Department of Dermatology, Tel Aviv Sourasky Medical Center, Israel.
Br J Dermatol. 2011 Mar;164(3):610-6. doi: 10.1111/j.1365-2133.2010.10133.x. Epub 2011 Feb 17.
CEDNIK (cerebral dysgenesis, neuropathy, ichthyosis and keratoderma) syndrome is a rare genodermatosis which was shown 5 years ago in one family to be associated with a loss-of-function mutation in SNAP29, encoding a member of the SNARE family of proteins. Decrease in SNAP29 expression was found to result in abnormal lamellar granule maturation leading to aberrant epidermal differentiation and ichthyosis.
To delineate the molecular consequences of disease-causing mutations in SNAP29.
We used direct sequencing, in vitro mutagenesis and three-dimensional organotypic cell cultures.
We identified a novel homozygous insertion in SNAP29 (c.486insA) in two sibs presenting with ichthyosis and dysgenesis of the corpus callosum. In vitro transfection experiments indicated that this mutation results in SNAP29 loss-of-function. Further substantiating this notion, we could replicate histological features typical for CEDNIK syndrome in three-dimensional primary human keratinocyte organotypic cell cultures downregulated for SNAP29.
The identification of a second mutation in SNAP29 in the present study definitely establishes a causal relationship between defective function of SNAP29 and the pleiotropic manifestations of CEDNIK syndrome. Our present and previous data position SNAP29 as an essential component of the epidermal differentiation machinery.
CEDNIK(脑发育不良、神经病、鱼鳞癣和角化过度)综合征是一种罕见的遗传性皮肤病,五年前在一个家族中发现与 SNAP29 的功能丧失突变有关,该基因编码 SNARE 家族蛋白的成员。发现 SNAP29 表达减少导致板层颗粒成熟异常,导致表皮分化和鱼鳞癣异常。
阐明 SNAP29 致病突变的分子后果。
我们使用直接测序、体外诱变和三维器官培养。
我们在两名患有鱼鳞癣和胼胝体发育不良的同胞中发现了 SNAP29 中的一个新的纯合插入突变(c.486insA)。体外转染实验表明该突变导致 SNAP29 功能丧失。进一步证实了这一观点,我们可以在下调 SNAP29 的三维原代人角质形成细胞器官培养物中复制出CEDNIK 综合征的典型组织学特征。
本研究中 SNAP29 的第二个突变的鉴定明确确立了 SNAP29 功能缺陷与 CEDNIK 综合征的多效性表现之间的因果关系。我们目前和以前的数据将 SNAP29 定位为表皮分化机制的重要组成部分。
