsin E, trypsin or pepsin. Biochemical characterization revealed that HBA1(111-132) has an in vitro stability of 52 min in human plasma and adopts a flexible monomeric conformation in solution. Structure-activity relationship studies revealed that the C-terminal 13 amino acids of HBA1(120-132) are sufficient to inhibit autophagy, two charged amino acids (D127, K128) mediate solubility, and two serines (S125, S132) are required for function. Successful viruses like human immunodeficiency virus 1 (HIV-1) evolved strategies to subvert autophagy for virion production. Our results show that HBA1(120-132) reduced virus yields of lab-adapted and primary HIV-1. Summarizing, our data identifies naturally occurring HBA1(111-132) as a physiological, non-inflammatory antagonist of autophagy. Optimized derivatives of HBA1(111-132) may offer perspectives to restrict autophagy-dependent viruses.
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title A naturally occurring 22-amino acid fragment of human hemoglobin A inhibits autophagy and HIV-1
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