Cooper Medical School of Rowan University, Camden, New Jersey, USA.
Division of Genetics, Cooper University Healthcare, Camden, New Jersey, USA.
Clin Genet. 2024 Oct;106(4):518-524. doi: 10.1111/cge.14578. Epub 2024 Jun 18.
The p21-activated kinase (PAK) family of proteins regulates various processes requiring dynamic cytoskeleton organization such as cell adhesion, migration, proliferation, and apoptosis. Among the six members of the protein family, PAK2 is specifically involved in apoptosis, angiogenesis, or the development of endothelial cells. We report a novel de novo heterozygous missense PAK2 variant, p.(Thr406Met), found in a newborn with clinical manifestations of Knobloch syndrome. In vitro experiments indicated that this and another reported variant, p.(Asp425Asn), result in substantially impaired protein kinase activity. Similar findings were described previously for the PAK2 p.(Glu435Lys) variant found in two siblings with proposed Knobloch syndrome type 2 (KNO2). These new variants support the association of PAK2 kinase deficiency with a second, autosomal dominant form of Knobloch syndrome: KNO2.
p21 激活激酶 (PAK) 家族蛋白调节多种需要动态细胞骨架组织的过程,如细胞黏附、迁移、增殖和凋亡。在该蛋白家族的六个成员中,PAK2 特别参与凋亡、血管生成或内皮细胞的发育。我们报告了一种新的从头杂合错义 PAK2 变体,p.(Thr406Met),在一个具有 Knobloch 综合征临床表现的新生儿中发现。体外实验表明,该变体和另一个报道的变体,p.(Asp425Asn),导致激酶活性显著受损。先前在具有拟议的 Knobloch 综合征 2 型 (KNO2) 的两个兄弟姐妹中发现的 PAK2 p.(Glu435Lys) 变体也描述了类似的发现。这些新变体支持 PAK2 激酶缺陷与 Knobloch 综合征的第二种常染色体显性形式的关联:KNO2。
