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单细胞 RNA 测序揭示了膀胱炎腺病中的免疫微环境和信号网络。

Single-cell RNA sequencing reveals the immune microenvironment and signaling networks in cystitis glandularis.

机构信息

Department of Urology, Xiangya Hosipital Central South University, Changsha, Hunan, China.

出版信息

Front Immunol. 2023 Feb 6;14:1083598. doi: 10.3389/fimmu.2023.1083598. eCollection 2023.

Abstract

INTRODUCTION

Cystitis glandularis (CG) is a rare chronic bladder hyperplastic disease that mainly manifests by recurrent frequent urination, dysuria and gross hematuria. The current lack of unified diagnosis and treatment criteria makes it essential to comprehensively describe the inflammatory immune environment in CG research.

METHODS

Here, we performed scRNA-sequencing in CG patients for the first time, in which four inflamed tissues as well as three surrounding normal bladder mucosa tissues were included. Specifically, we isolated 18,869 cells to conduct bioinformatic analysis and performed immunofluorescence experiments.

RESULTS

Our genetic results demonstrate that CG does not have the classic chromosomal variation observed in bladder tumors, reveal the specific effects of TNF in KRT15 epithelial cells, and identify a new population of PIGR epithelial cells with high immunogenicity. In addition, we confirmed the activation difference of various kinds of T cells during chronic bladder inflammation and discovered a new group of CD27-Switch memory B cells expressing a variety of immunoglobulins.

DISCUSSION

CG was regarded as a rare disease and its basic study is still weak.Our study reveals, for the first time, the different kinds of cell subgroups in CG and provides the necessary basis for the clinical treatment of cystitis glandularis. Besides, our study significantly advances the research on cystitis glandularis at the cellular level and provides a theoretical basis for the future treatment of cystitis glandularis.

摘要

简介

腺性膀胱炎(CG)是一种罕见的慢性膀胱增生性疾病,主要表现为反复发作的尿频、尿痛和肉眼血尿。目前缺乏统一的诊断和治疗标准,因此在 CG 研究中全面描述炎症免疫环境至关重要。

方法

我们首次对 CG 患者进行了 scRNA-seq 分析,其中包括四个炎症组织和三个周围正常膀胱黏膜组织。具体来说,我们分离了 18869 个细胞进行生物信息学分析,并进行了免疫荧光实验。

结果

我们的遗传学结果表明,CG 没有膀胱癌中观察到的经典染色体变异,揭示了 TNF 在 KRT15 上皮细胞中的特定作用,并鉴定了一种具有高免疫原性的新型 PIGR 上皮细胞群。此外,我们证实了慢性膀胱炎症中各种 T 细胞的激活差异,并发现了一组新的表达各种免疫球蛋白的 CD27-Switch 记忆 B 细胞。

讨论

CG 被认为是一种罕见疾病,其基础研究仍然薄弱。我们的研究首次揭示了 CG 中的不同细胞亚群,为 CG 的临床治疗提供了必要的基础。此外,我们的研究在细胞水平上显著推进了 CG 的研究,并为未来 CG 的治疗提供了理论依据。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/ca1a/9940314/6a6dc0affac1/fimmu-14-1083598-g001.jpg

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