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Small Dense Nuclear Bodies Are the Site of Localization of Herpes Simplex Virus 1 U(L)3 and U(L)4 Proteins and of ICP22 Only When the Latter Protein Is Present

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PubMed Central2026-05-16 收录
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https://pmc.ncbi.nlm.nih.gov/articles/PMC111565/
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The herpes simplex virus 1 U(L)3 and U(L)4 open reading frames are expressed late in infection and are not essential for viral replication in cultured cells in vitro. An earlier report showed that the U(L)4 protein colocalizes with the products of the α22/U(S)1.5 genes in small nuclear dense bodies. Here we report that the U(L)3 protein also colocalized in these small nuclear dense bodies and the localization of U(L)3 and U(L)4 proteins in these bodies required the presence of α22/U(S)1.5 genes. In cells infected with a mutant lacking intact α22/U(S)1.5 genes, U(L)3 was diffused throughout the nucleus even though the overall accumulation of the γ2 U(L)3 protein was decreased. The results suggest that ICP22 acts both as a regulator of U(L)3 accumulation and as the structural component and anchor of these small dense nuclear bodies.
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American Society for Microbiology (ASM)
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