SH2 domain

1lkkA SH2 domain

SH2 domain is a protein domain that plays a critical role in the signal transduction pathways within cells. The SH2 (Src Homology 2) domain was first identified in the Src oncogene of the Rous sarcoma virus, and it is approximately 100 amino acids in length. This domain allows proteins containing it to bind to specific phosphotyrosine-containing sequences in other proteins, which is a key mechanism in the transmission of cellular signals and the regulation of cellular activities such as growth, differentiation, and metabolic control.

Function[edit | edit source]

The primary function of the SH2 domain is to recognize and bind to parts of other proteins that are phosphorylated on tyrosine residues, a process that is often a result of signal transduction cascades. This binding can change the activity of the protein containing the SH2 domain, or it can bring two proteins into close proximity, facilitating their interaction with each other. This mechanism is vital for the activation and regulation of many signaling pathways, including those involved in cell growth, survival, and proliferation.

Structure[edit | edit source]

The SH2 domain has a conserved structure that includes a central beta-sheet flanked by two alpha-helices. The phosphotyrosine binding site is located in a deep pocket on the domain's surface, which allows for the specific interaction with phosphotyrosine residues. The specificity of the SH2 domain for different phosphotyrosine-containing sequences is determined by the amino acids that surround the phosphotyrosine on the target protein, allowing for a high degree of specificity in signal transduction pathways.

Role in Disease[edit | edit source]

Alterations in the function of SH2 domains can lead to aberrant signaling pathways, which are often associated with the development of various diseases, including cancer, autoimmune diseases, and cardiovascular diseases. For example, mutations in the SH2 domain that increase its affinity for phosphotyrosine can lead to enhanced signaling activity and potentially to oncogenesis. Conversely, mutations that decrease the SH2 domain's ability to bind phosphotyrosine can impair immune cell function and lead to immunodeficiency disorders.

Examples[edit | edit source]

Several proteins contain SH2 domains, including the Src family kinases, phospholipase C-gamma, SHP-2 phosphatase, and the signal transducer and activator of transcription (STAT) proteins. Each of these proteins plays a crucial role in specific signaling pathways, and their activity is tightly regulated by the interaction of their SH2 domains with phosphotyrosine-containing proteins.

Research and Therapeutic Implications[edit | edit source]

Understanding the specific interactions between SH2 domains and their binding partners has significant implications for the development of targeted therapies for diseases caused by aberrant signal transduction. Inhibitors that can specifically block the interaction of SH2 domains with their phosphotyrosine-containing targets are being explored as potential therapeutic agents, particularly in the treatment of cancer.