比较极性和脂质血浆代谢组学可区分KSHV感染和疾病状态。

IF 6 3区 医学 Q1 CELL BIOLOGY Cancer & Metabolism Pub Date : 2023-08-31 DOI:10.1186/s40170-023-00316-0
Sara R Privatt, Camila Pereira Braga, Alicia Johnson, Salum J Lidenge, Luke Berry, John R Ngowi, Owen Ngalamika, Andrew G Chapple, Julius Mwaiselage, Charles Wood, John T West, Jiri Adamec
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引用次数: 0

摘要

背景:卡波西肉瘤(KS)是一种与卡波西肉瘤相关疱疹病毒(KSHV)感染相关的肿瘤性疾病。KS主要表现为个体由于年龄(经典KS)、HIV感染(流行病KS)或移植中的组织排斥预防(病源性KS)引起的皮肤病变,但也可能发生在个体中,主要发生在撒哈拉以南非洲(SSA),缺乏任何明显的免疫抑制(地方性KS)。非洲KSHV和人类免疫缺陷病毒-1 (HIV)合并感染的高流行率导致KS成为那里的五大癌症之一。与大多数病毒性癌症一样,仅感染KSHV不足以诱导肿瘤发生。事实上,KSHV感染原代人内皮细胞培养物,即使在高水平,也很少与长期培养、转化或生长失调有关,但体内感染是终身持续的。对区分KSHV感染、KSHV/HIV合并感染和症状性KS疾病的免疫介质的研究尚未揭示对KS的保护或进展的一致相关性。除了病毒感染外,KS肿瘤的发病机制似乎还需要一个允许内皮细胞异常生长的免疫和代谢环境。在这项研究中,我们探讨了血浆代谢组学是否可以区分有无HIV合并感染的无症状kshv感染者和有症状的KS。方法:为了研究代谢变化与合并感染和肿瘤发生之间的关系,三组KSHV血清阳性的撒哈拉以南非洲受试者的血浆样本(A)无症状(无肿瘤疾病)仅感染KSHV, (B)无症状合并感染KSHV和HIV, (C)有症状并临床诊断为KS,分析脂质和极性代谢物谱。极性和非极性血浆代谢差异在两种比较中都很明显。代谢研究结果与我们之前报道的KS转录组学数据相结合,表明氨基酸/尿素循环和嘌呤代谢途径失调,与病毒感染在KS疾病进展中一致。结论:据我们所知,本研究首次报道了体内KSHV感染与HIV合并感染之间的血浆代谢差异,以及合并感染与流行KS之间的差异。
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Comparative polar and lipid plasma metabolomics differentiate KSHV infection and disease states.

Background: Kaposi sarcoma (KS) is a neoplastic disease etiologically associated with infection by the Kaposi sarcoma-associated herpesvirus (KSHV). KS manifests primarily as cutaneous lesions in individuals due to either age (classical KS), HIV infection (epidemic KS), or tissue rejection preventatives in transplantation (iatrogenic KS) but can also occur in individuals, predominantly in sub-Saharan Africa (SSA), lacking any obvious immune suppression (endemic KS). The high endemicity of KSHV and human immunodeficiency virus-1 (HIV) co-infection in Africa results in KS being one of the top 5 cancers there. As with most viral cancers, infection with KSHV alone is insufficient to induce tumorigenesis. Indeed, KSHV infection of primary human endothelial cell cultures, even at high levels, is rarely associated with long-term culture, transformation, or growth deregulation, yet infection in vivo is sustained for life. Investigations of immune mediators that distinguish KSHV infection, KSHV/HIV co-infection, and symptomatic KS disease have yet to reveal consistent correlates of protection against or progression to KS. In addition to viral infection, it is plausible that pathogenesis also requires an immunological and metabolic environment permissive to the abnormal endothelial cell growth evident in KS tumors. In this study, we explored whether plasma metabolomes could differentiate asymptomatic KSHV-infected individuals with or without HIV co-infection and symptomatic KS from each other.

Methods: To investigate how metabolic changes may correlate with co-infections and tumorigenesis, plasma samples derived from KSHV seropositive sub-Saharan African subjects in three groups, (A) asymptomatic (lacking neoplastic disease) with KSHV infection only, (B) asymptomatic co-infected with KSHV and HIV, and (C) symptomatic with clinically diagnosed KS, were subjected to analysis of lipid and polar metabolite profiles RESULTS: Polar and nonpolar plasma metabolic differentials were evident in both comparisons. Integration of the metabolic findings with our previously reported KS transcriptomics data suggests dysregulation of amino acid/urea cycle and purine metabolic pathways, in concert with viral infection in KS disease progression.

Conclusions: This study is, to our knowledge, the first to report human plasma metabolic differentials between in vivo KSHV infection and co-infection with HIV, as well as differentials between co-infection and epidemic KS.

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来源期刊
自引率
1.70%
发文量
17
审稿时长
14 weeks
期刊介绍: Cancer & Metabolism welcomes studies on all aspects of the relationship between cancer and metabolism, including: -Molecular biology and genetics of cancer metabolism -Whole-body metabolism, including diabetes and obesity, in relation to cancer -Metabolomics in relation to cancer; -Metabolism-based imaging -Preclinical and clinical studies of metabolism-related cancer therapies.
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