Adhesion of immature thymocytes to thymic stromal cells through fibronectin molecules and its significance for the induction of thymocyte differentiation.

Utsumi, K; Sawada, Masumi; Narumiya, Seiji; Nagamine, Jun; Sakata, T; Iwagami, Shoji; Kita, Yasuyuki; Teraoka, Hitoshi; Hirano, Hiroyuki; Ogata, Masato

doi:10.1073/pnas.88.13.5685

Cited by 92 publications

(55 citation statements)

References 40 publications

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“…Several laboratories including ours have shown that [31 integrins synergize with the TCR-CD3 pathway to promote T cell proliferation (4-6). [31 integrins are also reported to be involved in T or B cell differentiation through interaction with fibronectin expressed by stromal cells in thymus or bone marrow, respectively (7,8). Furthermore, it was also reported that integrin-ECM binding induced increases of cytoplasmic Ca 2+ and cytoplasmic pH (9, 10).…”

Section: Discussionmentioning

confidence: 99%

Direct association of pp125FAK with paxillin, the focal adhesion-targeting mechanism of pp125FAK.

Tachibana

Sato

D'Avirro

et al. 1995

The Journal of Experimental Medicine

244

230

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SummaryFocal adhesion kinase (pp125 FAK) is localized to focal adhesions and tyrosine phosphorylated by the engagement of 61 integrins. However, it is unclear how pp125 rAK is linked to integrin molecules. We demonstrate that pp125 FAK is directly associated with paxillin, a 68-kD cytoskeleton protein. The COOH-terminal domain ofppl25 FAK spanning FAK residues 919-1042 is sufficient for paxillin binding and has vinculin-homologous amino acids, which are essential for paxillin binding. Microinjection and subsequent imrnunohistochemical analysis reveal that glutathione S-transferase-FAK fusion proteins, which bind to paxillin, localize to focal adhesions, whereas fusion proteins with no paxillin-binding activity do not localize to focal adhesions. These findings strongly suggest that pp125 FAK is localized to focal adhesions by the direct association with paxillin.t h•at 1 integrins, also known as very late activation antigens, constitute a subfamily of integrin adhesion receptors is comprised by at least nine o~ subunits sharing a common [31 subunit (1,2). [31 integrins function as cell-surface receptors for extracellular matrix protein (ECM) 1 and also mediate cell-to-cell interaction (1, 2). The marked changes in morphology and behavior that occur when cells interact with ECM through their integrins suggest that these receptors can function as transducers of extracellular signals into cells (2, 3). Several laboratories including ours have shown that [31 integrins synergize with the TCR-CD3 pathway to promote T cell proliferation (4-6). [31 integrins are also reported to be involved in T or B cell differentiation through interaction with fibronectin expressed by stromal cells in thymus or bone marrow, respectively (7,8). Furthermore, it was also reported that integrin-ECM binding induced increases of cytoplasmic Ca 2+ and cytoplasmic pH (9, 10). These facts strongly support the notion that the interaction between [31 integrins and ECM transmits signals into the interior of cells.In an effort to clarify mechanisms ofT cell costinmlatory signals mediated by [31 integrins, we found that tyrosine kinase activation might be a key event in this process. We showed that tyrosine phosphorylation of 105-130-kD proIAbbreviations used in this paper: ECL, enhanced chemiluminescence; ECM, extracellular matrix protein; FAT, focal adhesion targeting; FN, fibronectin; FRNK, FAK-related nonkinase; GST, glutathione S-transferase; PBS-T, PBS containing 0.1% Tween 20; PBS1, paxillin-binding subdomain 1; PBS2, paxillin-binding subdomain 2; pp 125 yAK, focal adhesion kinase; PTK, protein tyrosine kinase.teins was induced by the ligation of [31 or ci4 integrin subunits using either fibronectin (FN) or mAbs in human peripheral T cells and H9, a T lymphoblastoid cell line (11,12). Several independent studies also showed that tyrosine phosphorylation of proteins in the range of 120-130 kD is induced by the engagement of [31 integrins in different types of cells including mouse fibroblasts and human epidermal cancer cell line (13,14). One ...

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Section: Discussionmentioning

confidence: 99%

Direct association of pp125FAK with paxillin, the focal adhesion-targeting mechanism of pp125FAK.

Tachibana

Sato

D'Avirro

et al. 1995

The Journal of Experimental Medicine

244

230

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“…The influence of fibronectin on proliferation and differentiation of erythroid cells has been documented (75,76). Adhesion of CD4-CD8 -thymocytes to thymic stromal cells through FN-FN receptor interaction is known to be critical for their differentiation (77 Disruption ofnormal adhesion pathways between stem and stromal cells has been implicated as a critical factor in pathogenesis of chronic myeloid leukemia (81,82). Furthermore, after chemotherapy and/or total body irradiation, the observed extravascation of stem cells into peripheral blood (83) …”

Section: Resultsmentioning

confidence: 99%

Role of beta 1 and beta 2 integrins in the adhesion of human CD34hi stem cells to bone marrow stroma.

Teixidó¹,

Hemler²,

Greenberger³

et al. 1992

J. Clin. Invest.

356

203

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“…Previously, in vitro systems have shown a requirement for integrins and integrin-related proteins for the maturation of CD4 Ϫ CD8 Ϫ to CD4 ϩ CD8 ϩ cells (12)(13)(14). Most of the in vitro data in mice point to the CD4 Ϫ CD8 Ϫ cells as being adhesive cells with activated integrins.…”

Section: Discussionmentioning

confidence: 99%

“…A number of in vitro studies have demonstrated that the engagement of integrins is required for the differentiation of CD4 Ϫ CD8 Ϫ cells to become CD4 ϩ CD8 ϩ cells (12)(13)(14). Furthermore, the Abmediated engagement of integrin receptors in addition to the engagement of the CD3 complex on CD4 ϩ CD8 ϩ thymocytes is required for cell proliferation in vitro (15,16).…”

Section: Integrin Functions Play a Key Role In The Differentiationmentioning

confidence: 99%

Integrin Functions Play a Key Role in the Differentiation of Thymocytes In Vivo

Schmeissner

Xie

Smilenov

et al. 2001

The Journal of Immunology

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T cells express a variety of surface proteins as they develop to maturity in the thymus. In addition to the TCR-CD3 complex and the two major coreceptors, CD4 and CD8, other surface proteins expressed include receptors for cytokines, growth factors, counterreceptors, and extracellular matrix molecules. To determine the role of integrin adhesion receptors in T cell development, we have expressed a trans-dominant inhibitor of integrin function in the thymus. This inhibitor leads to a block of adhesion to fibronectin due to reduced activation of integrin receptors. This reduced adhesion leads to a partial block in differentiation from CD4−CD8− cells to CD4+CD8+ cells, after the CD25+ stage, suggesting that integrins are important during Lck-mediated differentiation. Furthermore, the overall production of CD4+ cells is reduced compared with that of CD8+ cells without changes in negative selection, suggesting that integrins may be involved in the determination of the fate of the cell as well. These results demonstrate that integrin receptor function is required for proper thymocyte development in vivo.

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Adhesion of immature thymocytes to thymic stromal cells through fibronectin molecules and its significance for the induction of thymocyte differentiation.

Cited by 92 publications

References 40 publications

Direct association of pp125FAK with paxillin, the focal adhesion-targeting mechanism of pp125FAK.

Direct association of pp125FAK with paxillin, the focal adhesion-targeting mechanism of pp125FAK.

Role of beta 1 and beta 2 integrins in the adhesion of human CD34hi stem cells to bone marrow stroma.

Integrin Functions Play a Key Role in the Differentiation of Thymocytes In Vivo

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