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Titlebook: Aspartic Proteinases; Structure, Function, Kenji Takahashi Book 1995 The Editor(s) (if applicable) and The Author(s), under exclusive licen

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Advances in Experimental Medicine and Biologyhttp://image.papertrans.cn/b/image/163035.jpg
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Aspartic Proteinases978-1-4615-1871-6Series ISSN 0065-2598 Series E-ISSN 2214-8019
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https://doi.org/10.1007/978-3-642-70036-1on to pH 2. As the enzyme was purified, it became evident that it was in fact equivalent to the minor gastric enzyme originally named as progastricsin (EC 3.4.23.3) [2–6].This report provides a short review on the similarities and differences between human gastric and seminal progastricsin, and the possible function of the seminal progastricsin.
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Wirtschaftswissenschaftliche Beiträgenogenesis in higher vertebrates [1, 2]. The morphological and the functional differentiation of an organ necessarily involves the local expression or suppression of sets of genes in the cells constituting the organ.
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Local Visions for a Global Future,me, an increasingly rapid stream of structural information has issued from the crystallography groups [2]. At this point it is clear that members of this family are closely related structurally, with a central core composed of two domains, each of which has a two-layered β-sheet arrangement (see Fig
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https://doi.org/10.1007/978-3-319-78837-1ocatalytically at pH < 5.0 (1). The human gastric juice has two major groups of aspartic proteinases, the pepsins (EC3.4.23.1) and the gastricsins (EC3.4.23.3). Progastricsin or pepsinogen C (PGC) is converted to gastricsin by removal of the 43 amino-terminal residues of the prosegment. The resultin
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