Benzo[a]pyrene exposure causes exonal switch resulting in reduced surface CD5 expression in an AHR-dependent manner

IF 3.3 4区 医学 Q3 IMMUNOLOGY Immunology letters Pub Date : 2024-04-16 DOI:10.1016/j.imlet.2024.106858
Smita Kumari , Bharat Singh , Amit Kumar Kureel , Sheetal Saini , Satya Prakash , Aditi Chauhan , Prabin Kumar , Kulwant Singh , Ambak Kumar Rai
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Abstract

The function of CD5 protein in T cells is well documented, but regulation of its surface-level expression has yet to be fully understood. However, variation in its surface expression is associated with various immunopathological conditions and haematological malignancies. Briefly, expression of an alternate exon E1B of a human endogenous retroviruses (HERV) origin directly downregulates the conventional transcript variant (E1A), as its expression leads to the retention of the resultant protein at the intracellular level (cCD5). A separate promoter governs the expression of E1B and may be influenced by different transcription factors. Hence, we performed in silico transcription factor binding site (TFBS) analysis of the 3 kb upstream region from TSS of exon E1B and found five putative DREs (Dioxin Response elements) with good similarity scores. Further, we observed the upregulation in E1B expression after the exposure of BaP (a dioxin) and the reduction of E1A expression and their respective protein, i.e. sCD5 and cCD5. The binding of AHR at the predicted DRE sites was confirmed by ChIP qPCR and AHR specific inhibitor and gene silencing studies suggested the involvement of AHR in exonal switch. This study indicates that the polycyclic aromatic hydrocarbon decreases the sCD5 expression by upregulating alternative exon expression, which may adversely affect the overall T cell functions.

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苯并[a]芘暴露会导致外激素转换,从而以 AHR 依赖性方式减少表面 CD5 的表达
CD5 蛋白在 T 细胞中的功能已得到充分证实,但对其表面表达的调控仍有待全面了解。然而,其表面表达的变化与各种免疫病理状况和血液恶性肿瘤有关。简而言之,人类内源性逆转录病毒(HERV)起源的交替外显子 E1B 的表达会直接下调常规转录本变体(E1A),因为它的表达会导致所产生的蛋白质保留在细胞内水平(cCD5)。E1B 的表达由另一个启动子控制,可能受到不同转录因子的影响。因此,我们对从 E1B 外显子 TSS 开始的 3 kb 上游区域进行了转录因子结合位点(TFBS)分析,发现了五个具有良好相似性的假定 DRE(二恶英反应元件)。此外,我们观察到暴露于二恶英 BaP 后 E1B 的表达上调,而 E1A 的表达和它们各自的蛋白(即 sCD5 和 cCD5)均下降。ChIP qPCR 证实了 AHR 与预测的 DRE 位点的结合,AHR 特异性抑制剂和基因沉默研究表明 AHR 参与了外激素的转换。这项研究表明,多环芳烃通过上调替代外显子的表达来降低 sCD5 的表达,这可能会对 T 细胞的整体功能产生不利影响。
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来源期刊
Immunology letters
Immunology letters 医学-免疫学
CiteScore
7.60
自引率
0.00%
发文量
86
审稿时长
44 days
期刊介绍: Immunology Letters provides a vehicle for the speedy publication of experimental papers, (mini)Reviews and Letters to the Editor addressing all aspects of molecular and cellular immunology. The essential criteria for publication will be clarity, experimental soundness and novelty. Results contradictory to current accepted thinking or ideas divergent from actual dogmas will be considered for publication provided that they are based on solid experimental findings. Preference will be given to papers of immediate importance to other investigators, either by their experimental data, new ideas or new methodology. Scientific correspondence to the Editor-in-Chief related to the published papers may also be accepted provided that they are short and scientifically relevant to the papers mentioned, in order to provide a continuing forum for discussion.
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