[HTML][HTML] Calpain 8/nCL-2 and calpain 9/nCL-4 constitute an active protease complex, G-calpain, involved in gastric mucosal defense
S Hata, M Abe, H Suzuki, F Kitamura… - PLoS …, 2010 - journals.plos.org
S Hata, M Abe, H Suzuki, F Kitamura, N Toyama-Sorimachi, K Abe, K Sakimura, H Sorimachi
PLoS genetics, 2010•journals.plos.orgCalpains constitute a superfamily of Ca2+-dependent cysteine proteases, indispensable for
various cellular processes. Among the 15 mammalian calpains, calpain 8/nCL-2 and calpain
9/nCL-4 are predominantly expressed in the gastrointestinal tract and are restricted to the
gastric surface mucus (pit) cells in the stomach. Possible functions reported for calpain 8 are
in vesicle trafficking between ER and Golgi, and calpain 9 are implicated in suppressing
tumorigenesis. These highlight that calpains 8 and 9 are regulated differently from each …
various cellular processes. Among the 15 mammalian calpains, calpain 8/nCL-2 and calpain
9/nCL-4 are predominantly expressed in the gastrointestinal tract and are restricted to the
gastric surface mucus (pit) cells in the stomach. Possible functions reported for calpain 8 are
in vesicle trafficking between ER and Golgi, and calpain 9 are implicated in suppressing
tumorigenesis. These highlight that calpains 8 and 9 are regulated differently from each …
Calpains constitute a superfamily of Ca2+-dependent cysteine proteases, indispensable for various cellular processes. Among the 15 mammalian calpains, calpain 8/nCL-2 and calpain 9/nCL-4 are predominantly expressed in the gastrointestinal tract and are restricted to the gastric surface mucus (pit) cells in the stomach. Possible functions reported for calpain 8 are in vesicle trafficking between ER and Golgi, and calpain 9 are implicated in suppressing tumorigenesis. These highlight that calpains 8 and 9 are regulated differently from each other and from conventional calpains and, thus, have potentially important, specific functions in the gastrointestinal tract. However, there is no direct evidence implicating calpain 8 or 9 in human disease, and their properties and physiological functions are currently unknown. To address their physiological roles, we analyzed mice with mutations in the genes for these calpains, Capn8 and Capn9. Capn8−/− and Capn9−/− mice were fertile, and their gastric mucosae appeared normal. However, both mice were susceptible to gastric mucosal injury induced by ethanol administration. Moreover, the Capn8−/− stomach showed significant decreases in both calpains 9 and 8, and the same was true for Capn9−/−. Consistent with this finding, in the wild-type stomach, calpains 8 and 9 formed a complex we termed “G-calpain,” in which both were essential for activity. This is the first example of a “hybrid” calpain complex. To address the physiological relevance of the calpain 8 proteolytic activity, we generated calpain 8:C105S “knock-in” (Capn8CS/CS) mice, which expressed a proteolytically inactive, but structurally intact, calpain 8. Although, unlike the Capn8−/− stomach, that of the Capn8CS/CS mice expressed a stable and active calpain 9, the mice were susceptible to ethanol-induced gastric injury. These results provide the first evidence that both of the gastrointestinal-tract-specific calpains are essential for gastric mucosal defense, and they point to G-calpain as a potential target for gastropathies caused by external stresses.
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