Noncanonical Mechanisms for Direct Bone Marrow Generating Ang II (Angiotensin II) Predominate in CD68 Positive Myeloid Lineage Cells.

Q1 Earth and Planetary Sciences
Journal of Geophysical Research Pub Date : 2020-02-01 Epub Date: 2019-12-09 DOI:10.1161/HYPERTENSIONAHA.119.13754
Tomohisa Yamashita, Sarfaraz Ahmad, Kendra N Wright, Drew J Roberts, Jessica L VonCannon, Hao Wang, Leanne Groban, Louis J Dell'Italia, Carlos M Ferrario
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引用次数: 0

Abstract

Bone marrow (BM) Ang II (angiotensin II) is a major participant in the regulation of hematopoiesis and immunity. The novel tissue substrate Ang-(1-12) [angiotensin-(1-12)] and its cleaving enzyme chymase are an essential source of Ang II production in cardiac tissue. We hypothesized this noncanonical chymase-mediated Ang II-producing mechanism exists in the BM tissue. Immunohistostaining and flow cytometry confirmed the presence of Ang-(1-12) immunoreaction in the BM of SD (Sprague Dawley) rats. Chymase-mediated Ang II-producing activity in BM was ≈1000-fold higher than ACE (angiotensin-converting enzyme)-mediated Ang II-producing activity (4531±137 and 4.2±0.3 fmol/min per mg, respectively; n=6; P<0.001) and 280-fold higher than chymase activity in the left ventricle of 16.3±1.7 fmol/min per mg (P<0.001). Adding a selective chymase inhibitor, TEI-F00806, eliminated almost all 125I-Ang II production. Flow cytometry demonstrated that delta median fluorescence intensity of chymase in cluster of differentiation 68 positive cells was significantly higher than that in cluster of differentiation 68 negative cells (1546±157 and 222±48 arbitrary units, respectively; P=0.0021). Cluster of differentiation 68 positive and side scatter low subsets, considered to be myeloid progenitors, express the highest chymase fluorescence intensity in rat BM. Chymase activity and cellular expression was similar in both male and female rats. In conclusion, myeloid lineage cells, especially myeloid progenitors, have an extraordinary Ang II-producing activity by chymase in the BM.

骨髓直接生成血管紧张素 II(Angiotensin II)的非规范机制主要存在于 CD68 阳性的髓系细胞中。
骨髓(BM)Ang II(血管紧张素 II)是造血和免疫调节的主要参与者。新型组织底物 Ang-(1-12) [血管紧张素-(1-12)] 及其裂解酶糜蛋白酶是心脏组织产生 Ang II 的重要来源。我们假设这种由糜蛋白酶介导的非经典 Ang II 生成机制存在于 BM 组织中。免疫组化染色和流式细胞术证实,SD(Sprague Dawley)大鼠的BM中存在Ang-(1-12)免疫反应。乳腺组织中消融酶介导的 Ang II 生成活性比 ACE(血管紧张素转换酶)介导的 Ang II 生成活性高出≈1000 倍(分别为 4531±137 和 4.2±0.3 fmol/min/mg;n=6;PP125I-Ang II 生成)。流式细胞术显示,分化 68 群阳性细胞中糜蛋白酶的δ中值荧光强度明显高于分化 68 群阴性细胞(分别为 1546±157 和 222±48 任意单位;P=0.0021)。分化簇 68 阳性和侧散射低亚群被认为是骨髓祖细胞,在大鼠 BM 中表达最高的糜蛋白酶荧光强度。雌雄大鼠的糜蛋白酶活性和细胞表达相似。总之,髓系细胞,尤其是髓系祖细胞,在生化组织中具有通过糜蛋白酶产生 Ang II 的非凡活性。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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来源期刊
Journal of Geophysical Research
Journal of Geophysical Research 地学-地球科学综合
CiteScore
5.80
自引率
0.00%
发文量
0
审稿时长
1 months
期刊介绍: Journal of Geophysical Research (JGR) publishes original scientific research on the physical, chemical, and biological processes that contribute to the understanding of the Earth, Sun, and solar system and all of their environments and components. JGR is currently organized into seven disciplinary sections (Atmospheres, Biogeosciences, Earth Surface, Oceans, Planets, Solid Earth, Space Physics). Sections may be added or combined in response to changes in the science.
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