Elevated CCL2 causes Leydig cell malfunction in metabolic syndrome
Qingkui Jiang, … , Lanbo Shi, Thomas Linn
Qingkui Jiang, … , Lanbo Shi, Thomas Linn
Published November 5, 2020
Citation Information: JCI Insight. 2020;5(21):e134882. https://doi.org/10.1172/jci.insight.134882.
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Research Article Endocrinology Reproductive biology

Elevated CCL2 causes Leydig cell malfunction in metabolic syndrome

Abstract

Metabolic syndrome (MetS), which is associated with chronic inflammation, predisposes males to hypogonadism and subfertility. The underlying mechanism of these pathologies remains poorly understood. Homozygous leptin-resistant obese db/db mice are characterized by small testes, low testicular testosterone, and a reduced number of Leydig cells. Here we report that IL-1β, CCL2 (also known as MCP-1), and corticosterone concentrations were increased in the testes of db/db mice relative to those in WT controls. Cultured murine and human Leydig cells responded to cytokine stress with increased CCL2 release and apoptotic signals. Chemical inhibition of CCL2 rescued Leydig cell function in vitro and in db/db mice. Consistently, we found that Ccl2-deficient mice fed with a high-energy diet were protected from testicular dysfunction compared with similarly fed WT mice. Finally, a cohort of infertile men with a history of MetS showed that reduction of CCL2 plasma levels could be achieved by weight loss and was clearly associated with recovery from hypogonadism. Taken together, we conclude that CCL2-mediated chronic inflammation is, to a large extent, responsible for the subfertility in MetS by causing damage to Leydig cells.

Authors

Qingkui Jiang, Constanze C. Maresch, Sebastian Friedrich Petry, Agnieszka Paradowska-Dogan, Sudhanshu Bhushan, Yongsheng Chang, Christine Wrenzycki, Hans-Christian Schuppe, Petr Houska, Michaela F. Hartmann, Stefan A. Wudy, Lanbo Shi, Thomas Linn

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Figure 5

Testicular immune cells and corticosterone levels in db/db mice.

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Testicular immune cells and corticosterone levels in db/db mice. (A) Tot...
(A) Total testicular cells were isolated as described in Methods and examined by FACS. Representative flow cytometry gating schemes for testicular cells from WT and db/db mice are demonstrated. The gating strategy is shown for CD45+F4/80+ and F4/80+CD64+ cells. (B) Frequencies of testicular F4/80+ within CD45+ cells and CD64+ within F4/80+CD45+ cells from WT and db/db mice. (C) The Il-10 mRNA expression in testes. (D) The Nos2 and Arg1 mRNA expression in testes. (E) Corticosterone levels in TIF and serum. N= 3–8 mice, 12 to 24 weeks old, in each group. Data are shown as means ± SEM. Student’s 2-tailed t test was used to compare means between 2 groups. *P < 0.05, **P < 0.01, ****P < 0.0001.