Kabuki make‐up (Niikawa‐Kuroki) syndrome: A study of 62 patients

Norio Niikawa; Yoshikazu Kuroki; Tadashi Kajii; Nobuo Matsuura; Satoshi Ishikiriyama; Hidefumi Tonoki; Nobuyoshi Ishikawa; Yutaka Yamada; Masafumi Fujita; Hidehiko Umemoto; Yoshihiko Iwama; Ikuko Kondoh; Yoshimitsu Fukushima; Yasushi Nako; Ichiro Matsui; Tatsuhiko Urakami; Sekoiya Aritaki; Michiko Hara; Yasuyuki Suzuki; Hiroyuki Chyo; Yoshitsugu Sugio; Tomoko Hasegawa; Tsutomu Yamanaka; Ryuichi Tsukino; Akira Yoshida; Naoki Nomoto; Satomi Kawahito; Ryozo Aihara; Shigeki Toyota; Atsushi Ieshima; Hiromu Funaki; K Ishitobi; Satoshi Ogura; Toshiaki Furumae; Makoto Yoshino; Yoshiro Tsuji; Tatsuro Kondoh; Tadashi Matsumoto; Kyohko Abe; Naoki Harada; Teruhisa Miike; Shozo Ohdo; Kenji Naritomi; A. K. Abushwereb; O. H. Braun; E. E. Schmid; John M. Opitz; James F. Reynolds

doi:10.1002/ajmg.1320310312

Kabuki make‐up (Niikawa‐Kuroki) syndrome: A study of 62 patients

Norio Niikawa(Nagasaki University), Yoshikazu Kuroki(Kanagawa Children's Medical Center), Tadashi Kajii(Yamaguchi University), Nobuo Matsuura(Sapporo University), Satoshi Ishikiriyama(Sapporo University), Hidefumi Tonoki(Sapporo University), Nobuyoshi Ishikawa(Japanese Red Cross Hokkaido College of Nursing), Yutaka Yamada(Hakodate National Hospital), Masafumi Fujita(Asahikawa University), Hidehiko Umemoto(Asahikawa University), Yoshihiko Iwama(Dokkyo University), Ikuko Kondoh(University of Tsukuba), Yoshimitsu Fukushima(Saitama Children's Medical Center), Yasushi Nako(Gunma Chuo Hospital), Ichiro Matsui, Tatsuhiko Urakami(Tokyo National Hospital), Sekoiya Aritaki, Michiko Hara, Yasuyuki Suzuki(Hebei Rehabilitation Hospital), Hiroyuki Chyo(Hebei Rehabilitation Hospital), Yoshitsugu Sugio(Kanagawa Children's Medical Center), Tomoko Hasegawa(Shizuoka Children's Hospital), Tsutomu Yamanaka(Aichi Developmental Disability Center), Ryuichi Tsukino(Wakayama Medical University), Akira Yoshida(Kyoto Medical Center), Naoki Nomoto(Kyoto Medical Center), Satomi Kawahito(Tokushima University), Ryozo Aihara(Tokushima University), Shigeki Toyota(Kagawa University), Atsushi Ieshima(National Institute of Technology, Yonago College), Hiromu Funaki(National Institute of Technology, Yonago College), K Ishitobi(Tottori University), Satoshi Ogura(Hiroshima Prefectural Hospital), Toshiaki Furumae(Hiroshima Prefectural Hospital), Makoto Yoshino(Kurume University), Yoshiro Tsuji(Nagasaki University), Tatsuro Kondoh(Nagasaki University), Tadashi Matsumoto(Kumamoto University), Kyohko Abe, Naoki Harada, Teruhisa Miike(Nagasaki University), Shozo Ohdo(Miyazaki Welfare Medical College), Kenji Naritomi(University of the Ryukyus), A. K. Abushwereb(University of Tripoli), O. H. Braun(Pforzheim University of Applied Sciences), E. E. Schmid(Pforzheim University of Applied Sciences), John M. Opitz, James F. Reynolds

American Journal of Medical Genetics

November 1, 1988

10.1002/ajmg.1320310312

Cited by 457

Abstract

These 62 patients with the Kabuki make-up syndrome (KMS) were collected in a collaborative study among 33 institutions and analyzed clinically, cytogenetically, and epidemiologically to delineate the phenotypic spectrum of KMS and to learn about its cause. Among various manifestations observed, most patients had the following five cardinal manifestations: 1) a peculiar face (100%) characterized by eversion of the lower lateral eyelid; arched eyebrows, with sparse or dispersed lateral one-third; a depressed nasal tip; and prominent ears; 2) skeletal anomalies (92%), including brachydactyly V and a deformed spinal column, with or without sagittal cleft vertebrae; 3) dermatoglyphic abnormalities (93%), including increased digital ulnar loop and hypothenar loop patterns, absence of the digital triradius c and/or d, and presence of fingertip pads; 4) mild to moderate mental retardation (92%); and 5) postnatal growth deficiency (83%). Thus the core of the phenotypic spectrum of KMS is rather narrow and clearly defined. Many other inconsistent anomalies were observed. Important among them were early breast development in infant girls (23%), and congenital heart defects (31%), such as a single ventricle with a common atrium, ventricular septal defect, atrial septal defect, tetralogy of Fallot, coarctation of aorta, patent ductus arteriosus, aneurysm of aorta, transposition of great vessels, and right bundle branch block. Of the 62 KMS patients, 58 were Japanese, an indication that the syndrome is fairly common in Japan. It was estimated that its prevalence in Japanese newborn infants is 1/32,000. All the KMS cases in this study were sporadic, the sex ratio was even, there was no correlation with birth order, the consanguinity rate among the parents was not high, and no incriminated agent was found that was taken by the mothers during early pregnancy. Three of the 62 patients had a Y chromosome abnormality involving a possible common breakpoint (Yp11.2). This could indicate another possibility, i.e., that the KMS gene is on Yp11.2 and that the disease is pseudoautosomal dominant. These findings are compatible with an autosomal dominant disorder in which every patient represents a fresh mutation. The mutation rate was calculated at 15.6 X 10(6).

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