Capillary pericytes express α-smooth muscle actin, which requires prevention of filamentous-actin depolymerization for detection

毛细血管周细胞表达 α-平滑肌肌动蛋白,需要防止丝状肌动蛋白解聚才能检测

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作者:Luis Alarcon-Martinez #, Sinem Yilmaz-Ozcan #, Muge Yemisci, Jesse Schallek, Kıvılcım Kılıç, Alp Can, Adriana Di Polo, Turgay Dalkara

Abstract

Recent evidence suggests that capillary pericytes are contractile and play a crucial role in the regulation of microcirculation. However, failure to detect components of the contractile apparatus in capillary pericytes, most notably α-smooth muscle actin (α-SMA), has questioned these findings. Using strategies that allow rapid filamentous-actin (F-actin) fixation (i.e. snap freeze fixation with methanol at -20°C) or prevent F-actin depolymerization (i.e. with F-actin stabilizing agents), we demonstrate that pericytes on mouse retinal capillaries, including those in intermediate and deeper plexus, express α-SMA. Junctional pericytes were more frequently α-SMA-positive relative to pericytes on linear capillary segments. Intravitreal administration of short interfering RNA (α-SMA-siRNA) suppressed α-SMA expression preferentially in high order branch capillary pericytes, confirming the existence of a smaller pool of α-SMA in distal capillary pericytes that is quickly lost by depolymerization. We conclude that capillary pericytes do express α-SMA, which rapidly depolymerizes during tissue fixation thus evading detection by immunolabeling.

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