Masahide Ikema scite author profile

Background Desbuquois dysplasia (DD) is a recessively inherited condition characterised by short stature, generalised skeletal dysplasia and advanced bone maturation. DD is both clinically and radiographically heterogeneous, and two subtypes have been distinguished based on the presence (type 1) or absence (type 2) of an accessory metacarpal bone. In addition, an apparently distinct variant without additional metacarpal bone but with short metacarpals and long phalanges (Kim variant) has been described recently. Mutations in the gene that encodes for CANT1 (calcium-activated nucleotidase 1) have been identified in a subset of patients with DD type 1. Methods A series of 11 subjects with DD from eight families (one type 1, two type 2, five Kim variant) were examined for CANT1 mutations by direct sequencing of all coding exons and their flanking introns. Results Eight distinct mutations were identified in seven families (one type 1, one type 2 and all 5 Kim variant): three were nonsense and five were missense. All missense mutations occurred at highly conserved amino acids in the nucleotidase conserved regions of CANT1. Measurement of nucleotidase activity in vitro showed that the missense mutations were all associated with loss-of-function. Conclusion The clinical-radiographic spectrum produced by CANT1 mutations must be extended to include DD type 2 and Kim variant. While presence or absence of an additional metacarpal ossification centre has been used to distinguish subtypes of DD, this sign is not a distinctive criterion to predict the molecular basis in DD.

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A novel filamentous phage, fs-2, of Vibrio cholerae 0139

Ikema

Honma²

1998

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A novel filamentous bacteriophage, fs-2, was isolated from Vibrio cholerae 0139 strain MD014. The fs-2 phage was a long filamentous particle 1200 nm long and 7 nm wide. The purified phage formed a turbid plaque when spotted on a lawn of the host organisms. The plaque-formation activity was stable following heating to 70 "C but was inhibited by treatment with chloroform. fs-2 had a single-stranded DNA genome and was converted to a double-stranded replicative form in the host cell. Almost all V. cholerae 0139 and 01 El Tor biotype strains tested were sensitive to the phage, but most 01 classical strains and non-01 non-0139 strains were resistant. The fs-2 genome comprised 8651 nucleotides containing nine open reading frames, five of which had predicted protein products partially homologous to the reported protein products of other filamentous phages. Although the extent of the homology was not particularly high, the genetic organization of other filamentous phages appears t o be preserved in fs-2. The phage was not integrated into the chromosome of ifs host, but a 715 nucleotide fragment located in the large intergenic region of fs-2 was highly homologous to a part of region RS2 (repetitive sequence 2) of the V. cholerae CTXQ, sequence which is speculated t o be required for integration of the phage into the W. -cholerae chromosome at a specific site.

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Molecular analysis of a filamentous phage (fsl) of Vibrio cholerae O139

Honma

Ikema

Toma

et al. 1997

Biochimica et Biophysica Acta (BBA) - Molecular Basis of Diseas

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A Filamentous Phage of Vibrio parahaemolyticus O3:K6 Isolated in Laos

Nakasone

Ikema

Higa

et al. 1999

Microbiology and Immunology

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A founder mutation of CANT1 common in Korean and Japanese Desbuquois dysplasia

et al. 2011

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Desbuquois dysplasia (DBQD) is a severe skeletal dysplasia of autosomal recessive inheritance. DBQD is classified into types 1 and 2 based on presence or absence of hand anomalies. In a previous study, we found a CANT1 (for calcium-activated nucleotidase 1) mutation, c.676G4A in five DBQD families. They were all East Asians (Japanese or Korean). The high prevalence of the same mutation among Japanese and Korean suggested that it is a common founder mutation in the two populations. To examine a possible common founder, we examined the region around CANT1 in chromosomes with c.676G4A mutation by genotyping polymorphic markers in the region for the families. We examined their haplotypes using the family data. We identified in all families a common haplotype containing the CANT1 mutation that ranged up to 550 kb. The two unrelated carriers of the mutation in general populations in Korea and Japan could also have the haplotype. We estimated the age of the founder mutation as B1420 years (95% CI¼880-1940 years). The c.676G4A mutation of CANT1 commonly seen in Japanese and Korean DBQD should be derived from a common founder.

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Masahide Ikema

CANT1 mutation is also responsible for Desbuquois dysplasia, type 2 and Kim variant

A novel filamentous phage, fs-2, of Vibrio cholerae 0139

Molecular analysis of a filamentous phage (fsl) of Vibrio cholerae O139

A Filamentous Phage of Vibrio parahaemolyticus O3:K6 Isolated in Laos

A founder mutation of CANT1 common in Korean and Japanese Desbuquois dysplasia

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