Vasomotion in human arteries and their regulations based on ion channel regulations: 10 years study

Author:

Kim Dae Hoon1,Choi Jin Young2,Kim Su Mi2,Son Seung‐Myoung3,Choi Song‐Yi4,Koo Beommo5,Rah Cheong‐Sil6,Nam Ji Hyun5,Ju Moon Jin5,Lee Jong Sung7,You Ra Young8,Hong Seung Hwa2,Lee Junyoung9,Bae Jang‐Whan9,Kim Chan Hyung10,Choi Woong10,Kim Hun Sik10,Xu Wen‐Xie11,Lee Sang Jin8,Kim Young Chul8,Yun Hyo‐Yung1

Affiliation:

1. Department of Surgery, College of Medicine, Chungbuk National University Hospital (CBNUH) Chungbuk National University (CBNU) Cheongju Chungbuk Korea

2. Department of OBGY, College of Medicine, CBNU College of Medicine, CBNU, (CBNUH) Cheongju Korea

3. Department of Pathology College of Medicine, CBNU Cheongju Korea

4. Department of Pathology, College of Medicine Chungnam National University Daejeon Korea

5. College of Medicine, CBNU Cheongju Korea

6. Department of Surgery, Uijeongbu Eulji Medical Center Eulji University Uijeongbu‐si Gyeonggi‐do Korea

7. Department of Family Medicine Korea University College of Medicine Seoul Korea

8. Department of Physiology College of Medicine, CBNU Cheongju Korea

9. Department of Internal Medicine College of Medicine, CBNU & CBNUH Cheongju Korea

10. Department of Pharmacology College of Medicine, CBNU Cheongju Korea

11. Department of Physiology, College of Medcine Shanghai Jiaotong University Shanghai People's Republic of China

Abstract

AbstractVasomotion is the oscillation of vascular tone which gives rise to flow motion of blood into an organ. As is well known, spontaneous contractile organs such as heart, GI, and genitourinary tract produce rhythmic contraction. It imposes or removes pressure on their vessels alternatively for exchange of many substances. It was first described over 150 years ago, however the physiological mechanism and pathophysiological implications are not well understood. This study aimed to elucidate underlying mechanisms and physiological function of vasomotion in human arteries. Conventional contractile force measurement, immunohistochemistry, and Western blot analysis were employed to study human left gastric artery (HLGA) and uterine arteries (HUA). RESULTS: Circular muscle of HLGA and/or HUA produced sustained tonic contraction by high K+ (50 mM) which was blocked by 2 µM nifedipine. Stepwise stretch and high K+ produced nerve‐independent spontaneous contraction (vasomotion) (around 45% of tested tissues). Vasomotion was also produced by application of BayK 8644, 5‐HT, prostagrandins, oxytocin. It was blocked by nifedipine (2 µM) and blockers of intracellular Ca2+ stores. Inhibitors of Ca2+‐activated Cl channels (DIDS and/or niflumic acid) and ATP‐sensitive K+ (KATP) channels inhibited vasomotion reversibly. Metabolic inhibition by sodium cyanide (NaCN) and several neuropeptides also regulated vasomotion in KATP channel‐sensitive and ‐insensitive manner. Finally, we identified TMEM16A Ca2+‐activated Cl channels and subunits of KATP channels (Kir 6.1/6.2 and sulfonylurea receptor 2B [SUR2B]), and c‐Kit positivity by Western blot analysis. We conclude that vasomotion is sensitive to TMEM16A Ca2+‐activated Cl channels and metabolic changes in human gastric and uterine arteries. Vasomotion might play an important role in the regulation of microcirculation dynamics even in pacemaker‐related autonomic contractile organs in humans.

Publisher

Wiley

Subject

Cell Biology,Clinical Biochemistry,Physiology

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