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Literature DB >> 29404895

Molecular AFM imaging of Hsp70-1A association with dipalmitoyl phosphatidylserine reveals membrane blebbing in the presence of cholesterol.

Constanze Lamprecht^1,2,3, Mathias Gehrmann⁴, Josef Madl^5,6,7, Winfried Römer^5,6,7, Gabriele Multhoff⁴, Andreas Ebner⁸.

Abstract

Hsp70-1A-the major stress-inducible member of the HSP70 chaperone family-is being implicated in cancer diseases with the development of resistances to standard therapies. In normal cells, the protein is purely cytosolic, but in a growing number of tumor cells, a significant fraction can be identified on to the cell surface. The anchoring mechanism is still under debate, as Hsp70-1A lacks conventional signaling sequences for translocation from the cytosol to exoplasmic leaflet of the plasma membrane and common membrane binding domains. Recent reports propose a lipid-mediated anchoring mechanism based on a specific interaction with charged, saturated lipids such as dipalmitoyl phosphatidylserine (DPPS). Here, we prepared planar supported lipid bilayers (SLBs) to visualize the association of Hsp70-1A directly and on the single molecule level by atomic force microscopy (AFM). The single molecule sensitivity of our approach allowed us to explore the low concentration range of 0.05 to 1.0 μg/ml of Hsp70-1A which was not studied before. We compared the binding of the protein to bilayers with 20% DPPS lipid content both in the absence and presence of cholesterol. Hsp70-1A inserted exclusively into DPPS domains and assembled in clusters with increasing protein density. A critical density was reached for incubation with 0.5 μg/ml (7 nM); at higher concentrations, membrane defects were observed that originated from cluster centers. In the presence of cholesterol, this critical concentration leads to the formation of membrane blebs, which burst at higher concentrations supporting a previously proposed non-classical pathway for the export of Hsp70-1A by tumor cells. In the discussion of our data, we attempt to link the lipid-mediated plasma membrane localization of Hsp70-1A to its potential involvement in the development of resistances to radiation and chemotherapy based on our own findings and the current literature.

Entities: Chemical Disease Gene

Keywords: Cancer; DPPS; Heat shock protein; Hsp70; Membranes; Stress; Supported lipid bilayer

Mesh：

Substances：

Year: 2018 PMID： 29404895 PMCID： PMC6045550 DOI： 10.1007/s12192-018-0879-0

Source DB: PubMed Journal: Cell Stress Chaperones ISSN： 1355-8145 Impact factor: 3.667

41 in total

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8 in total

1. Phosphatidylinositol Monophosphates Regulate the Membrane Localization of HSPA1A, a Stress-Inducible 70-kDa Heat Shock Protein.

Authors: Larissa Smulders; Rachel Altman; Carolina Briseno; Alireza Saatchi; Leslie Wallace; Maha AlSebaye; Robert V Stahelin; Nikolas Nikolaidis
Journal: Biomolecules Date: 2022-06-20

2. Human heat shock cognate protein (HSC70/HSPA8) interacts with negatively charged phospholipids by a different mechanism than other HSP70s and brings HSP90 into membranes.

Authors: Paulo R Dores-Silva; David M Cauvi; Amanda L S Coto; Noeli S M Silva; Júlio C Borges; Antonio De Maio
Journal: Cell Stress Chaperones Date: 2021-05-18 Impact factor: 3.667

Review 3. Membrane-Associated Heat Shock Proteins in Oncology: From Basic Research to New Theranostic Targets.

Authors: Maxim Shevtsov; Zsolt Balogi; William Khachatryan; Huile Gao; László Vígh; Gabriele Multhoff
Journal: Cells Date: 2020-05-20 Impact factor: 6.600

4. Membrane Localization of HspA1A, a Stress Inducible 70-kDa Heat-Shock Protein, Depends on Its Interaction with Intracellular Phosphatidylserine.

Authors: Andrei D Bilog; Larissa Smulders; Ryan Oliverio; Cedra Labanieh; Julianne Zapanta; Robert V Stahelin; Nikolas Nikolaidis
Journal: Biomolecules Date: 2019-04-17

5. A Low Membrane Hsp70 Expression in Tumor Cells With Impaired Lactate Metabolism Mediates Radiosensitization by NVP-AUY922.

Authors: Melissa Schwab; Gabriele Multhoff
Journal: Front Oncol Date: 2022-04-07 Impact factor: 5.738

6. Interaction of HSPA5 (Grp78, BIP) with negatively charged phospholipid membranes via oligomerization involving the N-terminal end domain.

Authors: Paulo Roberto Dores-Silva; David M Cauvi; Amanda L S Coto; Vanessa T R Kiraly; Júlio C Borges; Antonio De Maio
Journal: Cell Stress Chaperones Date: 2020-07-28 Impact factor: 3.827

Review 7. Plasma Membrane Lipid Domains as Platforms for Vesicle Biogenesis and Shedding?

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Journal: Biomolecules Date: 2018-09-14

Review 8. The interaction of heat shock proteins with cellular membranes: a historical perspective.

Authors: Antonio De Maio; Lawrence Hightower
Journal: Cell Stress Chaperones Date: 2021-09-03 Impact factor: 3.667

8 in total