Roman Beth L, Pham Van N, Lawson Nathan D, Kulik Magdalena, Childs Sarah, Lekven Arne C, Garrity Deborah M, Moon Randall T, Fishman Mark C, Lechleider Robert J, Weinstein Brant M
Laboratory of Molecular Genetics, National Institute of Child Health and Human Development, National Institutes of Health, Bethesda, MD 20892, USA.
Development. 2002 Jun;129(12):3009-19. doi: 10.1242/dev.129.12.3009.
The zebrafish mutant violet beauregarde (vbg) can be identified at two days post-fertilization by an abnormal circulation pattern in which most blood cells flow through a limited number of dilated cranial vessels and fail to perfuse the trunk and tail. This phenotype cannot be explained by caudal vessel abnormalities or by a defect in cranial vessel patterning, but instead stems from an increase in endothelial cell number in specific cranial vessels. We show that vbg encodes activin receptor-like kinase 1 (Acvrl1; also known as Alk1), a TGFbeta type I receptor that is expressed predominantly in the endothelium of the vessels that become dilated in vbg mutants. Thus, vbg provides a model for the human autosomal dominant disorder, hereditary hemorrhagic telangiectasia type 2, in which disruption of ACVRL1 causes vessel malformations that may result in hemorrhage or stroke. Movies available on-line
斑马鱼突变体紫罗兰保皇党(vbg)在受精后两天可通过异常循环模式识别,即大多数血细胞流经数量有限的扩张颅血管,无法灌注躯干和尾部。这种表型无法用尾血管异常或颅血管模式缺陷来解释,而是源于特定颅血管中内皮细胞数量增加。我们发现vbg编码激活素受体样激酶1(Acvrl1;也称为Alk1),这是一种TGFβ I型受体,主要在内皮细胞中表达,而这些内皮细胞所在的血管在vbg突变体中会扩张。因此,vbg为人类常染色体显性疾病遗传性出血性毛细血管扩张症2型提供了一个模型,其中ACVRL1的破坏会导致血管畸形,可能导致出血或中风。在线观看相关视频
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