nvestigation The endogenous e pression of podoplanin on 293T cel

nvestigation. The endogenous e pression of podoplanin on 293T cells and the specific interaction of podoplanin with CLEC 2 raised the questions if podoplanin was incorpo rated into virions produced in 293T cells, and if incorpo ration of podoplanin was required for CLEC 2 binding of these virions. Western blot analysis and knock down of podoplanin e pression by shRNA provided affirmative answers to both questions Podoplanin depletion reduced CLEC 2, but not DC SIGN, dependent HIV 1 transmis sion by B THP cells, and diminished transmission by platelets by about 50%. The latter finding is in agreement with our previous observation that CLEC 2 specific antiserum reduced HIV 1 transmission by plate lets by about half.

Podoplanin therefore joins the list of host factors which can be incorporated into the HIV 1 envelope and impact HIV 1 infection by interacting with their cognate ligands. A prominent e ample for such a factor is ICAM 1 which was found to be incorpo rated into the viral membrane, and to facilitate HIV 1 infection by binding to its ligand LFA 1 on T cells. The potential relevance Anacetrapib of podoplanin incorporation for HIV spread in infected individuals is critically deter mined by the overlap of the podoplanin e pression pat tern with the cellular tropism of HIV. Analysis of T cell lines and PBMCs for podoplanin e pression yielded neg ative results, at least when viable cells were ana lyzed, indicating that HIV particles generated in patients might not harbour podoplanin. The e ception might be viruses released from kidney podocytes which have been documented to e press podoplanin and to be susceptible to HIV infection.

However, the biolog ical relevance of this process is questionable. In this con te t, it also needs to be noted that podoplanin e pression is up regulated in many tumours including Kaposi sar coma. Podoplanin CLEC 2 dependent platelet stimulation by tumour cells promotes hematogenous tumour metastasis, possibly by inducing growth factor secretion by platelets and by promoting formation of a platelet cap, which protects the tumour from mechanical forces. Thus, podoplanin might play a role in the development of the AIDS associated Kaposi sarcoma, but is unlikely to modulate HIV spread in patients.

Nev ertheless, HIV 1 produced in PBMCs was transmitted to target cells in a CLEC 2 dependent fashion, sug gesting that primary T cells might e press a so far unrec ognized CLEC 2 ligand, which is incorporated into the viral envelope and which facilitates HIV transmission by CLEC 2. Our ongoing studies are devoted to the identification of this factor. Podoplanin was not detected on viable CEM��174 cells and PBMCs, as determined by our gat ing strategy and by co staining with the apoptosis and necrosis markers anne in V and 7 AAD, respectively. In contrast, we observed efficient reactivity of two different podoplanin antibodies with non viable cells, raising the intriguing possibility that podoplanin might be e pressed at the cell surface i

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