Degradation of aggregated LDL occurs in complex extracellular sub-compartments of the lysosomal synapse

Author:

Singh Rajesh K.1,Barbosa-Lorenzi Valéria C.1,Lund Frederik W.1,Grosheva Inna1,Maxfield Frederick R.1,Haka Abigail S.1

Affiliation:

1. Department of Biochemistry, Weill Cornell Medical College, New York, NY 10065, USA

Abstract

Monocyte-derived cells use an extracellular, acidic, lytic compartment (a lysosomal synapse) for initial degradation of large objects or species bound to the extracellular matrix. Akin to osteoclast degradation of bone, extracellular catabolism is used by macrophages to degrade aggregates of LDL similar to those encountered during atherogenesis. However, unlike osteoclast catabolism, the lysosomal synapse is a highly dynamic and intricate structure. In this study, we use high resolution 3-dimensional imaging to visualize compartments formed by macrophages to catabolize aggregated LDL. We show that these compartments are topologically complex, have a convoluted structure and contain sub-regions that are acidified. These sub-regions are characterized by a close apposition of the macrophage plasma membrane and aggregates of LDL that are still connected to the extracellular space. Compartment formation is dependent on local actin polymerization. However, once formed, compartments are able to maintain a pH gradient when actin is depolymerized. These observations explain how compartments are able to maintain a proton gradient while remaining outside the boundaries of the plasma membrane.

Funder

National Center for Research Resources

National Institutes of Health

American Heart Association

Det Frie Forskningsråd

Conselho Nacional de Desenvolvimento Científico e Tecnológico

Publisher

The Company of Biologists

Subject

Cell Biology

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