The depletion of TFAM and p-β-catenin(S552) in mitochondria in response to BoAHV-1 productive infection leads to decreased mitochondrial biogenesis

IF 2.7 2区农林科学 Q3 MICROBIOLOGY Veterinary microbiology Pub Date : 2025-03-05 DOI:10.1016/j.vetmic.2025.110454

Jiayu Lin , Xiaotian Fu , Xuan Li , Xiuyan Ding , Shitao Li , Filomena Fiorito , Liqian Zhu

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Abstract

Varicellovirus bovinealpha (BoAHV) types 1(BoAHV-1) is one of the most significant viruses affecting cattle, causing substantial economic losses in the global cattle industry. Virus productive infection in cell cultures leads to mitochondrial dysfunction, resulting in the overproduction of reactive oxygen species (ROS), which act as inflammatory mediators and exert cytotoxic effects. But the underlying mechanisms remain poorly understood. Mitochondrial transcription factor A (TFAM) is a critical transcriptional activator of the mitochondrial DNA and plays a vital role in mitochondrial biogenesis. In this study, we report that virus acute infection in calves (at 4 days post-infection) increases TFAM protein expression and its accumulation in the peri-nuclear region in a subset of trigeminal ganglia (TG) neurons. Similarly, virus productive infection at later stages in MDBK cells also leads to increased TFAM protein expression and its accumulation in the nucleus. Using TFAM-specific siRNAs, we revealed that TFAM plays a significant role in BoAHV-1 productive infection. Consistent with decreased mitochondrial biogenesis, TFAM protein accumulation in mitochondria was significantly reduced following viral infection, which is corroborated by the reduced accumulation of TOM70 and Tim44 proteins in mitochondria. These proteins are key components of the mitochondrial membrane transport system that facilitates the translocation of TFAM into mitochondria. Interestingly, we found that a subset of β-catenin resides in mitochondria, and viral infection decreases the accumulation of transcriptionally active β-catenin, p-β-catenin(S552), in mitochondria. This may contribute to decreased mitochondrial biogenesis, as the β-catenin-specific inhibitor iCRT14 reduces the protein expression of Cytb, a key regulator of mitochondrial biosynthesis. Collectively, we suggest that the depletion of both TFAM and p-β-catenin(S552) in mitochondria may contribute to the mitochondrial dysfunction induced by BoAHV-1 productive infection.

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BoAHV-1产生性感染导致线粒体中TFAM和p-β-catenin（S552）的减少，导致线粒体生物发生减少

牛α水痘病毒（BoAHV） 1型（BoAHV-1）是影响牛的最重要病毒之一，给全球养牛业造成重大经济损失。细胞培养中的病毒产生性感染导致线粒体功能障碍，导致活性氧（ROS）过量产生，活性氧作为炎症介质并发挥细胞毒性作用。但人们对其潜在机制仍知之甚少。线粒体转录因子A （Mitochondrial transcription factor A， TFAM）是线粒体DNA的重要转录激活因子，在线粒体生物发生中起着至关重要的作用。在这项研究中，我们报告了小牛的病毒急性感染（感染后4天）增加了三叉神经节（TG）神经元子集核周围区域的TFAM蛋白表达及其积累。同样，MDBK细胞后期的病毒生产感染也导致TFAM蛋白表达增加及其在细胞核中的积累。利用TFAM特异性sirna，我们发现TFAM在BoAHV-1产生性感染中起重要作用。与线粒体生物发生减少一致，病毒感染后线粒体中TFAM蛋白的积累显著减少，线粒体中TOM70和Tim44蛋白的积累减少证实了这一点。这些蛋白质是线粒体膜运输系统的关键组成部分，促进TFAM转运到线粒体。有趣的是，我们发现β-catenin的一个子集存在于线粒体中，病毒感染减少了线粒体中转录活性β-catenin p-β-catenin（S552）的积累。这可能导致线粒体生物发生减少，因为β-catenin特异性抑制剂iCRT14降低了Cytb的蛋白表达，Cytb是线粒体生物合成的关键调节因子。总之，我们认为线粒体中TFAM和p-β-catenin（S552）的缺失可能导致BoAHV-1产生性感染诱导的线粒体功能障碍。

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来源期刊

Veterinary microbiology 农林科学-兽医学

CiteScore

5.90

自引率

6.10%

发文量

221

审稿时长

52 days

期刊介绍： Veterinary Microbiology is concerned with microbial (bacterial, fungal, viral) diseases of domesticated vertebrate animals (livestock, companion animals, fur-bearing animals, game, poultry, fish) that supply food, other useful products or companionship. In addition, Microbial diseases of wild animals living in captivity, or as members of the feral fauna will also be considered if the infections are of interest because of their interrelation with humans (zoonoses) and/or domestic animals. Studies of antimicrobial resistance are also included, provided that the results represent a substantial advance in knowledge. Authors are strongly encouraged to read - prior to submission - the Editorials (''Scope or cope'' and ''Scope or cope II'') published previously in the journal. The Editors reserve the right to suggest submission to another journal for those papers which they feel would be more appropriate for consideration by that journal. Original research papers of high quality and novelty on aspects of control, host response, molecular biology, pathogenesis, prevention, and treatment of microbial diseases of animals are published. Papers dealing primarily with immunology, epidemiology, molecular biology and antiviral or microbial agents will only be considered if they demonstrate a clear impact on a disease. Papers focusing solely on diagnostic techniques (such as another PCR protocol or ELISA) will not be published - focus should be on a microorganism and not on a particular technique. Papers only reporting microbial sequences, transcriptomics data, or proteomics data will not be considered unless the results represent a substantial advance in knowledge. Drug trial papers will be considered if they have general application or significance. Papers on the identification of microorganisms will also be considered, but detailed taxonomic studies do not fall within the scope of the journal. Case reports will not be published, unless they have general application or contain novel aspects. Papers of geographically limited interest, which repeat what had been established elsewhere will not be considered. The readership of the journal is global.