基于全转录组测序的继发性免疫缺陷患者皮肤病毒组特征分析

Leila Youssefian , Amir Hossein Saeidian , Zahra Saffarian , Mona Ariamanesh , Fahimeh Abdollahimajd , Sara Molkara , Mohammad Shahidi-Dadras , Reem Diab , Fatemeh Vahidnezhad , Sirous Zeinali , Vivien Béziat , Emmanuelle Jouanguy , Jean-Laurent Casanova , Jouni Uitto , Hassan Vahidnezhad
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引用次数: 0

摘要

大多数病毒感染都是自限性的,无需医疗干预。然而,对于因单基因疾病、获得性免疫缺陷综合征、血液系统恶性肿瘤或接受免疫抑制药物治疗而导致免疫力低下的患者来说,同样的病毒也会引起严重的疾病。有时,这些免疫力低下的患者会携带一种传染病原,需要同时进行多项诊断检测。据我们所知,我们已经开发出一种以前从未报道过的基于全转录组测序的方法,通过对从单个病变皮肤活检组织中分离出的 RNA 进行测序,可以对 926 种不同病毒进行病毒组分析、定量和表达模式分析。如果存在孟德尔感染易感性,该方法还能探索宿主遗传学。我们对 6 名伊朗患者应用了这一方法,这些患者的皮肤病变是由病毒引起的,与继发于 HIV、人类 T 淋巴细胞病毒 1、慢性淋巴细胞白血病和移植后免疫抑制的免疫缺陷有关。在 5 个病例中,发现了明确的人类乳头瘤病毒感染,其中一些是由多种病毒引起的。除人类乳头瘤病毒外,在一些病变中还发现了与其他病毒(梅克尔细胞多瘤病毒、巨细胞病毒和人类疱疹病毒 4)的合并感染。在一个病例中,全转录组测序验证了初步诊断为真菌病/塞扎里综合征的患者的成人T细胞白血病/淋巴瘤临床诊断。这些发现证明了全转录组测序在分析免疫受损情况下的皮肤病毒组方面的强大功能。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Whole-Transcriptome Sequencing–Based Profiling of the Cutaneous Virome in Patients with Secondary Immunodeficiency

Most viral infections can be self-limited, with no requirement for medical intervention. However, the same viruses can cause severe diseases in patients with compromised immunity due to single-gene diseases, acquired immune deficiency syndrome, or hematologic malignancies or those receiving immunosuppressive drugs. Occasionally, these immunocompromised patients harbor >1 infectious agent, requiring several concomitant diagnostic tests. We have developed, to our knowledge, a previously unreported whole-transcriptome sequencing–based pipeline that allows virome profiling, quantitation, and expression pattern analysis of 926 distinct viruses by sequencing of RNA isolated from a single lesional skin biopsy. This pipeline can also explore host genetics if there is a Mendelian predisposition to infection. We applied this pipeline to 6 Iranian patients with viral-induced skin lesions associated with immune deficiency secondary to HIV, human T-lymphotropic virus 1, chronic lymphocytic leukemia, and post transplant immunosuppression. In 5 cases, definitive human papillomavirus infections were identified, some caused by multiple viral types. In addition to human papillomavirus, coinfection with other viruses (Merkle cell polyomavirus, cytomegalovirus, and human herpesvirus 4) was detected in some lesions. In 1 case, whole-transcriptome sequencing validated the clinical diagnosis of adult T-cell leukemia/lymphoma in a patient with an initial diagnosis of mycosis fungoides/Sézary syndrome. These findings attest to the power of whole-transcriptome sequencing in profiling the cutaneous virome in the context of compromised immunity.

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