Influx of podoplanin‐expressing inflammatory macrophages into the genital tract following Chlamydia infection

平足蛋白 沙眼衣原体 CD11c公司 整合素αM 炎症 免疫学 巨噬细胞 生物 甘露糖受体 盆腔炎 CD14型 流式细胞术 医学 体外 淋巴系统 表型 基因 生物化学 妇科
作者
Yee Teng Chan,Yi Ying Cheok,Heng Choon Cheong,Guan Huat Tan,Shi Rui Seow,Ting Tang,Sofiah Sulaiman,Chung Yeng Looi,Rishein Gupta,Bernard P. Arulanandam,Won Fen Wong
出处
期刊:Immunology and Cell Biology [Wiley]
卷期号:101 (4): 305-320
标识
DOI:10.1111/imcb.12621
摘要

Abstract Genital Chlamydia trachomatis infection remains a major health issue as it causes severe complications including pelvic inflammatory disease, ectopic pregnancy and infertility in females as a result of infection‐associated chronic inflammation. Podoplanin, a transmembrane receptor, has been previously reported on inflammatory macrophages. Thus, strategies that specifically target podoplanin might be able to reduce local inflammation. This study investigated the expression level and function of podoplanin in a C. trachomatis infection model. C57BL/6 mice infected with the mouse pathogen Chlamydia muridarum were examined intermittently from days 1 to 60 using flow cytometry analysis. Percentages of conventional macrophages (CD11b + CD11c − F4/80 + ) versus inflammatory macrophages (CD11b + CD11c + F4/80 + ), and the expression of podoplanin in these cells were investigated. Subsequently, a podoplanin‐knockout RAW264.7 cell was used to evaluate the function of podoplanin in C. trachomatis infection. Our findings demonstrated an increased CD11b + cell volume in the spleen at day 9 after the infection, with augmented podoplanin expression, especially among the inflammatory macrophages. A large number of podoplanin‐expressing macrophages were detected in the genital tract of C. muridarum –infected mice. Furthermore, analysis of the C. trachomatis –infected patients demonstrated a higher percentage of podoplanin‐expressing monocytes than that in the noninfected controls. Using an in vitro infection in a transwell migration assay, we identified that macrophages deficient in podoplanin displayed defective migratory function toward C. trachomatis –infected HeLa 229 cells. Lastly, using immunoprecipitation–mass spectrometry method, we identified two potential podoplanin interacting proteins, namely, Cofilin 1 and Talin 1 actin‐binding proteins. The present study reports a role of podoplanin in directing macrophage migration to the chlamydial infection site. Our results suggest a potential for reducing inflammation in individuals with chronic chlamydial infections by targeting podoplanin.
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