Expression of GPR56 reflects a hypoactivated state of circulating B cells and is downregulated in B cell subsets in patients with early‐stage lung adenocarcinoma

Author:

Bahabayi Ayibaota1,Guan Zhao1,Zheng Mohan12,Yu He1,Hasimu Ainizati1,Nie Yuying1,Zhao Ming1,Zhu Yaoyi1,Ren Jiaxin1,Zhao Yiming1,Ma Xiancan1,Li Qi1,Zhang Zhonghui1,Zeng Xingyue1,Liu Chen1ORCID

Affiliation:

1. Department of Clinical Laboratory Peking University People's Hospital Beijing China

2. School of Basic Medical Sciences Peking University Health Science Center Beijing China

Abstract

AbstractLung adenocarcinoma (LUAD) is the most prevalent subtype of lung cancer, and the early detection and diagnosis of this disease are crucial in reducing mortality rates. The timely diagnosis of LUAD is essential for controlling tumour development and enabling early surgical treatment. GPR56 is a vital G protein‐coupled receptor and its role in T lymphocytes has received considerable attention. However, its function in B cells remains unclear. This study aimed to investigate the significance of GPR56 in LUAD. We found that GPR56 exhibited a significant increase in circulating plasmablasts and a decrease in new memory B cells. GPR56 expression in B cells was significantly reduced after LPS stimulation and the proportion of HLA‐DR+ and CD40+ proportions were also decreased in GPR56+ B cells after stimulation. Additionally, GPR56 exhibited significant down‐regulation in circulating B cell subsets of early‐stage LUAD patients, and there were significant correlations between GPR56+ B cell subsets and tumour markers. In conclusion, GPR56 could reflect the hypoactivation state of B cells and the decreased proportion of GPR56+ B cell subset in LUAD patients can signify the active humoral immunity in vivo. The expression of GPR56 in B cells could potentially hold value in the early diagnosis of LUAD.

Funder

National Natural Science Foundation of China

Publisher

Wiley

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