Russell Theron A, Ito Masafumi, Ito Mika, Yu Richard N, Martinson Fred A, Weiss Jeffrey, Jameson J Larry
Department of Endocrinology, Metabolism, and Molecular Medicine, Northwestern University Feinberg School of Medicine, 251 East Huron Street, Chicago, Illinois 60611, USA.
J Clin Invest. 2003 Dec;112(11):1697-706. doi: 10.1172/JCI18616.
Familial neurohypophyseal diabetes insipidus (FNDI) is an autosomal dominant disorder caused by mutations in the arginine vasopressin (AVP) precursor. The pathogenesis of FNDI is proposed to involve mutant protein-induced loss of AVP-producing neurons. We established murine knock-in models of two different naturally occurring human mutations that cause FNDI. A mutation in the AVP signal sequence [A(-1)T] is associated with a relatively mild phenotype or delayed presentation in humans. This mutation caused no apparent phenotype in mice. In contrast, heterozygous mice expressing a mutation that truncates the AVP precursor (C67X) exhibited polyuria and polydipsia by 2 months of age and these features of DI progressively worsened with age. Studies of the paraventricular and supraoptic nuclei revealed induction of the chaperone protein BiP and progressive loss of AVP-producing neurons relative to oxytocin-producing neurons. In addition, Avp gene products were not detected in the neuronal projections, suggesting retention of WT and mutant AVP precursors within the cell bodies. In summary, this murine model of FNDI recapitulates many features of the human disorder and demonstrates that expression of the mutant AVP precursor leads to progressive neuronal cell loss.
家族性神经垂体性尿崩症(FNDI)是一种常染色体显性疾病,由精氨酸加压素(AVP)前体的突变引起。FNDI的发病机制被认为涉及突变蛋白诱导的AVP产生神经元的丧失。我们建立了两种不同的导致FNDI的自然发生的人类突变的小鼠基因敲入模型。AVP信号序列中的一个突变[A(-1)T]与人类相对较轻的表型或延迟表现相关。该突变在小鼠中未引起明显的表型。相比之下,表达截断AVP前体的突变(C67X)的杂合小鼠在2月龄时出现多尿和烦渴,并且这些尿崩症特征随着年龄的增长而逐渐恶化。对室旁核和视上核的研究显示伴侣蛋白BiP的诱导以及相对于催产素产生神经元而言AVP产生神经元的逐渐丧失。此外,在神经投射中未检测到Avp基因产物,这表明野生型和突变型AVP前体保留在细胞体内。总之,这种FNDI小鼠模型概括了人类疾病的许多特征,并证明突变型AVP前体的表达导致神经元细胞的逐渐丧失。
