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流行性卡波西肉瘤中独特的循环微小RNA谱

Unique circulating microRNA profiles in epidemic Kaposi's sarcoma.

作者信息

Muwonge Haruna, Kasujja Hassan, Niyonzima Nixon, Atugonza Carolyne, Kasolo Josephine, Lugaajju Allan, Nfambi Joshua, Fred Sembajwe Larry, Damani Ali Moses, Kimuli Ivan, Zavuga Robert, Nakazzi Faith, Kigozi Edgar, Nakanjako Damalie, Kateete David Patrick, Bwanga Freddie

机构信息

Department of Physiology, School of Biomedical Sciences, Makerere University College of Health Sciences, P. O Box 7072, Kampala, Uganda.

Habib Medical School, Islamic University in Uganda (IUIU), Uganda.

出版信息

Noncoding RNA Res. 2022 Apr 10;7(2):114-122. doi: 10.1016/j.ncrna.2022.02.002. eCollection 2022 Jun.

Abstract

BACKGROUND

Human herpesvirus 8 (HHV-8) causes Kaposi's sarcoma (KS). Kaposi sarcoma in HIV/AIDS patients is referred to as epidemic KS and is the most common HIV-related malignancy worldwide. The lack of a diagnostic assay to detect latent and early-stage disease has increased disease morbidity and mortality. Serum miRNAs have previously been used as potential biomarkers of normal physiology and disease. In the current study, we profiled unique serum miRNAs in patients with epidemic KS to generate baseline data to aid in developing a miRNA-based noninvasive biomarker assay for epidemic KS.

METHODS

This was a comparative cross-sectional study involving 27 patients with epidemic KS and 27 HIV-positive adults with no prior diagnosis or clinical manifestation of KS. DNA and RNA were isolated from blood and serum collected from study participants. Nested PCR for circulating HHV-8 DNA was performed on the isolated DNA, whereas miRNA library preparation and sequencing for circulating miRNA were performed on the RNA samples. The miRge2 pipeline and EdgeR were used to analyse the sequencing data.

RESULTS

Fifteen out of the 27 epidemic KS-positive subjects (55.6%) tested positive for HHV-8 DNA, whereas only 3 (11.1%) out of the 27 HIV-positive, KS-negative subjects tested positive for HHV-8 DNA. Additionally, we found a unique miRNA expression signature in 49 circulating miRNAs in epidemic KS subjects compared to subjects with no epidemic KS, with 41 miRNAs upregulated and 8 miRNAs downregulated. Subjects with latent KS infection had a differential upregulation of circulating miR-193a compared to HIV-positive, KS-negative subjects for whom circulating HHV-8 DNA was not detected. Further analysis of serum from epidemic KS patients revealed a miRNA signature according to KS tumor status and time since first HIV diagnosis.

CONCLUSIONS

This study reveals unique circulating miRNA profiles in the serum of patients with epidemic KS versus HIV-infected subjects with no KS, as well as in subjects with latent KS. Many of the dysregulated miRNAs in epidemic KS patients were previously reported to have crucial roles in KS infection and latency, highlighting their promising roles as potential biomarkers of latent or active KS infection.

摘要

背景

人类疱疹病毒8型(HHV-8)可引发卡波西肉瘤(KS)。HIV/AIDS患者中的卡波西肉瘤被称为流行性KS,是全球最常见的与HIV相关的恶性肿瘤。缺乏用于检测潜伏性和早期疾病的诊断检测方法增加了疾病的发病率和死亡率。血清微小RNA(miRNA)此前已被用作正常生理和疾病的潜在生物标志物。在本研究中,我们分析了流行性KS患者独特的血清miRNA,以生成基线数据,有助于开发基于miRNA的流行性KS非侵入性生物标志物检测方法。

方法

这是一项比较性横断面研究,纳入了27例流行性KS患者和27例既往未诊断或无KS临床表现的HIV阳性成年人。从研究参与者采集的血液和血清中分离DNA和RNA。对分离出的DNA进行巢式PCR检测循环中的HHV-8 DNA,而对RNA样本进行循环miRNA的文库制备和测序。使用miRge2流程和EdgeR分析测序数据。

结果

27例流行性KS阳性受试者中有15例(55.6%)HHV-8 DNA检测呈阳性,而27例HIV阳性、KS阴性受试者中只有3例(11.1%)HHV-8 DNA检测呈阳性。此外,与无流行性KS的受试者相比,我们在流行性KS受试者的49种循环miRNA中发现了独特的miRNA表达特征,其中41种miRNA上调,8种miRNA下调。与未检测到循环HHV-8 DNA的HIV阳性、KS阴性受试者相比,潜伏性KS感染的受试者循环miR-193a有差异上调。对流行性KS患者血清的进一步分析揭示了根据KS肿瘤状态和首次HIV诊断后的时间得出的miRNA特征。

结论

本研究揭示了流行性KS患者与无KS的HIV感染受试者以及潜伏性KS受试者血清中独特的循环miRNA谱。流行性KS患者中许多失调的miRNA此前被报道在KS感染和潜伏中起关键作用,突出了它们作为潜伏性或活动性KS感染潜在生物标志物的有前景的作用。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/172b/9065625/ac355feff54c/gr1.jpg

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