Wang J, Niu W, Witte D P, Chernausek S D, Nikiforov Y E, Clemens T L, Sharifi B, Strauch A R, Fagin J A
Division of Endocrinology and Metabolism, University of Cincinnati, Ohio 45267-0547, USA.
Endocrinology. 1998 May;139(5):2605-14. doi: 10.1210/endo.139.5.5986.
Insulin-like growth factor I (IGF-I) has been postulated to function as a smooth muscle cell (SMC) mitogen and to play a role in the pathogenesis of bladder hypertrophy, estrogen-induced uterine growth, and restenosis after arterial angioplasty. IGF-binding protein-4 (IGFBP-4) inhibits IGF-I action in vitro and is the most abundant IGFBP in the rodent arterial wall. To explore the function of this binding protein in vivo, transgenic mouse lines were developed harboring fusion genes consisting of a rat IGFBP-4 complementary DNA cloned downstream of either a -724 bp fragment of the mouse smooth muscle alpha-actin 5'-flanking region (SMP2-BP-4) or -1074 bp, 63 bp of 5'-untranslated region, and 2.5 kb of intron 1 of smooth muscle alpha-actin (SMP8-BP-4). SMP2-BP-4 mice expressed low levels of the exogenous IGFBP-4 messenger RNA (mRNA), which was not specifically targeted to SMC-rich tissue environments, and were therefore not analyzed further. Six SMP8-BP-4 transgenic lines derived from separate founders were characterized. Mating of hemizygous SMP8-BP-4 mice with controls produced about 50% transgenic offspring, with equal sex distribution. Expression of IGFBP-4 mRNA in nontransgenic littermates was maximal in liver and kidney. By contrast, transgenic IGFBP-4 mRNA expression, distinguished because of a smaller transcript size, was confined to SMC-containing tissues, with the following hierarchy: bladder > aorta > stomach = uterus. There was no transgene expression in skeletal muscle, brain, or cardiac myocytes. The abundance of IGFBP-4 measured by Western ligand blotting or by immunoblotting, was 8- to 10-fold higher in aorta and bladder of SMP8-BP-4 mice than in their nontransgenic littermates, with no change in plasma IGFBP-4 levels. Transgenic mice exhibited a significant reduction in wet weight of SMC-rich tissues, including bladder, intestine, aorta, uterus, and stomach, with no change in total body or carcass weight. In situ hybridization showed that transgene expression was targeted exclusively to the muscular layers of the arteries, veins, bladder, ureter, stomach, intestine, and uterus. Overexpression of IGFBP-4 was associated with SMC hypoplasia, a reciprocal phenotype to that of transgenic mice overexpressing IGF-I under control of the same promoter (SMP8-IGF-I). Double transgenic mice derived from mating SMP8-BP-4 with SMP8-IGF-I animals showed a modest decrease in wet weight at selected SMC tissues. Although we cannot exclude that the effects of IGFBP-4 may be IGF independent, these data suggest that IGFBP-4 is a functional antagonist of IGF-I action on SMC in vivo.
胰岛素样生长因子I(IGF-I)被推测可作为平滑肌细胞(SMC)有丝分裂原,并在膀胱肥大、雌激素诱导的子宫生长以及动脉血管成形术后再狭窄的发病机制中发挥作用。胰岛素样生长因子结合蛋白4(IGFBP-4)在体外抑制IGF-I的作用,并且是啮齿动物动脉壁中最丰富的IGFBP。为了在体内探索这种结合蛋白的功能,构建了转基因小鼠品系,其携带由大鼠IGFBP-4互补DNA克隆到小鼠平滑肌α-肌动蛋白5'侧翼区的-724 bp片段(SMP2-BP-4)或-1074 bp、63 bp的5'非翻译区以及2.5 kb的平滑肌α-肌动蛋白内含子1(SMP8-BP-4)下游组成的融合基因。SMP2-BP-4小鼠表达低水平的外源性IGFBP-4信使RNA(mRNA),其并非特异性靶向富含SMC的组织环境,因此未作进一步分析。对来自不同奠基者的6个SMP8-BP-4转基因品系进行了特征分析。半合子SMP8-BP-4小鼠与对照交配产生约50%的转基因后代,性别分布均等。非转基因同窝仔鼠中IGFBP-4 mRNA在肝脏和肾脏中的表达最高。相比之下,转基因IGFBP-4 mRNA表达(因其转录本大小较小而可区分)局限于含SMC的组织,其顺序如下:膀胱>主动脉>胃 = 子宫。在骨骼肌、脑或心肌细胞中无转基因表达。通过Western配体印迹法或免疫印迹法测定的IGFBP-4丰度,在SMP8-BP-4小鼠的主动脉和膀胱中比其非转基因同窝仔鼠高8至10倍,而血浆IGFBP-4水平无变化。转基因小鼠富含SMC的组织(包括膀胱、肠道、主动脉、子宫和胃)的湿重显著降低,而总体重或胴体重无变化。原位杂交显示转基因表达仅靶向动脉、静脉、膀胱、输尿管、胃、肠道和子宫的肌层。IGFBP-4的过表达与SMC发育不全相关,这是与在相同启动子控制下过表达IGF-I的转基因小鼠(SMP8-IGF-I)相反的表型。将SMP8-BP-4与SMP8-IGF-I动物交配产生的双转基因小鼠在选定的SMC组织中湿重略有降低。尽管我们不能排除IGFBP-4的作用可能不依赖于IGF,但这些数据表明IGFBP-4在体内是IGF-I对SMC作用的功能性拮抗剂。
