Mapping autophagosome contents identifies interleukin-7 receptor-α as a key cargo modulating CD4+ T cell proliferation

Author:

Zhou Dingxi,Borsa MarianaORCID,Puleston Daniel J.,Zellner SusanneORCID,Capera JesusaORCID,Sanderson Sharon,Schifferer MartinaORCID,Hester Svenja S.,Ge XinORCID,Fischer RomanORCID,Jostins LukeORCID,Behrends ChristianORCID,Alsaleh Ghada,Simon Anna KatharinaORCID

Abstract

AbstractCD4+ T cells are pivotal cells playing roles in the orchestration of humoral and cytotoxic immune responses. It is known that CD4+ T cell proliferation relies on autophagy, but identification of the autophagosomal cargo involved is missing. Here we create a transgenic mouse model, to enable direct mapping of the proteinaceous content of autophagosomes in primary cells by LC3 proximity labelling. Interleukin-7 receptor-α, a cytokine receptor mostly found in naïve and memory T cells, is reproducibly detected in autophagosomes of activated CD4+ T cells. Consistently, CD4+ T cells lacking autophagy show increased interleukin-7 receptor-α surface expression, while no defect in internalisation is observed. Mechanistically, excessive surface interleukin-7 receptor-α sequestrates the common gamma chain, impairing the interleukin-2 receptor assembly and downstream signalling crucial for T cell proliferation. This study shows that key autophagy substrates can be reliably identified in this mouse model and help mechanistically unravel autophagy’s contribution to healthy physiology and disease.

Funder

China Scholarship Council

University of Oxford

Kennedy Trust

the European Union’s Horizon 2020

Wellcome Trust

Cue Biopharma KTRR Cell Dynamics Platform

Deutsche Forschungsgemeinschaft

Collaborative Research Center 1177

Versus Arthritis - 22617

Publisher

Springer Science and Business Media LLC

Subject

General Physics and Astronomy,General Biochemistry, Genetics and Molecular Biology,General Chemistry,Multidisciplinary

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