Chymase-dependent Angiotensin II Formation in Human Vascular Tissue
Overview
Authors
Affiliations
Background: Some reports have suggested that, in vitro, human heart chymase in homogenates contributes little to angiotensin (Ang) II formation in the presence of natural protease inhibitors such as alpha-antitrypsin. We studied whether chymase bound to heparin, resembling an in vivo form, could contribute to Ang II formation in the presence of natural protease inhibitors.
Methods And Results: The Ang II formation was increased time-dependently after incubation in an extract (1 mg of protein/mL) of human vascular tissues containing Ang I. The concentration of Ang II in the extract after incubation for 30 minutes was 1.67+/-0.06 nmol/mL, and we regarded this quantity of Ang II as 100%. The Ang II formation was inhibited 10%, 95%, and 96% by 1 micromol/L lisinopril, 100 micromol/L chymostatin, and 0.1 g/L alpha-antitrypsin, respectively. The extract was applied to a heparin affinity column. After the column was washed with PBS, the eluted PBS contained a weak Ang II-forming activity, which was completely inhibited by lisinopril. The eluted PBS, to which >0.8 mol/L NaCl had been added, showed a strong Ang II-forming activity which was inhibited by chymostatin and alpha-antitrypsin. After the application of the extract, the column was washed with PBS and then an Ang I solution in PBS was applied to the column. The Ang II formation in the PBS eluted from the incubated column was increased time-dependently. The concentration of Ang II in the PBS (1 mL) eluted from the column after incubation for 30 minutes was 2.56+/-0.28 nmol/mL, and we regarded this quantity of Ang II as 100%. To study the effects of inhibitors, the extract (1 mg of protein/mL) was applied to a heparin affinity column (1 mL) which was preequilibrated with PBS (3 mL); 100 micromol/L chymostatin or 0.1 g/L alpha-antitrypsin in PBS (1 mL) was then applied to the column. After the column was washed with PBS (3 mL), Ang I solution (1 mg/mL) in PBS was applied to the column, and the column was incubated for 30 minutes. The Ang II formation in the PBS eluted from the column was suppressed up to 5% by application of chymostatin, although this was not affected by application of alpha-antitrypsin.
Conclusions: These findings suggest that human chymase bound to heparin plays a functional role in Ang II formation in the presence of natural protease inhibitors such as alpha-antitrypsin.
Mechanism of Albuminuria Reduction by Chymase Inhibition in Diabetic Mice.
Terai K, Jin D, Watase K, Imagawa A, Takai S Int J Mol Sci. 2020; 21(20).
PMID: 33050674 PMC: 7589797. DOI: 10.3390/ijms21207495.
Chymase inhibition retards albuminuria in type 2 diabetes.
Bivona B, Takai S, Seth D, Satou R, Harrison-Bernard L Physiol Rep. 2019; 7(24):e14302.
PMID: 31872559 PMC: 6928241. DOI: 10.14814/phy2.14302.
Okamura K, Okuda T, Takamiya Y, Shirai K, Urata H Heart Vessels. 2019; 34(9):1559-1569.
PMID: 30919112 DOI: 10.1007/s00380-019-01391-4.
Involvement of premacular mast cells in the pathogenesis of macular diseases.
Sato T, Morishita S, Horie T, Fukumoto M, Kida T, Oku H PLoS One. 2019; 14(2):e0211438.
PMID: 30794552 PMC: 6386310. DOI: 10.1371/journal.pone.0211438.
Okamura K, Okuda T, Shirai K, Urata H Heart Vessels. 2019; 34(7):1148-1157.
PMID: 30680494 DOI: 10.1007/s00380-019-01352-x.