Signal-Transducing Adaptor Protein-2 Regulates Stromal Cell-Derived Factor-1α-Induced Chemotaxis in T Cells

Sekine, Yoshifumi; Ikeda, Osamu; Tsuji, Satoshi; Yamamoto, Chihiro; Muromoto, Ryuta; Nanbo, Asuka; Oritani, Kenji; Yoshimura, Akihiko; Matsuda, Tadashi

doi:10.4049/jimmunol.0902096

Cited by 36 publications

(62 citation statements)

References 42 publications

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“…Thus, our data suggest a strong involvement of STAP-2 in the linkage of BCR-ABL and CXCR4. Coupled with our previous results indicating that STAP-2 enhances SDF-1a signaling through interactions with Vav (Sekine et al, 2009a), STAP-2 is likely to regulate SDF-1a/CXCR4 at multiple levels in CML cells. Therefore, STAP-2 is likely to play a crucial role in the pathogenesis of CML.…”

Section: Discussionsupporting

confidence: 86%

“…In this study we demonstrated that STAP-2 interacts with and modifies the function of various signaling or transcription molecules Yamamoto et al, 2003;Sekine et al, 2005Sekine et al, , 2006Sekine et al, , 2007bSekine et al, , 2009a. We also demonstrated that BCR-ABL acts as a novel binding partner for STAP-2 in the presence of both the STAP-2 SH2-like domain and STAP-2 Tyr250 phosphorylation.…”

Section: Discussionmentioning

confidence: 60%

“…We previously showed that STAP-2 regulates SDF-1a-induced T-cell migration via activation of Vav1/Rac1 signaling, suggesting that STAP-2 may be involved in chemokine functions (Sekine et al, 2009a). To clarify the tumor progression between BCR-ABL/STAP-2 and BCR-ABL-expressing Ba/F3 cells, we examined the mRNA expression levels of a series of chemokine receptors in the Ba/F3 transfectants.…”

Section: Stap-2 Cooperates With Bcr-abl To Modify the Expression Of Cmentioning

confidence: 99%

“…Previous works in this laboratory found that STAP-2 have the ability to associate with and influence a variety of signaling or transcriptional molecules Yamamoto et al, 2003;Sekine et al, 2005Sekine et al, , 2006Sekine et al, , 2007bSekine et al, , 2009a, including the finding that STAP-2 can modulate the transcriptional activity of STAT3 and STAT5 Sekine et al, 2005), in addition to the FceRI and Toll-like receptor-mediated signals Sekine et al, 2006). Furthermore, thymocytes and peripheral T cells from STAP-2-deficient mice show enhanced interleukin-2 (IL-2)-or T cell receptor-dependent cell growth, integrin-mediated T-cell adhesion and impaired stromal cell-derived factor-1a (SDF-1a)-induced T-cell migration (Sekine et al, , 2007b(Sekine et al, , 2009a. Because STAP-2 is expressed in a variety of tissues and cells, such as lymphocytes, macrophages and hepatocytes, STAP-2 is also likely to function in a variety of different cells.…”

Section: Introductionmentioning

confidence: 98%

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STAP-2 interacts with and modulates BCR-ABL-mediated tumorigenesis

et al. 2012

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In chronic myeloid leukemia (CML), the BCR-ABL fusion oncoprotein activates multiple pathways involved in cell survival, growth promotion and disease progression. In this report, we show that the signal transducing adaptor protein-2 (STAP-2) is involved in BCR-ABL activity. We demonstrate that STAP-2 bound to BCR-ABL, and BCR and ABL proteins, depending on the STAP-2 Src homology 2-like domain. BCR-ABL phosphorylates STAP-2 Tyr250 and the phosphorylated STAP-2 in turn up-regulated BCR-ABL phosphorylation, leading to enhanced activation of downstream signaling molecules including ERK, STAT5, BCL-xL and BCL-2. In addition, STAP-2 interacts with BCR-ABL to alter chemokine receptor expression leading to downregulation of CXCR4 and upregulation of CCR7. The interaction between STAP-2 and BCR-ABL plays a crucial role in conferring a growth advantage and resistance to imatinib, a BCR-ABL inhibitor, as well as tumor progression. Notably, mice injected with BCR-ABL/STAP-2-expressing Ba/F3 cells developed lymph node enlargement and hepatosplenomegaly. Moreover, suppression of STAP-2 in K562 CML cells resulted in no tumor formation in mice. Our results demonstrate a critical contribution of STAP-2 in BCR-ABL activity, and suggest that STAP-2 might be an important candidate for drug development for patients with CML. Further, the expression of STAP-2 provides useful information for estimating the characteristics of individual CML clones

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Section: Discussionsupporting

confidence: 86%

Section: Discussionmentioning

confidence: 60%

Section: Stap-2 Cooperates With Bcr-abl To Modify the Expression Of Cmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 98%

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STAP-2 interacts with and modulates BCR-ABL-mediated tumorigenesis

et al. 2012

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“…STAP-2 is expressed in a variety of tissues and cells, such as lymphocytes, macrophages, and hepatocytes (9), and its abundant expression pattern suggests that STAP-2 influences a variety of signaling or transcriptional molecules. Indeed, we previously reported that STAP-2 can modulate the transcriptional activity of STAT3 and STAT5, as well as TLR-mediated signals in macrophages and integrin-or SDF1a-mediated signals in T cells (9,(11)(12)(13)(14). Through these interactions, STAP-2 plays physiological roles in immune responses.…”

mentioning

confidence: 99%

Signal-Transducing Adaptor Protein-2 Controls the IgE-Mediated, Mast Cell–Mediated Anaphylactic Responses

Sekine

Nishida

Yamasaki

et al. 2014

The Journal of Immunology

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Signal-transducing adaptor protein-2 (STAP-2) is a recently identified adaptor protein that regulates immune and inflammatory responses through interactions with a variety of signaling and transcriptional molecules. In the current study, we clarified the physiological role of STAP-2 in mast cell function, a key mediator of IgE-associated allergic responses. STAP-2 is constitutively expressed in mast cells. STAP-2 deficiency in mast cells greatly enhances FcεRI-mediated signals, resulting in the increased tyrosine phosphorylation of the phospholipase C-γ isoform, calcium mobilization, and degranulation. Of importance, STAP-2–deficient mice challenged with DNP-BSA after passive sensitization with anti-DNP IgE show more severe rectal temperature decrease than do wild-type mice. STAP-2–deficient mice also show increased vascular permeability and more severe cutaneous anaphylaxis after DNP-BSA injection. These regulatory functions performed by STAP-2 indicate that there is an interaction between STAP-2 and FcεRI. In addition, our previous data indicate that STAP-2 binds to the phospholipase C-γ isoform and IκB kinase-β. Therefore, our data described in this article strongly suggest that manipulation of STAP-2 expression in mast cells may control the pathogenesis of allergic diseases and have the potential for treating patients with allergy.

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STAP‐2 negatively regulates BCR‐mediated B cell activation by recruiting tyrosine‐protein kinase CSK to LYN

Kashiwakura,

Kawahara,

Inagaki

et al. 2023

FEBS Letters

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Although signal‐transducing adaptor protein‐2 (STAP‐2) acts in certain immune responses, its role in B cell receptor (BCR)‐mediated signals remains unknown. In this study, we have revealed that BCR‐mediated signals, cytokine production and antibody production were increased in STAP‐2 knockout (KO) mice compared with wild‐type (WT) mice. Phosphorylation of tyrosine‐protein kinase LYN Y508 was reduced in STAP‐2 KO B cells after BCR stimulation. Mechanistic analysis revealed that STAP‐2 directly binds to LYN, dependently of STAP‐2 Y250 phosphorylation by LYN. Furthermore, phosphorylation of STAP‐2 enhanced interactions between LYN and tyrosine‐protein kinase CSK, resulting in enhanced CSK‐mediated LYN Y508 phosphorylation. These results suggest that STAP‐2 is crucial for controlling BCR‐mediated signals and antibody production by enhanced CSK‐mediated feedback regulation of LYN.

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Signal-Transducing Adaptor Protein-2 Regulates Stromal Cell-Derived Factor-1α-Induced Chemotaxis in T Cells

Cited by 36 publications

References 42 publications

STAP-2 interacts with and modulates BCR-ABL-mediated tumorigenesis

STAP-2 interacts with and modulates BCR-ABL-mediated tumorigenesis

Signal-Transducing Adaptor Protein-2 Controls the IgE-Mediated, Mast Cell–Mediated Anaphylactic Responses

STAP‐2 negatively regulates BCR‐mediated B cell activation by recruiting tyrosine‐protein kinase CSK to LYN

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