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HGF, also known as scatter factor and hepatopoietin A, is a multifunctional protein involved in organoid culture. It belongs to the plasminogen subfamily of S1 peptidases and consists of several domains, including an N-terminal PAN/APPLE-like domain, four Kringle domains, and a serine proteinase-like domain without protease activity. HGF is initially secreted as an inactive propeptide containing 728 amino acids. It undergoes cleavage after the fourth Kringle domain by a serine protease to generate bioactive disulfide-linked HGF, consisting of a 60 kDa alpha chain and a 30 kDa beta chain. Alternative splicing of the HGF gene leads to the production of isoforms lacking the proteinase-like domain and varying numbers of Kringle domains. Human HGF shares significant sequence identity (91%-94%) with HGF from other species, including bovine, canine, feline, mouse, and rat.

HGF exerts its effects by binding to heparan-sulfate proteoglycans and the widely expressed receptor tyrosine kinase, HGF R/c-MET. The activation of c-MET by HGF is implicated in the development of various human cancers. In the context of organoid culture, HGF plays a crucial role in regulating epithelial morphogenesis by inducing cell scattering and branching tubulogenesis. It promotes the up-regulation of integrin alpha 2 beta 1, a collagen I receptor, and its blockade disrupts epithelial cell branching tubulogenesis. HGF also influences epithelium morphology by inducing the shedding of the nectin-1 alpha ectodomain, an adhesion protein component of adherens junctions .

Furthermore, HGF affects the thyroid by inducing the proliferation, motility, and loss of differentiation markers in thyrocytes, as well as inhibiting TSH-stimulated iodine uptake. In damaged myocardium, HGF promotes the motility of cardiac stem cells. These diverse functions of HGF make it an essential factor in organoid culture.