TLiSA1 (PTA1) Activation Antigen Implicated in T Cell Differentiation and Platelet Activation Is a Member of the Immunoglobulin Superfamily Exhibiting Distinctive Regulation of Expression

Sherrington, Paul D.; Scott, Judith L.; Jin, Boquan; Simmons, David L.; Dorahy, Douglas J.; Lloyd, Jennifer; Brien, J. H.; Aebersold, Ruedi; Adamson, Janet; Zuzel, Mirko; Burns, Gordon F.

doi:10.1074/jbc.272.35.21735

Cited by 42 publications

(30 citation statements)

References 36 publications

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“…PTA-1 cDNA was subcloned into the high expression level eukaryotic vector, pEF-BOS, as described previously (54). The permanent Jurkat-PTA-1 cell line was established using the LipofectAMINE™ 2000 reagent (Invitrogen) to introduce a 10:1 excess of the pEF-BOS-PTA-1 vector (which lacks a eukaryotic selection marker) to pREP9 (which encodes neomycin phosphotransferase; Invitrogen), followed by selection with 750 g/ml G-418 (Invitrogen).…”

Section: Methodsmentioning

confidence: 99%

“…PTA-1 (also known as CD226, TLiSA-1, and DNAM-1) is a member of the immunoglobulin superfamily, the expression of which is regulated by phorbol ester and calcium (53,54). Initially identified as a T cell activation antigen, antibodies and F(abЈ) 2 fragments against PTA-1 inhibit the development of cytotoxic T cells and T cell clones from their precursors (55)(56)(57).…”

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confidence: 99%

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The LFA-1-associated Molecule PTA-1 (CD226) on T Cells Forms a Dynamic Molecular Complex with Protein 4.1G and Human Discs Large

Ralston

Hird

Zhang

et al. 2004

Journal of Biological Chemistry

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Clustering of the T cell integrin, LFA-1, at specialized regions of intercellular contact initiates integrin-mediated adhesion and downstream signaling, events that are necessary for a successful immunological response. But how clustering is achieved and sustained is not known. Here we establish that an LFA-1-associated molecule, PTA-1, is localized to membrane rafts and binds the carboxyl-terminal domain of isoforms of the actinbinding protein 4.1G. Protein 4.1 is known to associate with the membrane-associated guanylate kinase homologue, human discs large. We show that the carboxylterminal peptide of PTA-1 also can bind human discs large and that the presence or absence of this peptide greatly influences binding between PTA-1 and different isoforms of 4.1G. T cell stimulation with phorbol ester or PTA-1 cross-linking induces PTA-1 and 4.1G to associate tightly with the cytoskeleton, and the PTA-1 from such activated cells now can bind to the amino-terminal region of 4.1G. We propose that these dynamic associations provide the structural basis for a regulated molecular adhesive complex that serves to cluster and transport LFA-1 and associated molecules.

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Section: Methodsmentioning

confidence: 99%

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confidence: 99%

The LFA-1-associated Molecule PTA-1 (CD226) on T Cells Forms a Dynamic Molecular Complex with Protein 4.1G and Human Discs Large

Ralston

Hird

Zhang

et al. 2004

Journal of Biological Chemistry

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“…T he CD226, also named TliSA1, PTA1, or DNAM-1, is a member of the Ig superfamily containing two Ig V-like domains in its extracellular region and three tyrosine residues in its cytoplasmic portion (1,2). In humans, CD226 is constitutively expressed in hematopoietic cells such as T cells, NK cells, NKT cells, a subset of B cells, monocytes/macrophages, and dendritic cells and is involved in a variety of immunological functions, including T cell differentiation and cytotoxicity, NK cell cytotoxicity, NKT cell apoptosis, monocyte extravasation, and dendritic cell maturation (1)(2)(3)(4)(5)(6)(7)(8)(9)(10)(11)(12).…”

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confidence: 99%

Expression of CD226 Antagonizes Apoptotic Cell Death in Murine Thymocytes

Fang¹,

Zhang

Miao³

et al. 2009

The Journal of Immunology

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*CD226 is known to be expressed on many types of peripheral lymphoid cells and involved in T cell differentiation, activation, and cytotoxicity. In this study, we report that CD226 is also expressed on mouse thymocytes at varying developmental stages, and its expression is associated with resistance of thymocytes to apoptosis. The levels of CD226 expression appeared to be closely coupled with thymocyte development, in that it was preferentially expressed on CD4 ؉ CD8 ؊ and CD4 ؊ CD8 ؉ thymocytes at all stages during mouse development, and was markedly increased on the cells in neonatal mice. Of the CD4 ؉ CD8 ؉ population, CD226 was predominantly expressed by the cells also positive for CD69, suggesting that CD226 expression may be induced in thymocytepositive selection. Inhibition of CD226 by short hairpin RNA in a fetal thymus organ culture model led to reduced thymus cellularity, which was associated with enhanced apoptotic cell death. In contrast, CD226-transgenic mice displayed enlarged thymus lobes resulting from increased thymus cellularity. T he CD226, also named TliSA1, PTA1, or DNAM-1, is a member of the Ig superfamily containing two Ig V-like domains in its extracellular region and three tyrosine residues in its cytoplasmic portion (1, 2). In humans, CD226 is constitutively expressed in hematopoietic cells such as T cells, NK cells, NKT cells, a subset of B cells, monocytes/macrophages, and dendritic cells and is involved in a variety of immunological functions, including T cell differentiation and cytotoxicity, NK cell cytotoxicity, NKT cell apoptosis, monocyte extravasation, and dendritic cell maturation (1-12).In the murine system, engagement of CD226 with its ligands (mCD112 and Tage4) is believed to mediate a costimulatory signal in Ag-specific T cells (13). It has been reported that Th1 cells differentiation are involved in increased levels of CD226 expression, whereas the levels of CD226 were down-regulated upon Th2 cell polarization in BALB/c mice. In addition, treatment with a specific mAb against CD226(10E5) was shown to inhibit T cell proliferation in spleens and lymph nodes in SJL/J mice (14).Thymus is an organ for T lymphocyte development from early thymocyte progenitors to functional competent T cells ready for emigration to the periphery. To date, there has been no report on the expression status and the potential functional significance of CD226 in thymocytes. In view of this, we have examined the expression levels of CD226 on thymocytes during mouse development. We show in this report that CD226 is preferentially expressed on CD4 ϩ CD8 Ϫ and CD4 Ϫ CD8 ϩ thymocytes at all stages during mouse development and is markedly increased in the cells in neonatal mice. Of the CD4 ϩ CD8 ϩ population, CD226 is predominantly expressed by the cells also positive for CD69. Moreover, we demonstrate that CD226 is an antiapoptotic molecule that may play an important role in regulating thymus cellularity during murine development. Materials and Methods Cell culture and AbThe EL-4 thymoma cell line and the...

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“…Initiation of the cytotoxicity function by cross-linking of the CD226 receptor depends upon its Ser329 phosphorylation by protein kinase C (PKC) and physical and functional interactions with LFA-1 (Shibuya et al, 1999). CD226 is also known as platelet and T-cell antigen 1 and its cross-linking by a mAb stimulates platelet secretion and activation in a PKC-dependent manner (Sherrington et al, 1997). On the other hand, Necl-5 colocalizes with integrin a v b 3 at the leading edges of moving cells and enhances growth factor-induced cell movement and proliferation by facilitating growth factor-induced activation of Cdc42 and Rac small G proteins Kakunaga et al, 2004).…”

Section: Discussionmentioning

confidence: 99%

Interaction of cancer cells with platelets mediated by Necl-5/poliovirus receptor enhances cancer cell metastasis to the lungs

et al. 2007

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Necl-5 is an immunoglobulin (Ig)-like molecule that was originally identified as a poliovirus receptor and is often upregulated in cancer cells. We recently found that it colocalizes with integrin a v b 3 at the leading edges of moving cells and enhances growth factor-induced cell movement and proliferation. Upon cell-cell contact, Necl-5 is removed from the cell surface by its trans-interaction with the cell adhesion molecule nectin-3, resulting in reduced cell movement and proliferation. Here, we investigated the role of Necl-5 in the interaction of cancer cells with platelets. Necl-5 was upregulated in CT26 cells, a colon adenocarcinoma cell line. When CT26 cells were injected into the tail vein of mice, they were arrested in the pulmonary vessels by adhering to platelets and subsequently metastasized to the lungs. Overexpression of Necl-5 in CT26 cells enhanced this metastasis, while inhibition of the trans-interaction of Necl-5 with CD226 by an anti-Necl-5 monoclonal antibody reduced the metastasis. Depletion of platelets by treatment with a rabbit anti-mouse platelet serum reduced the Necl-5-enhanced metastasis in mice. Thus, the trans-interaction of upregulated Necl-5 in cancer cells with its counterreceptor in platelets, probably CD226, is critical for efficient metastasis of cancer cells to the lungs.

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TLiSA1 (PTA1) Activation Antigen Implicated in T Cell Differentiation and Platelet Activation Is a Member of the Immunoglobulin Superfamily Exhibiting Distinctive Regulation of Expression

Cited by 42 publications

References 36 publications

The LFA-1-associated Molecule PTA-1 (CD226) on T Cells Forms a Dynamic Molecular Complex with Protein 4.1G and Human Discs Large

The LFA-1-associated Molecule PTA-1 (CD226) on T Cells Forms a Dynamic Molecular Complex with Protein 4.1G and Human Discs Large

Expression of CD226 Antagonizes Apoptotic Cell Death in Murine Thymocytes

Interaction of cancer cells with platelets mediated by Necl-5/poliovirus receptor enhances cancer cell metastasis to the lungs

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