Sinnaeve Peter, Chiche Jean-Daniel, Gillijns Hilde, Van Pelt Natascha, Wirthlin Douglas, Van De Werf Frans, Collen Desire, Bloch Kenneth D, Janssens Stefan
Center for Transgene Technology and Gene Therapy, Flanders Interuniversity Institute for Biotechnology, and the Cardiac Unit, University Hospital Gasthuisberg, University of Leuven, Belgium.
Circulation. 2002 Jun 18;105(24):2911-6. doi: 10.1161/01.cir.0000018169.59205.ca.
Neointima formation after arterial injury is associated with reduced vascular cyclic guanosine monophosphate (cGMP) and cGMP-dependent protein kinase (PKG), a major cGMP effector in vascular smooth muscle. We tested the effect of PKG overexpression on the neointimal response to vascular injury. Methods and Results- Infection of cultured rat aortic smooth muscle cells (RASMCs) with an adenoviral vector specifying a cGMP-independent, constitutively active PKG mutant (AdPKGcat) reduced serum-induced migration by 33% and increased serum-deprivation-induced apoptosis 2-fold (P<0.05 for both). Infection with wild-type PKG (AdPKG), in the absence of cGMP, did not affect migration or apoptosis. Two weeks after balloon-injured rat carotid arteries were infected with 1x 10(10) pfu AdPKGcat (n=12), AdPKG (n=8), or a control adenovirus (n=8), intima-to-media ratio was less in AdPKGcat-infected arteries than in AdPKG- or control adenovirus-infected vessels (0.26+/-0.06 versus 0.61+/-0.12 and 0.70+/-0.12, respectively, P<0.05 for both). Two weeks after intramural administration of 1.75x10(10) pfu AdPKGcat (n=8) or a control adenovirus (n=8) into porcine coronary arteries with in-stent restenosis, luminal diameter was greater in AdPKGcat-infected arteries than in control adenovirus-infected vessels (2.32+/-0.16 versus 1.81+/-0.13 mm, P=0.028), associated with reduced neointimal area (3.30+/-0.24 versus 4.15+/-0.13 mm(2), P=0.008), neointima-to-vessel area ratio (0.42+/-0.05 versus 0.58+/-0.04, P<0.05), and percent stenosis (45+/-6% versus 70+/-4%, P<0.05).
Expression of a constitutively active PKG reduces neointima formation after balloon injury in rats and reduces coronary in-stent restenosis in pigs. PKGcat gene transfer may be a promising strategy for vasculoproliferative disorders.
动脉损伤后的新生内膜形成与血管环磷酸鸟苷(cGMP)及cGMP依赖性蛋白激酶(PKG,血管平滑肌中主要的cGMP效应器)减少有关。我们测试了PKG过表达对血管损伤后新生内膜反应的影响。
用一种腺病毒载体感染培养的大鼠主动脉平滑肌细胞(RASMCs),该载体携带一种不依赖cGMP的、组成型激活的PKG突变体(AdPKGcat),可使血清诱导的迁移减少33%,并使血清剥夺诱导的凋亡增加2倍(两者P均<0.05)。在无cGMP的情况下,用野生型PKG(AdPKG)感染对迁移或凋亡无影响。在用1×10¹⁰ pfu AdPKGcat(n = 12)、AdPKG(n = 8)或对照腺病毒(n = 8)感染大鼠颈动脉球囊损伤两周后,AdPKGcat感染动脉的内膜中膜比低于AdPKG或对照腺病毒感染的血管(分别为0.26±0.06、0.61±0.12和0.70±0.12,两者P均<0.05)。在用1.75×10¹⁰ pfu AdPKGcat(n = 8)或对照腺病毒(n = 8)向有支架内再狭窄的猪冠状动脉壁内给药两周后,AdPKGcat感染动脉的管腔直径大于对照腺病毒感染的血管(2.32±0.16对1.81±0.13 mm,P = 0.028),同时新生内膜面积减少(3.30±0.24对4.15±0.13 mm²,P = 0.008),新生内膜与血管面积比降低(0.42±0.05对0.58±0.04,P<0.05),狭窄百分比降低(45±6%对70±4%,P<0.05)。
组成型激活的PKG表达可减少大鼠球囊损伤后的新生内膜形成,并减少猪冠状动脉支架内再狭窄。PKGcat基因转移可能是治疗血管增殖性疾病的一种有前景的策略。
