Sanchez Erica L, Carroll Patrick A, Thalhofer Angel B, Lagunoff Michael
Molecular and Cellular Biology Program, University of Washington, Seattle, Washington, United States of America; Department of Microbiology, University of Washington, Seattle, Washington, United States of America.
Fred Hutchinson Cancer Research Center, Seattle, Washington, United States of America.
PLoS Pathog. 2015 Jul 21;11(7):e1005052. doi: 10.1371/journal.ppat.1005052. eCollection 2015 Jul.
Kaposi's Sarcoma-associated Herpesvirus (KSHV) is the etiologic agent of Kaposi's Sarcoma (KS). KSHV establishes a predominantly latent infection in the main KS tumor cell type, the spindle cell, which is of endothelial cell origin. KSHV requires the induction of multiple metabolic pathways, including glycolysis and fatty acid synthesis, for the survival of latently infected endothelial cells. Here we demonstrate that latent KSHV infection leads to increased levels of intracellular glutamine and enhanced glutamine uptake. Depletion of glutamine from the culture media leads to a significant increase in apoptotic cell death in latently infected endothelial cells, but not in their mock-infected counterparts. In cancer cells, glutamine is often required for glutaminolysis to provide intermediates for the tri-carboxylic acid (TCA) cycle and support for the production of biosynthetic and bioenergetic precursors. In the absence of glutamine, the TCA cycle intermediates alpha-ketoglutarate (αKG) and pyruvate prevent the death of latently infected cells. Targeted drug inhibition of glutaminolysis also induces increased cell death in latently infected cells. KSHV infection of endothelial cells induces protein expression of the glutamine transporter, SLC1A5. Chemical inhibition of SLC1A5, or knockdown by siRNA, leads to similar cell death rates as glutamine deprivation and, similarly, can be rescued by αKG. KSHV also induces expression of the heterodimeric transcription factors c-Myc-Max and related heterodimer MondoA-Mlx. Knockdown of MondoA inhibits expression of both Mlx and SLC1A5 and induces a significant increase in cell death of only cells latently infected with KSHV, again, fully rescued by the supplementation of αKG. Therefore, during latent infection of endothelial cells, KSHV activates and requires the Myc/MondoA-network to upregulate the glutamine transporter, SLC1A5, leading to increased glutamine uptake for glutaminolysis. These findings expand our understanding of the required metabolic pathways that are activated during latent KSHV infection of endothelial cells, and demonstrate a novel role for the extended Myc-regulatory network, specifically MondoA, during latent KSHV infection.
卡波西肉瘤相关疱疹病毒(KSHV)是卡波西肉瘤(KS)的病原体。KSHV在主要的KS肿瘤细胞类型即纺锤状细胞中建立了主要的潜伏感染,纺锤状细胞起源于内皮细胞。KSHV需要诱导多种代谢途径,包括糖酵解和脂肪酸合成,以维持潜伏感染的内皮细胞的存活。在此,我们证明潜伏的KSHV感染会导致细胞内谷氨酰胺水平升高以及谷氨酰胺摄取增强。从培养基中去除谷氨酰胺会导致潜伏感染的内皮细胞凋亡性细胞死亡显著增加,但未感染的对照细胞则不会。在癌细胞中,谷氨酰胺分解通常需要谷氨酰胺来为三羧酸(TCA)循环提供中间体,并支持生物合成和生物能量前体的产生。在缺乏谷氨酰胺的情况下,TCA循环中间体α-酮戊二酸(αKG)和丙酮酸可防止潜伏感染细胞死亡。对谷氨酰胺分解的靶向药物抑制也会诱导潜伏感染细胞的细胞死亡增加。内皮细胞的KSHV感染会诱导谷氨酰胺转运蛋白SLC1A5的蛋白表达。对SLC1A5进行化学抑制或通过小干扰RNA(siRNA)敲低,会导致与谷氨酰胺剥夺相似的细胞死亡率,同样,αKG可以挽救这种情况。KSHV还会诱导异二聚体转录因子c-Myc-Max和相关异二聚体MondoA-Mlx的表达。敲低MondoA会抑制Mlx和SLC1A5两者的表达,并仅在潜伏感染KSHV的细胞中诱导细胞死亡显著增加,同样,补充αKG可完全挽救这种情况。因此,在内皮细胞的潜伏感染期间,KSHV激活并需要Myc/MondoA网络来上调谷氨酰胺转运蛋白SLC1A5,从而导致谷氨酰胺摄取增加以进行谷氨酰胺分解。这些发现扩展了我们对内皮细胞潜伏KSHV感染期间激活的所需代谢途径的理解,并证明了扩展的Myc调节网络,特别是MondoA,在潜伏KSHV感染期间的新作用。
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