Your search keyword '"Junya Fujimura"' showing total 5 results

1. Clinical and genetic variability of PAX2-related disorder in the Japanese population

Author

Shuichi Ito, Tomohiko Yamamura, Junya Fujimura, Tomoko Horinouchi, Koichi Kamei, Hiroshi Kaito, Shogo Minamikawa, Kazumoto Iijima, Ryojiro Tanaka, Nana Sakakibara, Rini Rossanti, Takeshi Ninchoji, Naoya Morisada, Kandai Nozu, and China Nagano

Subjects

0301 basic medicine, Proband, Kidney, Pediatrics, medicine.medical_specialty, business.industry, Hearing loss, Kidney metabolism, Disease, 030105 genetics & heredity, urologic and male genital diseases, medicine.disease, Developmental disorder, 03 medical and health sciences, 030104 developmental biology, medicine.anatomical_structure, Focal segmental glomerulosclerosis, Genetics, medicine, sense organs, medicine.symptom, business, Genetics (clinical), Kidney disease

Abstract

Pathogenic variants of paired box gene 2 (PAX2) cause autosomal-dominant PAX2-related disorder, which includes renal coloboma syndrome (RCS). Patients with PAX2-related disorder present with renal and ophthalmological pathologies, as well as with other abnormalities, including developmental problems and hearing loss. We sequenced PAX2 in 457 patients with congenital anomalies of the kidney and urinary tract or with renal dysfunction of unknown cause and identified 19 different pathogenic variants in 38 patients from 30 families (6.5%). Thirty-four patients had renal hypodysplasia or chronic kidney disease of unknown cause, and three had focal segmental glomerulosclerosis. Although no obvious genotype–phenotype correlation was observed, six of the seven patients who developed end-stage renal disease in childhood had truncating variants. Twenty-three patients had ocular disabilities, mostly optic disc coloboma. Non-renal and non-ophthalmological manifestations included developmental disorder, electrolyte abnormality, and gonadal abnormalities. Two unrelated patients had congenital cystic adenomatoid malformations in their lungs. Six of ten probands with PAX2 mutation identified by next-generation sequencing did not show typical RCS manifestations. We conclude that PAX2-related disorder has a variable clinical presentation and can be diagnosed by next-generation sequencing even in the absence of typical RCS manifestations.

Published

2020

2. Clinical spectrum of male patients with OFD1 mutations

Author

Tomoko Horinouchi, Junya Shimizu, Takuzo Wada, China Nagano, Yuko Shima, Akemi Shono, Toshiyuki Ohta, Shogo Minamikawa, Tomohiko Yamamura, Koichi Nakanishi, Junya Fujimura, Ming Juan Ye, Yoshimi Nozu, Naoya Morisada, Koji Nagatani, Kazumoto Iijima, Nana Sakakibara, and Kandai Nozu

Subjects

0301 basic medicine, Adult, Male, Pediatrics, medicine.medical_specialty, 030105 genetics & heredity, 03 medical and health sciences, Genetics, medicine, Missense mutation, Humans, Global developmental delay, Child, male patients, Genetics (clinical), Cystic kidney, business.industry, Brachydactyly, Proteins, Micropenis, Orofaciodigital Syndromes, medicine.disease, Prognosis, Pedigree, Ciliopathy, 030104 developmental biology, ciliopathy, Child, Preschool, Speech delay, Mutation, Female, Oral-facial-digital syndrome, medicine.symptom, OFD1, business, Kidney disease

Abstract

Oral-facial-digital syndrome type 1 (OFD1) is a ciliopathy characterized by oral, facial, and digital malformations that are often accompanied by polycystic lesion of the kidney and central nervous involvement. OFD1 shows an X-linked recessive inheritance caused by mutation in the OFD1 gene (Xp22.2). The disease is generally considered embryonic lethal for hemizygous males. However, males with OFD1 mutations were recently reported. Here, we report four additional Japanese male patients with OFD1 variants and describe the variable clinical manifestation and disease severity among the four patients. Patient 1 with pathogenic indels including a 19-bp deletion and 4-bp insertion (c.2600–18_2600delinsACCT) had end-stage renal disease (ESRD) with bilateral cystic kidneys and sensory hearing loss. He showed neither intellectual disability nor facial or digital dysmorphism. Patient 2 with a missense variant in exon 7 (c.539 A > T, p.Asp180Val) presented head circumference enlargement, brachydactyly, high-arched palate, micropenis, severe global developmental delay, and ESRD. Patient 3 had a single base substitution at the splice donor site of intron 16 (c.2260 + 2 T > G) causing a 513-bp deletion at the transcript level. The patient had chronic kidney disease and speech delay, but no oral, facial, or digital dysmorphism. His uncle (patient 4) carried the same OFD1 variant and showed ESRD with extra-renal malformations including obesity and micropenis, which was previously diagnosed as Bardet-Biedl syndrome. The OFD1 mutations were not lethal in these four male patients, likely because the three mutations were in-frame or missense. This report provided insights into the onset mechanism and phenotype-genotype association in patients with OFD1 mutations.

Published

2018

3. Development of ultra-deep targeted RNA sequencing for analyzing X-chromosome inactivation in female Dent disease

Author

Naoya Morisada, Hiroshi Kaito, Masuji Hattori, China Nagano, Kyoko Kanda, Yuko Shima, Mariko Taniguchi-Ikeda, Koichi Nakanishi, Tomohiko Yamamura, Hiroaki Nagase, Shogo Minamikawa, Ichiro Morioka, Keita Nakanishi, Yoshimi Nozu, Junya Fujimura, Ryojiro Tanaka, Tomoko Horinouchi, Kazumoto Iijima, Nana Sakakibara, and Kandai Nozu

Subjects

0301 basic medicine, Biopsy, Dent Disease, 030105 genetics & heredity, Biology, Genetic analysis, X-inactivation, law.invention, 03 medical and health sciences, Chloride Channels, X Chromosome Inactivation, law, Leukocytes, Genetics, Humans, Gene, Genetics (clinical), Polymerase chain reaction, Chromosomes, Human, X, Gene Expression Profiling, Genetic Variation, High-Throughput Nucleotide Sequencing, Sequence Analysis, DNA, Pedigree, Gene expression profiling, genomic DNA, 030104 developmental biology, DNA methylation, Female, Transcriptome, Biomarkers

Abstract

The pattern of X-chromosome inactivation (XCI) can affect the clinical severity of X-linked disorders in females. XCI pattern analysis has been conducted mainly by HUMARA assay, a polymerase chain reaction-based assay using a methylation-sensitive restriction enzyme. However, this assay examines the XCI ratio of the androgen receptor gene at the genomic DNA level and does not reflect the ratio of either targeted gene directly or at the mRNA level. Here, we report four females with Dent disease, and we clarified the correlation between XCI and female cases of Dent disease using not only HUMARA assay but also a novel analytical method by RNA sequencing. We constructed genetic analysis for 4 female cases showing high level of urinary low-molecular-weight proteinuria and their parents. Their XCI pattern was analyzed by both HUMARA assay and an ultra-deep targeted RNA sequencing of the CLCN5 gene using genomic DNA and mRNA extracted from both leukocytes and urine sediment. All four cases possessed pathogenic variants of the CLCN5 gene. XCI analysis revealed skewed XCI in only two cases, while the other two showed random XCI. All assay results of HUMARA and targeted RNA sequencing in both leukocytes and urinary sediment were clearly identical in all four cases. We developed a novel XCI analytical assay of ultra-deep targeted RNA sequencing and revealed that skewed XCI explains the mechanism of onset of female Dent disease in only half of such cases.

Published

2018

4. Congenital chloride diarrhea needs to be distinguished from Bartter and Gitelman syndrome

Author

Kazumoto Iijima, Naoya Morisada, Mariko Taniguchi-Ikeda, Natsuki Matsunoshita, Tomohiko Yamamura, Shingo Ishimori, Shogo Minamikawa, Azusa Kawaguchi, Masahide Yoshikane, Takeshi Ninchoji, Keita Nakanishi, Hiroshi Kaito, Ichiro Morioka, Junya Fujimura, Tomoko Horinouchi, Kandai Nozu, Naoya Fujita, and Hiroaki Nagase

Subjects

0301 basic medicine, Diarrhea, Male, Congenital chloride diarrhea, Dent Disease, SLC26A3, Pseudo-Gitelman syndrome, Compound heterozygosity, Bartter syndrome, Diagnosis, Differential, 03 medical and health sciences, symbols.namesake, 0302 clinical medicine, Genetics, medicine, Humans, 030212 general & internal medicine, Child, Genetics (clinical), Genetic testing, Sanger sequencing, biology, medicine.diagnostic_test, Pseudo-Bartter syndrome, Base Sequence, business.industry, Bartter Syndrome, Infant, Sequence Analysis, DNA, Gitelman syndrome, medicine.disease, 030104 developmental biology, biology.protein, symbols, Targeted sequencing, Next-generation sequencing, Female, business, Gitelman Syndrome, Metabolism, Inborn Errors

Abstract

Pseudo-Bartter/Gitelman syndrome (p-BS/GS) encompasses a clinically heterogeneous group of inherited or acquired disorders similar to Bartter syndrome (BS) or Gitelman syndrome (GS), both renal salt-losing tubulopathies. Phenotypic overlap frequently occurs between p-BS/GS and BS/GS, which are difficult to diagnose based on their clinical presentation and require genetic tests for accurate diagnosis. In addition, p-BS/GS can occur as a result of other inherited diseases such as cystic fibrosis, autosomal dominant hypocalcemia, Dent disease, or congenital chloride diarrhea (CCD). However, the detection of the variants in genes other than known BS/GS-causing genes by conventional Sanger sequencing requires substantial time and resources. We studied 27 cases clinically diagnosed with BS/GS, but with negative genetic tests for known BS/GS genes. We conducted targeted sequencing for 22 genes including genes responsible for tubulopathies and other inherited diseases manifesting with p-BS/GS symptoms. We detected the SLC26A3 gene variants responsible for CCD in two patients. In Patient 1, we found the SLC26A3 compound heterozygous variants: c.354delC and c.1008insT. In Patient 2, we identified the compound heterozygous variants: c.877G > A, p.(Glu293Lys), and c.1008insT. Our results suggest that a comprehensive genetic screening system using targeted sequencing is useful for the diagnosis of patients with p-BS/GS with alternative genetic origins.

Published

2018

5. Cryptic exon activation in SLC12A3 in Gitelman syndrome

Author

Naoya Morisada, Shogo Minamikawa, Koichi Nakanishi, Takeshi Ninchoji, Mariko Taniguchi-Ikeda, Tomohiko Yamamura, Kazumoto Iijima, Takao Konomoto, Junya Fujimura, Tomoko Horinouchi, Akemi Shono, Yoshimi Nozu, Igor Vorechovsky, Ichiro Morioka, Keita Nakanishi, Kandai Nozu, and Hiroshi Kaito

Subjects

0301 basic medicine, Candidate gene, 030232 urology & nephrology, Biology, Bioinformatics, medicine.disease_cause, Sudden death, Hypocalciuria, 03 medical and health sciences, 0302 clinical medicine, Tubulopathy, Genetics, medicine, Intronic Mutation, Humans, Solute Carrier Family 12, Member 3, Allele, Kidney Tubules, Distal, Genetics (clinical), Mutation, Base Sequence, High-Throughput Nucleotide Sequencing, Exons, Sequence Analysis, DNA, Gitelman syndrome, medicine.disease, Introns, 030104 developmental biology, Child, Preschool, Female, medicine.symptom, Gitelman Syndrome

Abstract

Gitelman syndrome (GS) is an autosomal recessive renal tubulopathy characterized by hypokalemic metabolic alkalosis with hypocalciuria and hypomagnesemia. GS clinical symptoms range from mild weakness to muscular cramps, paralysis or even sudden death as a result of cardiac arrhythmia. GS is caused by loss-of-function mutations in the solute carrier family 12 member 3 (SLC12A3) gene, but molecular mechanisms underlying such a wide range of symptoms are poorly understood. Here we report cryptic exon activation in SLC12A3 intron 12 in a clinically asymptomatic GS, resulting from an intronic mutation c.1669+297?T>G that created a new acceptor splice site. The cryptic exon was sandwiched between the L3 transposon upstream and a mammalian interspersed repeat downstream, possibly contributing to inclusion of the cryptic exon in mature transcripts. The mutation was identified by targeted next-generation sequencing of candidate genes in GS patients with missing pathogenic SLC12A3 alleles. Taken together, this work illustrates the power of next-generation sequencing to identify causal mutations in intronic regions in asymptomatic individuals at risk of developing potentially fatal disease complications, improving clinical management of these cases

Published

2016