鼻病毒16型2A蛋白酶在感染过程中影响3CD的核定位。
Rhinovirus 16 2A Protease Affects Nuclear Localization of 3CD during Infection.
作者信息
Walker Erin, Jensen Lora, Croft Sarah, Wei Kejun, Fulcher Alex J, Jans David A, Ghildyal Reena
机构信息
Centre for Research in Therapeutic Solutions, University of Canberra, Canberra, Australian Capital Territory, Australia.
Department of Biochemistry and Molecular Biology, Monash University, Clayton, Victoria, Australia.
出版信息
J Virol. 2016 Nov 28;90(24):11032-11042. doi: 10.1128/JVI.00974-16. Print 2016 Dec 15.
UNLABELLED
The human rhinovirus (HRV) 3C and 2A proteases (3C and 2A, respectively) are critical in HRV infection, as they are required for viral polyprotein processing as well as proteolysing key host factors to facilitate virus replication. Early in infection, 3C is present as its precursor 3CD, which, although the mechanism of subcellular targeting is unknown, is found in the nucleus as well as the cytoplasm. In this study, we use transfected and infected cell systems to show that 2A activity is required for 3CD nuclear localization. Using green fluorescent protein (GFP)-tagged forms of 3C, 3D, and mutant derivatives thereof, we show that 3C is located in the cytoplasm and the nucleus, whereas 3CD and 3D are localized predominantly in the cytoplasm, implying that 3D lacks nuclear targeting ability and that 3C activity within 3CD is not sufficient to allow the larger protein into the nucleus. Importantly, by coexpressing mCherry-2A fusion proteins, we demonstrate formally that 2A activity is required to allow HRV 3CD access to the nucleus. In contrast, mCherry-3C is insufficient to allow 3CD access to the nucleus. Finally, we confirm the relevance of these results to HRV infection by demonstrating that nuclear localization of 3CD correlates with 2A activity and not 3C activity, which is observed only later in infection. The results thus define the temporal activities of 2A and 3CD/3C activities in HRV serotype16 infection.
IMPORTANCE
The human rhinovirus genome encodes two proteases, 2A and 3C, as well as a precursor protease, 3CD. These proteases are essential for efficient virus replication. The 3CD protein is found in the nucleus early during infection, though the mechanism of subcellular localization is unknown. Here we show that 2A protease is required for this localization, the 3C protease activity of 3CD is not sufficient to allow 3CD entry into the nucleus, and 3D lacks nuclear targeting ability. This study demonstrates that both 2A and 3C proteases are required for the correct localization of proteins during infection and defines the temporal regulation of 2A and 3CD/3C protease activities during HRV16 infection.
未标记
人鼻病毒(HRV)的3C蛋白酶和2A蛋白酶(分别为3C和2A)在HRV感染过程中至关重要,因为它们对于病毒多聚蛋白的加工以及裂解关键宿主因子以促进病毒复制是必需的。在感染早期,3C以其前体3CD的形式存在,尽管其亚细胞靶向机制尚不清楚,但在细胞核和细胞质中均能发现。在本研究中,我们利用转染和感染的细胞系统表明,2A活性是3CD核定位所必需的。使用绿色荧光蛋白(GFP)标记的3C、3D及其突变衍生物形式,我们发现3C位于细胞质和细胞核中,而3CD和3D主要定位于细胞质中,这意味着3D缺乏核靶向能力,并且3CD中的3C活性不足以使较大的蛋白进入细胞核。重要的是,通过共表达mCherry-2A融合蛋白,我们正式证明2A活性是使HRV 3CD进入细胞核所必需的。相比之下,mCherry-3C不足以使3CD进入细胞核。最后,我们通过证明3CD的核定位与2A活性相关而非3C活性(3C活性仅在感染后期才观察到),证实了这些结果与HRV感染的相关性。因此,这些结果确定了2A和3CD/3C活性在HRV 16型感染中的时间活性。
重要性
人鼻病毒基因组编码两种蛋白酶,2A和3C,以及一种前体蛋白酶3CD。这些蛋白酶对于有效的病毒复制至关重要。在感染早期能在细胞核中发现3CD蛋白,但其亚细胞定位机制尚不清楚。在这里我们表明这种定位需要2A蛋白酶,3CD的3C蛋白酶活性不足以使3CD进入细胞核,并且3D缺乏核靶向能力。这项研究表明,2A和3C蛋白酶在感染期间对于蛋白质的正确定位都是必需的,并确定了HRV 16感染期间2A和3CD/3C蛋白酶活性的时间调控。
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