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impact of renin–angiotensin–aldosterone system polymorphisms on myocardial perfusion: correlations with myocardial single photon emission computed tomography-derived parameters
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نویسنده
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angelidis george ,samara maria ,papathanassiou maria ,satra maria ,valotassiou varvara ,tsougos ioannis ,psimadas dimitrios ,tzavara chara ,alexiou sotiria ,koutsikos john ,demakopoulos nikolaos ,giamouzis gregory ,triposkiadis filippos ,skoularigis john ,kollia panagoula ,georgoulias panagiotis
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منبع
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journal of nuclear cardiology - 2019 - دوره : 26 - شماره : 4 - صفحه:1298 -1308
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چکیده
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Renin–angiotensin–aldosterone system (raas) has an important role in atherosclerosis. we investigated the effects of six raas gene polymorphisms on myocardial perfusion. we examined 810 patients with known or suspected coronary artery disease (cad) using stress–rest myocardial single-photon emission computed tomography. summed stress score (sss), summed rest score (srs), summed difference score (sds), transient ischemic dilation (tid), and lung/heart ratio (lhr) were recorded. the following gene polymorphisms were investigated: angiotensin-converting enzyme (ace) insertion/deletion (i/d), angiotensinogen (agt) m235t and t174m, angiotensin ii type 1 receptor (at1r) a1166c, renin (ren) c5312t, and angiotensin ii type 2 receptor (at2r) c3123a. the heterozygotes or homozygotes on ace d allele were 7.54 times more likely to have abnormal sss, while the agt (t174m) heterozygotes were 5.19 times more likely to have abnormal sss. the homozygotes of ace d had significantly higher values on tid and lhr, while the agt (t174m) heterozygotes had higher values on tid. the at1r heterozygotes had greater odds for having sss ≥ 3. the patients carried at1r homozygosity of c allele had significantly higher values on tid, while heterozygotes of at1r had significantly higher values on lhr. among the polymorphisms investigated, ace d allele had the strongest association with abnormal myocardial perfusion.
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کلیدواژه
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ace ,angiotensinogen ,angiotensin ιι receptors ,cad ,renin
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آدرس
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university hospital of larissa, department of nuclear medicine, greece. army share fund hospital (417 nimts), department of nuclear medicine, greece, university of thessaly, department of pathology, greece, university of thessaly, department of pathology, greece, university of thessaly, department of biology & genetics, greece, university hospital of larissa, department of nuclear medicine, greece, university hospital of larissa, department of nuclear medicine, greece, university hospital of larissa, department of nuclear medicine, greece, university hospital of larissa, department of nuclear medicine, greece, university hospital of larissa, department of nuclear medicine, greece, army share fund hospital (417 nimts), department of nuclear medicine, greece, army share fund hospital (417 nimts), department of nuclear medicine, greece, university hospital of larissa, department of cardiology, greece, university hospital of larissa, department of cardiology, greece, university hospital of larissa, department of cardiology, greece, national & kapodistrian university of athens, faculty of biology, department of genetics & biotechnology, greece, university hospital of larissa, department of nuclear medicine, greece
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Authors
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