Rapamycin induces binding activity to the terminal oligopyrimidine tract of ribosomal protein mRNA in rats |
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Authors: | Kakegawa Tomohito Ito Makoto Hayakawa Akiko Matsuda Megumi Tamura Sayoko Saito Hiromi Kaspar Roger L Kobayashi Hiroshi |
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Institution: | Department of Oral Medicine and Diagnostic Sciences and Center for Molecular Biology of Oral Diseases, University of Illinois at Chicago, Chicago, Illinois 60612, USA. |
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Abstract: | Cathepsin G, elastase, and proteinase 3 are serine proteinases released by activated neutrophils. Cathepsin G can cleave angiotensinogen to release angiotensin II, but this activity has not been previously reported for elastase or proteinase 3. In this study we show that elastase and proteinase 3 can release angiotensin I from angiotensinogen and release angiotensin II from angiotensin I and angiotensinogen. The relative order of potency in releasing angiotensin II by the three proteinases at equivalent concentrations is cathepsin G > elastase > proteinase 3. When all three proteinases are used together, the release of angiotensin II is greater than the sum of the release when each proteinase is used individually. Cathepsin G and elastase can also degrade angiotensin II, reactions which might be important in regulating the activity of angiotensin II. The release and degradation of angiotensin II by the neutrophil proteinases are reactions which could play a role in the local inflammatory response and wound healing. |
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Keywords: | angiotensinogen angiotensin cathepsin G elastase proteinase 3 serpin proteolysis inflammation neutrophil |
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