Author: Schmidt, Sarah; Schenkova, Kristina; Adam, Tarek; Erikson, Elina; Lehmannâ€Koch, Judith; Sertel, Serkan; Verhasselt, Bruno; Fackler, Oliver T.; Lasitschka, Felix; Keppler, Oliver T.
Title: SAMHD1's protein expression profile in humans Cord-id: 4lh2swjd Document date: 2015_2_2
ID: 4lh2swjd
Snippet: The deoxynucleoside triphosphate triphosphohydrolase and 3′ → 5′ exonuclease SAMHD1 restricts HIVâ€1 infection in noncycling hematopoietic cells in vitro, and SAMHD1 mutations are associated with AGS. Little is known about the in vivo expression and functional regulation of this cellular factor. Here, we first assessed the SAMHD1 protein expression profile on a microarray of 25 human tissues from >210 donors and in purified primary cell populations. In vivo, SAMHD1 was expressed in the ma
Document: The deoxynucleoside triphosphate triphosphohydrolase and 3′ → 5′ exonuclease SAMHD1 restricts HIVâ€1 infection in noncycling hematopoietic cells in vitro, and SAMHD1 mutations are associated with AGS. Little is known about the in vivo expression and functional regulation of this cellular factor. Here, we first assessed the SAMHD1 protein expression profile on a microarray of 25 human tissues from >210 donors and in purified primary cell populations. In vivo, SAMHD1 was expressed in the majority of nucleated cells of hematopoietic origin, including tissueâ€resident macrophages, DCs, pDCs, all developmental stages of thymic T cells, monocytes, NK cells, as well as at lower levels in B cells. Of note, SAMHD1 was abundantly expressed in HIV target cells residing in the anogenital mucosa, providing a basis for its evaluation as a cellular factor that may impact the efficiency of HIV transmission. Next, we examined the effect of the activation status and proinflammatory cytokine treatment of cells on expression and phosphorylation of SAMHD1. Activated, HIVâ€susceptible CD4(+) T cells carried pSAMHD1(T592), whereas resting CD4(+) T cells and macrophages expressed the unphosphorylated protein with HIVâ€restrictive activity. Surprisingly, stimulation of these primary cells with IFNâ€Î±, IFNâ€Î³, ILâ€4, ILâ€6, ILâ€12, ILâ€18, ILâ€27, or TNFâ€Î± affected neither SAMHD1 expression levels nor threonine 592 phosphorylation. Only ILâ€1β moderately downâ€regulated SAMHD1 in activated CD4(+) T cells. Taken together, this study establishes the first crossâ€sectional protein expression profile of SAMHD1 in human tissues and provides insight into its cell cycleâ€dependent phosphorylation and unresponsiveness to multiple proinflammatory cytokines.
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