Gil-Rodríguez María Concepción, Deardorff Matthew A, Ansari Morad, Tan Christopher A, Parenti Ilaria, Baquero-Montoya Carolina, Ousager Lilian B, Puisac Beatriz, Hernández-Marcos María, Teresa-Rodrigo María Esperanza, Marcos-Alcalde Iñigo, Wesselink Jan-Jaap, Lusa-Bernal Silvia, Bijlsma Emilia K, Braunholz Diana, Bueno-Martinez Inés, Clark Dinah, Cooper Nicola S, Curry Cynthia J, Fisher Richard, Fryer Alan, Ganesh Jaya, Gervasini Cristina, Gillessen-Kaesbach Gabriele, Guo Yiran, Hakonarson Hakon, Hopkin Robert J, Kaur Maninder, Keating Brendan J, Kibaek María, Kinning Esther, Kleefstra Tjitske, Kline Antonie D, Kuchinskaya Ekaterina, Larizza Lidia, Li Yun R, Liu Xuanzhu, Mariani Milena, Picker Jonathan D, Pié Ángeles, Pozojevic Jelena, Queralt Ethel, Richer Julie, Roeder Elizabeth, Sinha Anubha, Scott Richard H, So Joyce, Wusik Katherine A, Wilson Louise, Zhang Jianguo, Gómez-Puertas Paulino, Casale César H, Ström Lena, Selicorni Angelo, Ramos Feliciano J, Jackson Laird G, Krantz Ian D, Das Soma, Hennekam Raoul C M, Kaiser Frank J, FitzPatrick David R, Pié Juan
Unit of Clinical Genetics and Functional Genomics, Departments of Pharmacology-Physiology and Pediatrics, Medical School, University of Zaragoza, CIBERER-GCV and ISS-Aragon, Zaragoza, Spain.
Hum Mutat. 2015 Apr;36(4):454-62. doi: 10.1002/humu.22761. Epub 2015 Mar 17.
Cornelia de Lange syndrome (CdLS) is characterized by facial dysmorphism, growth failure, intellectual disability, limb malformations, and multiple organ involvement. Mutations in five genes, encoding subunits of the cohesin complex (SMC1A, SMC3, RAD21) and its regulators (NIPBL, HDAC8), account for at least 70% of patients with CdLS or CdLS-like phenotypes. To date, only the clinical features from a single CdLS patient with SMC3 mutation has been published. Here, we report the efforts of an international research and clinical collaboration to provide clinical comparison of 16 patients with CdLS-like features caused by mutations in SMC3. Modeling of the mutation effects on protein structure suggests a dominant-negative effect on the multimeric cohesin complex. When compared with typical CdLS, many SMC3-associated phenotypes are also characterized by postnatal microcephaly but with a less distinctive craniofacial appearance, a milder prenatal growth retardation that worsens in childhood, few congenital heart defects, and an absence of limb deficiencies. While most mutations are unique, two unrelated affected individuals shared the same mutation but presented with different phenotypes. This work confirms that de novo SMC3 mutations account for ∼ 1%-2% of CdLS-like phenotypes.
科妮莉亚·德朗格综合征(CdLS)的特征为面部畸形、生长发育迟缓、智力障碍、肢体畸形以及多器官受累。编码黏连蛋白复合体亚基(SMC1A、SMC3、RAD21)及其调节因子(NIPBL、HDAC8)的五个基因发生突变,导致至少70%的CdLS患者或具有CdLS样表型的患者发病。迄今为止,仅发表过一例SMC3突变的CdLS患者的临床特征。在此,我们报告一项国际研究与临床合作成果,对16例由SMC3突变引起的具有CdLS样特征的患者进行临床比较。对突变对蛋白质结构影响的建模表明,其对多聚体黏连蛋白复合体具有显性负效应。与典型的CdLS相比,许多与SMC3相关的表型还具有出生后小头畸形的特征,但颅面部外观特征不那么明显,产前生长迟缓较轻,在儿童期会加重,先天性心脏缺陷较少,且无肢体缺陷。虽然大多数突变是独特的,但两名无亲缘关系的患者共享相同的突变却表现出不同的表型。这项研究证实,新发SMC3突变约占CdLS样表型的1%-2%。
