Mitochondrial proteases act on STARD3 to activate progesterone synthesis in human syncytiotrophoblast |
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| Authors: | Mercedes Esparza-Perusquí a,Sofí a Olvera-Sá nchez,Oscar Flores-Herrera,Hé ctor Flores-Herrera,Alberto Guevara-Flores,Juan Pablo Pardo,Marí a Teresa Espinosa-Garcí a,Federico Martí nez |
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| Affiliation: | 1. Departamento de Bioquímica, Facultad de Medicina, Universidad Nacional Autónoma de México, Mexico;2. Departamento de Bioquímica y Biología Molecular, Instituto Nacional de Perinatología “Isidro Espinosa de los Reyes”, Mexico |
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| Abstract: | BackgroundSTARD1 transports cholesterol into mitochondria of acutely regulated steroidogenic tissue. It has been suggested that STARD3 transports cholesterol in the human placenta, which does not express STARD1. STARD1 is proteolytically activated into a 30-kDa protein. However, the role of proteases in STARD3 modification in the human placenta has not been studied.MethodsProgesterone determination and Western blot using anti-STARD3 antibodies showed that mitochondrial proteases cleave STARD3 into a 28-kDa fragment that stimulates progesterone synthesis in isolated syncytiotrophoblast mitochondria. Protease inhibitors decrease STARD3 transformation and steroidogenesis.ResultsSTARD3 remained tightly bound to isolated syncytiotrophoblast mitochondria. Simultaneous to the increase in progesterone synthesis, STARD3 was proteolytically processed into four proteins, of which a 28-kDa protein was the most abundant. This protein stimulated mitochondrial progesterone production similarly to truncated-STARD3. Maximum levels of protease activity were observed at pH 7.5 and were sensitive to 1,10-phenanthroline, which inhibited steroidogenesis and STARD3 proteolytic cleavage. Addition of 22(R)-hydroxycholesterol increased progesterone synthesis, even in the presence of 1,10-phenanthroline, suggesting that proteolytic products might be involved in mitochondrial cholesterol transport.ConclusionMetalloproteases from human placental mitochondria are involved in steroidogenesis through the proteolytic activation of STARD3. 1,10-Phenanthroline inhibits STARD3 proteolytic cleavage. The 28-kDa protein and the amino terminal truncated-STARD3 stimulate steroidogenesis in a comparable rate, suggesting that both proteins share similar properties, probably the START domain that is involved in cholesterol binding.General significanceMitochondrial proteases are involved in syncytiotrophoblast-cell steroidogenesis regulation. Understanding STARD3 activation and its role in progesterone synthesis is crucial to getting insight into its action mechanism in healthy and diseased syncytiotrophoblast cells. |
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| Keywords: | Human syncytiotrophoblast mitochondria Progesterone synthesis STARD3 protein Mitochondrial metalloprotease |
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