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血管平滑肌细胞中BTEB2转录因子的调控表达:发育和病理表达谱分析显示其作为再狭窄预测因子的意义。

Regulated expression of the BTEB2 transcription factor in vascular smooth muscle cells: analysis of developmental and pathological expression profiles shows implications as a predictive factor for restenosis.

作者信息

Hoshino Y, Kurabayashi M, Kanda T, Hasegawa A, Sakamoto H, Okamoto E, Kowase K, Watanabe N, Manabe I, Suzuki T, Nakano A, Takase S, Wilcox J N, Nagai R

机构信息

Second Department of Internal Medicine, Gunma University School of Medicine, Gunma.

出版信息

Circulation. 2000 Nov 14;102(20):2528-34. doi: 10.1161/01.cir.102.20.2528.

DOI:10.1161/01.cir.102.20.2528
PMID:11076828
Abstract

BACKGROUND

We have previously shown BTEB2, a Krüppel-like zinc finger transcription factor, to regulate expression of the SMemb/NMHC-B gene, which has been implicated in phenotypic modulation of smooth muscle cells (SMCs). The present study was done to assess the developmental and pathological expression profiles of BTEB2 and to further evaluate the clinical relevance of BTEB2 expression in human coronary artery disease.

METHODS AND RESULTS

Immunohistochemistry showed developmentally regulated expression of BTEB2 with abundant expression in fetal but not in adult aortic SMCs of humans and rabbits. In balloon-injured aortas, predominant expression of BTEB2 was seen in neointimal SMCs. Atherectomy specimens obtained from primary and restenotic lesions showed predominant expression of BTEB2 to stellate SMCs. The incidence of restenosis in primary lesions was significantly higher in lesions containing BTEB2-positive cells than in lesions without (55.6% versus 25.0%, P:=0.01).

CONCLUSIONS

The present study shows that BTEB2 expression is developmentally and pathologically regulated. BTEB2 is preferentially expressed in dedifferentiated or activated SMCs. Examination of human coronary artery specimens suggests that primary lesions containing BTEB2-positive cells are associated with higher risk of restenosis than BTEB2-negative lesions. These results suggest that BTEB2 can serve as a molecular marker for phenotypic modulation of vascular SMCs.

摘要

背景

我们之前已表明,Krüppel样锌指转录因子BTEB2可调节SMemb/NMHC-B基因的表达,该基因与平滑肌细胞(SMC)的表型调节有关。本研究旨在评估BTEB2的发育和病理表达谱,并进一步评估BTEB2表达在人类冠状动脉疾病中的临床相关性。

方法与结果

免疫组织化学显示,BTEB2的表达具有发育调控性,在人类和兔的胎儿主动脉SMC中大量表达,而在成年主动脉SMC中不表达。在球囊损伤的主动脉中,BTEB2主要在内膜下SMC中表达。从原发性和再狭窄病变获取的动脉粥样硬化斑块切除标本显示,BTEB2主要在星状SMC中表达。原发性病变中含有BTEB2阳性细胞的病变再狭窄发生率显著高于无BTEB2阳性细胞的病变(55.6%对25.0%,P = 0.01)。

结论

本研究表明,BTEB2的表达受到发育和病理调控。BTEB2在去分化或活化的SMC中优先表达。对人类冠状动脉标本的检查表明,含有BTEB2阳性细胞的原发性病变比BTEB2阴性病变具有更高的再狭窄风险。这些结果表明,BTEB2可作为血管SMC表型调节的分子标志物。

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