KLK5 induces shedding of DPP4 from circulatory Th17 cells in type 2 diabetes

Titli Nargis; Krishna Kumar; Amrit Raj Ghosh; Amit Sharma; Dipayan Rudra; Debrup Sen; Saikat Chakrabarti; Satinath Mukhopadhyay; Dipyaman Ganguly; Partha Chakrabarti

doi:10.1016/j.molmet.2017.09.004

Molecular Metabolism (Nov 2017)

KLK5 induces shedding of DPP4 from circulatory Th17 cells in type 2 diabetes

Titli Nargis,
Krishna Kumar,
Amrit Raj Ghosh,
Amit Sharma,
Dipayan Rudra,
Debrup Sen,
Saikat Chakrabarti,
Satinath Mukhopadhyay,
Dipyaman Ganguly,
Partha Chakrabarti

Affiliations

Titli Nargis: Division of Cell Biology and Physiology, CSIR-Indian Institute of Chemical Biology, Kolkata, India
Krishna Kumar: Division of Structural Biology and Bioinformatics, CSIR-Indian Institute of Chemical Biology, Kolkata, India
Amrit Raj Ghosh: Division of Cancer Biology and Inflammatory Disorder, CSIR-Indian Institute of Chemical Biology, Kolkata, India
Amit Sharma: Academy of Immunology and Microbiology, Institute for Basic Science (IBS), Pohang 37673, Republic of Korea
Dipayan Rudra: Academy of Immunology and Microbiology, Institute for Basic Science (IBS), Pohang 37673, Republic of Korea
Debrup Sen: Zoology Department, Vidyasagar College, Kolkata, India
Saikat Chakrabarti: Division of Structural Biology and Bioinformatics, CSIR-Indian Institute of Chemical Biology, Kolkata, India
Satinath Mukhopadhyay: Department of Endocrinology & Metabolism, Institute of Postgraduate Medical Education and Research, Kolkata, India
Dipyaman Ganguly: Division of Cancer Biology and Inflammatory Disorder, CSIR-Indian Institute of Chemical Biology, Kolkata, India
Partha Chakrabarti: Division of Cell Biology and Physiology, CSIR-Indian Institute of Chemical Biology, Kolkata, India

DOI: https://doi.org/10.1016/j.molmet.2017.09.004
Journal volume & issue: Vol. 6, no. 11
pp. 1529 – 1539

Abstract

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Objective: Increasing plasma levels and activity of dipeptidyl peptidase-4 (DPP4 or CD26) are associated with rapid progression of metabolic syndrome to overt type 2 diabetes mellitus (T2DM). While DPP4 inhibitors are increasingly used as anti-hyperglycemic agents, the reason for the increase in plasma DPP4 activity in T2DM patients remains elusive. Methods: We looked into the source of plasma DPP4 activity in a cohort of 135 treatment naive nonobese (BMI < 30) T2DM patients. A wide array of ex vivo, in vitro, and in silico methods were employed to study enzyme activity, gene expression, subcellular localization, protease identification, surface expression, and protein–protein interactions. Results: We show that circulating immune cells, particularly CD4+ T cells, served as an important source for the increase in plasma DPP4 activity in T2DM. Moreover, we found kallikrein-related peptidase 5 (KLK5) as the enzyme responsible for cleaving DPP4 from the cell surface by directly interacting with the extracellular loop. Expression and secretion of KLK5 is induced in CD4+ T cells of T2DM patients. In addition, KLK5 shed DPP4 from circulating CD4+ T helper (Th)17 cells and shed it into the plasma of T2DM patients. Similar cleavage and shedding activities were not seen in controls. Conclusions: Our study provides mechanistic insights into the molecular interaction between KLK5 and DPP4 as well as CD4+ T cell derived KLK5 mediated enzymatic cleavage of DPP4 from cell surface. Thus, our study uncovers a hitherto unknown cellular source and mechanism behind enhanced plasma DPP4 activity in T2DM.

Published in Molecular Metabolism

ISSN: 2212-8778 (Online)
Publisher: Elsevier
Country of publisher: Netherlands
LCC subjects: Medicine: Internal medicine
Website: https://www.journals.elsevier.com/molecular-metabolism/

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