FYB

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FYN binding protein (FYB-120/130), also known as FYB, ADAP (Adhesion and degranulation-promoting adapter protein), and SLAP-130 (SLP-76-associated phosphoprotein) is a protein that is encoded by the FYB gene in humans.[1] The protein is expressed in T cells, monocytes, mast cells, macrophages, NK cells, but not B cells.[2][3][4][5] FYB is a multifunctional protein involved in post-activation T cell signaling, lymphocyte cytokine production, cell adhesion, and actin remodeling.[3][4][5][6][7]

Structure

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Two isoforms of FYB with different lengths of 120 and 130 kDa (FYB-120 and FYB-130) exist.[4] The 130kDa version has an extra insertion of 46 amino acids and is preferentially expressed in peripheral T cells.[4] The FYB protein has a variety of binding domains: a non-structured N-terminal region, a proline-rich region, two SH3 domains, a FPPP-motif which binds the ENA/VASP protein family, and other tyrosine-based signaling motifs.[7]

Function

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FYB is critical for activation and proliferation of T-helper cells (CD4+) and required for chemokine signal transduction in T-helper cells and cytotoxic T cells (CD8+).[7]

FYB regulates cytokine production in T cells as well as in activated NK cells through the FYN-ADAP axis.[5] In T cells, after TCR stimulation, a unique region of FYB, pYDGI, allows phosphorylation of the protein by FYN.[5] After being phosphorylated, ADAP can bind to Carma1, causing NF-κB translocation into the nucleus and cytokine production.[5]

In mast cells, FYB regulates cell adhesion as well as degranulation.[3] In T cells, FYB allows for cell adhesion and migration through blood vessels through the SLP-76-FYB-SKAP1 complex.[6] After being phosphorylated by FYN, FYB can bind to SLP-76.[3] This binding of FYB and SLP-76 regulates "outside-in signaling" or the transfer of signals from outside the cell to inside the cell by integrin.[6] FYB can also bind to SKAP1, which allows SKAP1 to upregulate integrin activity through interactions with Rap1.[4][6] The bacteria Yersinia can interfere with this pathway in macrophages through the secretion of YopH (Yersinia protein tyrosine phosphatase) into the macrophage, which de-phosphorylates FYB and SKAP1, leading to a decrease in integrin activity that results in an inhibition of adhesion, phagocytosis, and cytotoxicity.[4]

FYB is also an important protein for actin remodeling of immune cells.[7] This is thought to occur through the binding of proteins of the ENA/VASP protein family to the FPPPP-motif of the FYB protein.[7]

References

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Further reading

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