Your search keyword '"Tsutomu Ogata"' showing total 650 results

151. SHOX Haploinsufficiency as a Cause of Syndromic and Nonsyndromic Short Stature

Author

Tsutomu Ogata, Atsuhito Seki, and Maki Fukami

Subjects

0301 basic medicine, Genetics, business.industry, Pseudoautosomal region, Review Article, medicine.disease, Short stature, Idiopathic short stature, Growth hormone treatment, 03 medical and health sciences, Exon, 030104 developmental biology, Short Stature Homeobox Protein, Turner syndrome, Medicine, medicine.symptom, business, Haploinsufficiency, Genetics (clinical)

Abstract

SHOX in the short arm pseudoautosomal region (PAR1) of sex chromosomes is one of the major growth genes in humans. SHOX haploinsufficiency results in idiopathic short stature and Léri-Weill dyschondrosteosis and is associated with the short stature of patients with Turner syndrome. The SHOX protein likely controls chondrocyte apoptosis by regulating multiple target genes including BNP, Fgfr3, Agc1, and Ctgf. SHOX haploinsufficiency frequently results from deletions and duplications in PAR1 involving SHOX exons and/or the cis-acting enhancers, while exonic point mutations account for a small percentage of cases. The clinical severity of SHOX haploinsufficiency reflects hormonal conditions rather than mutation types. Growth hormone treatment seems to be beneficial for cases with SHOX haploinsufficiency, although the long-term outcomes of this therapy require confirmation. Future challenges in SHOX research include elucidating its precise function in the developing limbs, identifying additional cis-acting enhancers, and determining optimal therapeutic strategies for patients.

Published

2016

152. A Chronic Graft-versus-host Disease Case after Improvement of Basedow's Disease developed after Allogeneic Bone Marrow Transplantation

Author

Hiroyoshi Takahashi, Toshiki Nakanishi, Eiichiro Satake, Tsutomu Ogata, Kimiyoshi Sakaguchi, Daisuke Shimizu, and Rie Matsushita

Subjects

medicine.medical_specialty, Graft-versus-host disease, Marrow transplantation, business.industry, medicine, Disease, Autogenous bone, business, medicine.disease, Surgery

Published

2016

153. Chromosome 6q24 methylation defects are uncommon in childhood-onset non-autoimmune diabetes mellitus patients born appropriate- or large-for-gestational age

Author

Ichiro Yokota, Misako Okuno, Toru Kikuchi, Shin Amemiya, Nobuyuki Kikuchi, Adolescent Diabetes, Junichi Suzuki, Tomoyuki Kawamura, Masayo Kagami, Tadayuki Ayabe, Shigetaka Sugihara, Tohru Yorifuji, Tsutomu Ogata, Tatsuhiko Urakami, and Maki Fukami

Subjects

0301 basic medicine, medicine.medical_specialty, Short Communication, Endocrinology, Diabetes and Metabolism, 030209 endocrinology & metabolism, Locus (genetics), 03 medical and health sciences, 0302 clinical medicine, Endocrinology, Diabetes mellitus, Internal medicine, medicine, Imprinting (psychology), Allele, diabetes, business.industry, Gestational age, 6q24, Methylation, medicine.disease, Phenotype, Uniparental disomy, pyrosequencing, 030104 developmental biology, Pediatrics, Perinatology and Child Health, methylation, imprinting, business

Abstract

Methylation defects in the imprinting locus at chromosome 6q24 result in transient neonatal diabetes and small-for-gestational age (SGA) births (1). These phenotypes are primarily ascribed to the overexpression of PLAGL1, a paternally expressed gene on 6q24 that regulates cell cycle and apoptosis (2). Paternal uniparental disomy involving 6q24, as well as copy-number gains of paternal PLAGL1 alleles and epimutations in maternal alleles, have been identified as the causes of hypomethylation at the differentially methylated region (DMR) of PLAGL1 (3, 4). Recently, Yorifuji et al. reported the identification of 6q24 uniparental disomy in three patients with childhood-onset non-autoimmune diabetes mellitus (5). The three patients were identified through methylation-specific PCR analysis of the PLAGL1 DMR of 113 patients clinically suspected of having maturity-onset diabetes of the young (MODY). These results expanded the phenotypic consequences of 6q24 methylation defects to include MODY-like manifestations without a history of neonatal diabetes. However, the frequency of 6q24 methylation defects among patients with childhood-onset non-autoimmune diabetes remained unknown.

Published

2016

154. Extra-adrenal induction of Cyp21a1 ameliorates systemic steroid metabolism in a mouse model of congenital adrenal hyperplasia

Author

Noriyuki Katsumata, Yasuhiro Naiki, Songya Pang, Reiko Horikawa, Maki Fukami, Tsutomu Ogata, Mami Miyado, and Masafumi Onodera

Subjects

0301 basic medicine, medicine.medical_specialty, endocrine system diseases, medicine.drug_class, Steroid 21-Hydroxylase, Endocrinology, Diabetes and Metabolism, medicine.medical_treatment, Genetic enhancement, urologic and male genital diseases, Viral vector, Steroid, 03 medical and health sciences, Endocrinology, Internal medicine, medicine, Congenital adrenal hyperplasia, business.industry, Extra-Adrenal, nutritional and metabolic diseases, medicine.disease, 030104 developmental biology, Mineralocorticoid, business, Glucocorticoid, medicine.drug

Abstract

Congenital adrenal hyperplasia (CAH) due to steroid 21-hydroxylase (21-OH) deficiency (21-OHD) is an autosomal recessive disorder, in which CYP21A2 mutations or deletions result in underproduction of glucocorticoid and mineralocorticoid, and overproduction of androgens. Patients with CAH are treated with oral steroid supplementation, but optimal control of blood steroid levels remains difficult. Thus, new therapeutic approaches are still needed. Previously, adenovirus-mediated administration of human CYP21A2 to adrenal glands rescued the phenotype of a mouse model of 21-OHD. In this study, we examined whether transduction of murine Cyp21a1 in extra-adrenal tissues could rescue steroid metabolism in 21-OHD mice. We transduced primary fibroblasts obtained from 21-OHD mice with a retroviral vector containing Cyp21a1. In vitro assays demonstrated that Cyp21a1-expressing fibroblasts can uptake progesterone from the culture media, convert it to deoxycorticosterone (DOC), and subsequently release DOC back into the media. Autotransplantation of Cyp21a1-expressing fibroblasts into the subcutaneous tissues of the back resulted in a significant reduction in the serum progesterone/DOC ratio in four of six 21-OHD mice at 4 weeks after injection. We also directly injected an adeno-associated viral vector containing Cyp21a1 into the thigh muscles of 21-OHD mice. Serum progesterone/DOC ratios were markedly reduced in all four animals at 4 weeks after injection. These results indicate that extra-adrenal induction of Cyp21a1 ameliorates steroid metabolism in 21-OHD mice. This study suggests a novel therapeutic strategy for congenital adrenal hyperplasia, which warrants further investigations.

Published

2016

155. Classic and non-classic 21-hydroxylase deficiency can be discriminated from P450 oxidoreductase deficiency in Japanese infants by urinary steroid metabolites

Author

Mitsuru Murata, Tomonobu Hasegawa, Kazushige Ikeda, Keiko Homma, Yuhei Koyama, Tsutomu Ogata, Maki Fukami, and Masayuki Miwa

Subjects

0301 basic medicine, medicine.medical_specialty, Pregnanetriolone, Endocrinology, Diabetes and Metabolism, medicine.medical_treatment, Urinary system, 030209 endocrinology & metabolism, Biochemical diagnosis, Steroid, 03 medical and health sciences, chemistry.chemical_compound, 0302 clinical medicine, Endocrinology, non-classical 21-hydroxylase deficiency, Internal medicine, cytochrome P450 oxidoreductase deficiency, Medicine, Tetrahydrocortisone, Creatinine, biology, business.industry, 21-Hydroxylase, urinary steroid metabolites, 030104 developmental biology, chemistry, Pediatrics, Perinatology and Child Health, biology.protein, P450 Oxidoreductase Deficiency, Original Article, business

Abstract

We previously reported a two-step biochemical diagnosis to discriminate classic 21-hydroxylase deficiency (C21OHD) from P450 oxidoreductase deficiency (PORD) by using urinary steroid metabolites: the pregnanetriolone/tetrahydrocortisone ratio (Ptl / the cortisol metabolites 5α- and 5β-tetrahydrocortisone (sum of these metabolites termed THEs), and 11β-hydroxyandrosterone (11OHAn). The objective of this study was to investigate whether both C21OHD and non-classic 21OHD (C+NC21OHD) could be biochemically differentiated from PORD. We recruited 55 infants with C21OHD, 8 with NC21OHD, 16 with PORD, 57 with transient hyper-17α-hydroxyprogesteronemia (TH17OHP), and 2,473 controls. All infants were Japanese with ages between 0–180 d. In addition to Ptl, THEs, and 11OHAn, we measured urinary tetrahydroaldosterone (THAldo) and pregnenediol (PD5). The first step: by Ptl with the age-specific cutoffs 0.06 mg/g creatinine (0–10 d of age) and 0.3 mg/g creatinine (11–180 d of age), we were able to differentiate C+NC21OHD and PORD from TH17OHP and controls (0–10 d of age: 0.065–31 vs. < 0.001–0.052, 11–180 d of age: 0.40–42 vs. < 0.001–0.086) with 100% sensitivity and specificity. The second step: by the 11OHAn/THAldo or 11OHAn/PD5 ratio with a cutoff of 0.80 or 1.0, we were able to discriminate between C+NC21OHD and PORD (1.0–720 vs. 0.021–0.61 or 1.8–160 vs. 0.005–0.32, respectively) with 100% sensitivity and specificity. Ptl, 11OHAn/THAldo, and 11OHAn/PD5 could differentiate between C+NC21OHD and PORD in Japanese infants.

Published

2016

156. Long-term clinical course in three patients with MAMLD1 mutations

Author

Ayumi Uematsu, Tomonobu Hasegawa, Koji Muroya, Yasuko Fujisawa, Tsutomu Ogata, and Maki Fukami

Subjects

0301 basic medicine, medicine.medical_specialty, Endocrinology, Diabetes and Metabolism, Urology, 030209 endocrinology & metabolism, 03 medical and health sciences, Basal (phylogenetics), 0302 clinical medicine, Endocrinology, Hypergonadotropic hypogonadism, medicine, Sex organ, Testosterone, Gynecology, biology, business.industry, biology.organism_classification, medicine.disease, Pubic hair, Penoscrotal hypospadias, 030104 developmental biology, medicine.anatomical_structure, Microphallus, medicine.symptom, Chordee, business

Abstract

Although MAMLD1 on chromosome Xq28 is known as a causative gene for 46,XY disorders of sex development, clinical information is virtually limited in patients of infancy to early childhood. Here, we report long-term genital and hormonal findings in three previously described Japanese patients with MAMLD1 mutations, i.e., patients 1 and 2 with p.E197X and patient 3 with p.R726X. As previously reported, patients 1-3 exhibited penoscrotal hypospadias with chordee, microphallus, bifid/hypoplastic scrotum, and/or bilateral cryptorchidism/retractile testes, in the presence of sufficiently high serum basal or hCG-stimulated testosterone values in the mini-pubertal period to early childhood. Subsequently, patient 1 had low serum hCG-stimulated testosterone value (126 ng/dL) at 13 11/12 years of age, and manifested microphallus (4.5 cm), relatively small testes (left 8 mL and right 10 mL), Tanner stage 3 genitalia and pubic hair development at 18 3/12 years of age. Similarly, patients 2 and 3 showed mild hypergonadotropic hypogonadism at 7 0/12 and 9 9/12 years of age, respectively, with serum GnRH-stimulated LH values of 5.5 and 7.2 mIU/mL and FSH values of 10.3 and 19.8 mIU/mL and hCG-stimulated testosterone values of 70 and 80 ng/dL, respectively. Testis ultrasound studies delineated microlithiasis in patients 1 and 3. These results imply for the first time deterioration of testicular function with age in patients with pathologic MAMLD1 mutations.

Published

2016

157. TSC1 intragenic deletion transmitted from a mosaic father to two siblings with cardiac rhabdomyomas: Identification of two aberrant transcripts

Author

Yohei Masunaga, Tsutomu Ogata, Hiroki Uchiyama, Hirotomo Saitsu, Takamichi Ishikawa, Tetsuya Fukuoka, and Maki Fukami

Subjects

Male, Germline mosaicism, tuberous sclerosis complex, Biology, aberrant transcript, Tuberous Sclerosis Complex 1 Protein, Germline, Frameshift mutation, Heart Neoplasms, Exon, Tuberous sclerosis, INDEL Mutation, Cell Line, Tumor, cardiac rhabdomyoma, Genetics, medicine, Humans, RNA, Messenger, intragenic deletion, Genetics (clinical), Exome sequencing, germline mosaicism, Mosaicism, Intron, General Medicine, Rhabdomyoma, medicine.disease, Pedigree, TSC1, medicine.anatomical_structure, Child, Preschool, Female, RNA Splice Sites

Abstract

Tuberous sclerosis complex (TSC) is a rare autosomal dominant disorder characterized by non-cancerous tumors in multiple organs including the brain, kidney, lung, heart, and skin. We encountered a Japanese family consisting of two siblings (a four-year-old boy and a one-year-old girl) with multiple cardiac rhabdomyomas conveying a high risk of TSC and apparently unaffected sibling (a two-year-old girl) and parents. Whole exome sequencing and application of Integrative Genomic Viewer revealed an identical intragenic TSC1 deletion with the breakpoints on intron 15 and exon 19 in the affected siblings, but not in the apparently unaffected sibling and parents. Subsequently, PCR-based analyses were performed using primers flanking the deletion, showing that the deletion was also present in the father and that the deletion occurred between chr9:135,777,038 (bp) and chr9:135,780,540 (bp) in association with a one bp overlap. Furthermore, RT-PCR analyses were carried out using lymphoblastoid cell lines, revealing a major in-frame insertion/deletion transcript produced by aberrant splicing using a cryptic ″ag″ splice acceptor motif at intron 15 (r.1998_2438delinsTTCATTAGGTGG) and a minor frameshift transcript generated by aberrant splicing between exon 15 and exon 20 (r.1998_2502del, p.Lys666Asnfs*15) in the affected siblings. These findings imply that the intragenic deletion producing two aberrant transcripts was generated as a somatic pathogenic variant involving the germline in the father and was transmitted to the affected siblings.

Published

2020

158. Exome reports A de novo GNB2 variant associated with global developmental delay, intellectual disability, and dysmorphic features

Author

Tomoko Kawai, Hirotomo Saitsu, Mitsuko Nakashima, Takuya Hiraide, Kumiko Yanagi, Tokiko Fukuda, Tsutomu Ogata, and Kaori Yamoto

Subjects

0301 basic medicine, Muscle Hypotonia, Developmental Disabilities, global developmental delay, 030105 genetics & heredity, Biology, 03 medical and health sciences, GNB2, GTP-Binding Proteins, Intellectual Disability, Exome Sequencing, Genetics, medicine, Humans, Abnormalities, Multiple, Exome, Global developmental delay, whole-exome sequencing, Child, Genetics (clinical), Exome sequencing, Genetic Variation, General Medicine, Hypotonia, 030104 developmental biology, Face, GNB4, Female, Joints, medicine.symptom, GNB1, GNB3

Abstract

Heterotrimeric G proteins are composed of α, β, and γ subunits and are involved in integrating signals between receptors and effector proteins. The 5 human Gβ proteins (encoded by GNB1, GNB2, GNB3, GNB4, and GNB5) are highly similar. Variants in GNB1 were identified as a genetic cause of developmental delay. De novo variant in GNB2 has recently been reported as a cause of sinus node dysfunction and atrioventricular block but not as a cause of developmental delay. Trio-based whole-exome sequencing was performed on an individual with global developmental delay, muscle hypotonia, multiple congenital joint contractures and dysmorphism such as brachycephalus, thick eyebrows, thin upper lip, micrognathia, prominent chin, and bilateral tapered fingers. We identified a de novo GNB2 variant c.229G>A, p.(Gly77Arg). Notably, pathogenic substitutions of the homologous Gly77 residue including an identical variant (p.Gly77Arg, p.Gly77Val, p.Gly77Ser, p.Gly77Ala) of GNB1, a paralog of GNB2, was reported in individuals with global developmental delay and hypotonia. Clinical features of our case overlap with those of GNB1 variants. Our study suggests that a GNB2 variant may be associated with syndromic global developmental delay.

Published

2020

159. Temple syndrome in a patient with variably methylated CpGs at the primary MEG3/DLK1:IG-DMR and severely hypomethylated CpGs at the secondary MEG3:TSS-DMR

Author

Keiko Matsubara, Miyuki Ota, Atsuhiro Yanagisawa, Tsutomu Ogata, Masayo Kagami, Kazuhiko Nakabayashi, Maki Fukami, Akie Nakamura, Shuji Takada, and Kentaro Matsuoka

Subjects

0301 basic medicine, Temple syndrome, lcsh:QH426-470, Somatic cell, Bisulfite sequencing, Short Report, Secondary DMR, lcsh:Medicine, Nails, Malformed, Epigenesis, Genetic, 03 medical and health sciences, Genomic Imprinting, Multilocus imprinting disturbance, 0302 clinical medicine, Primary DMR, Placenta, Intellectual Disability, Genetics, GNAS complex locus, medicine, Humans, Imprinting (psychology), Molecular Biology, Genetics (clinical), MEG3, biology, lcsh:R, Calcium-Binding Proteins, Membrane Proteins, Methylation, DNA Methylation, Uniparental Disomy, Molecular biology, lcsh:Genetics, 030104 developmental biology, medicine.anatomical_structure, Thumb, 030220 oncology & carcinogenesis, Child, Preschool, DNA methylation, embryonic structures, biology.protein, Hallux, CpG Islands, Female, RNA, Long Noncoding, Developmental Biology

Abstract

Background The human chromosome 14q32.2 imprinted region harbors the primary MEG3/DLK1:IG-differentially methylated region (DMR) and secondary MEG3:TSS-DMR. The MEG3:TSS-DMR can remain unmethylated only in the presence of unmethylated MEG3/DLK1:IG-DMR in somatic tissues, but not in the placenta, because of a hierarchical regulation of the methylation pattern between the two DMRs. Methods We performed molecular studies in a 4-year-old Japanese girl with Temple syndrome (TS14). Results Pyrosequencing analysis showed extremely low methylation levels of five CpGs at the MEG3:TSS-DMR and grossly normal methylation levels of four CpGs at the MEG3/DLK1:IG-DMR in leukocytes. HumanMethylation450 BeadChip confirmed marked hypomethylation of the MEG3:TSS-DMR and revealed multilocus imprinting disturbance (MLID) including mild hypomethylation of the H19/IGF2:IG-DMR and mild hypermethylation of the GNAS A/B:TSS-DMR in leukocytes. Bisulfite sequencing showed markedly hypomethylated CpGs at the MEG3:TSS-DMR and irregularly and non-differentially methylated CpGs at the MEG3/DLK1:IG-DMR in leukocytes and apparently normal methylation patterns of the two DMRs in the placenta. Maternal uniparental disomy 14 and a deletion involving this imprinted region were excluded. Conclusions Such a methylation pattern of the MEG3/DLK1:IG-DMR has not been reported in patients with TS14. It may be possible that a certain degree of irregular hypomethylation at the MEG3/DLK1:IG-DMR has prevented methylation of the MEG3:TSS-DMR in somatic tissues and that a hypermethylation type MLID has occurred at the MEG3/DLK1:IG-DMR to yield the apparently normal methylation pattern in the placenta. Electronic supplementary material The online version of this article (10.1186/s13148-019-0640-2) contains supplementary material, which is available to authorized users.

Published

2018

160. 11-oxygenated C19 steroids as circulating androgens in women with polycystic ovary syndrome

Author

Minoru Irahara, Kazuki Saito, Takeshi Iwasa, Tomoko Yoshida, Maki Fukami, Tsutomu Ogata, Mami Miyado, Yoichi Matsubara, and Toshiya Matsuzaki

Subjects

0301 basic medicine, Adult, medicine.medical_specialty, medicine.drug_class, Endocrinology, Diabetes and Metabolism, 030209 endocrinology & metabolism, Overweight, Body Mass Index, 03 medical and health sciences, chemistry.chemical_compound, Young Adult, 0302 clinical medicine, Endocrinology, Tandem Mass Spectrometry, Internal medicine, medicine, Humans, Clinical significance, In patient, Obesity, business.industry, Androgen, medicine.disease, Polycystic ovary, 030104 developmental biology, Normal weight, chemistry, Androgens, 11-Ketotestosterone, Female, medicine.symptom, business, Chromatography, Liquid, Polycystic Ovary Syndrome

Abstract

11-oxygenated C19 steroids (11oxC19s) are newly specified human androgens. Although median serum levels of 11oxC19 were reported to be higher in patients with polycystic ovary syndrome (PCOS) than in unaffected women, inter-individual variations in androgen levels among PCOS patients have poorly been investigated. Here, we quantified four 11oxC19s, i.e., 11-ketotestosterone (11KT), 11β-hydroxytestosterone (11OHT), 11β-hydroxyandrostenedione (11OHΔ4A), and 11-ketoandrostenedione (11KΔ4A), in blood samples of 28 PCOS patients and 31 eumenorrheic women using liquid chromatography-tandem mass spectrometry. We referred to our previous data of classic androgens in these individuals. We found that 11OHT levels were higher in the PCOS group than in the eumenorrheic group. Moreover, although the median values of 11KT, 11KΔ4A, and 11OHΔ4A were comparable between the two groups, these steroids were markedly increased in some patients. Of the 28 patients, 8 had high levels of both 11oxC19s and classic androgens, whereas 4 had an increase only in 11oxC19 levels, and 12 had an increase only in classic androgen levels. Intragroup variations in androgen levels were relatively large in the PCOS group. Levels of 11OHT and 11KT were significantly higher in overweight/obese patients than in normal weight patients and correlated with body mass indexes. These results highlight the clinical significance of 11oxC19s as circulating androgens in PCOS patients and indicate that the accumulation of 11oxC19s and/or classic androgens is an essential feature of PCOS. The profiles of circulating androgens appear to vary among patients. In particular, overweight/obesity likely enhances the 11oxC19s accumulation in PCOS, although this notion awaits further validation.

Published

2018

161. Congenital limb deficiency in Japan: a cross-sectional nationwide survey on its epidemiology

Author

Shuji Hashimoto, Nobuhiko Haga, Kazuyuki Takamura, Sayaka Fujiwara, Hiroshi Mano, Tsutomu Ogata, Hiroshi Kitoh, and Shinichiro Takayama

Subjects

Male, Pediatrics, medicine.medical_specialty, lcsh:Diseases of the musculoskeletal system, Time Factors, Sports medicine, Cross-sectional study, Epidemiology, medicine.medical_treatment, Disease, 03 medical and health sciences, 0302 clinical medicine, Age Distribution, Rheumatology, Japan, medicine, Prevalence, Humans, Orthopedics and Sports Medicine, 030212 general & internal medicine, Upper Extremity Deformities, Congenital, Sex Distribution, Child, Congenital limb deficiency, Birth prevalence, Response rate (survey), Rehabilitation, business.industry, Infant, Newborn, Infant, Health Surveys, Confidence interval, body regions, Cross-Sectional Studies, Child, Preschool, Orthopedic surgery, Female, lcsh:RC925-935, business, Nationwide survey, 030217 neurology & neurosurgery, Research Article, Lower Extremity Deformities, Congenital

Abstract

Background Congenital limb deficiency is a rare and intractable disease, which impairs both function and appearance of the limbs. To establish adequate medical care, it is necessary to reveal the actual conditions and problems associated with this disease. However, there have been no extensive epidemiological surveys in Japan addressing this disease. This is the first nationwide epidemiological survey of congenital limb deficiency in this country. Methods With the cooperation of epidemiology experts, we performed a two-stage nationwide survey to estimate the number of patients with congenital limb deficiency and reveal basic patient features. We targeted orthopaedic surgery, paediatric, and plastic surgery departments. Hospitals were categorized according to the institution type and the number of hospital beds; hospitals were randomly selected from these categories. We selected 2283 departments from a total 7825 departments throughout Japan. In this study, we defined congenital limb deficiency as partial or total absence of the limbs, proximal to the proximal interphalangeal joint of the fingers/lesser toes or interphalangeal joint of the thumb/great toe. We distributed the first survey querying the number of initial patient visits from January 2014 to December 2015. Targets of the second survey were departments that reported one or more initial patient visits in the first survey. Results In the first survey, 1767 departments responded (response rate: 77.4%). Among them, 161 departments reported one or more initial patient visits. We conducted the second survey among these 161 departments, of which 96 departments responded (response rate: 59.6%). The estimated number of initial visits by patients with congenital limb deficiency was 417 (95% confidence interval: 339–495) per year in 2014 and 2015. The estimated prevalence of congenital limb deficiency in Japan was 4.15 (95% confidence interval: 3.37–4.93) per 10,000 live births. The sex ratio was 1.40. Upper limbs were more affected than lower limbs. Conclusions We revealed the estimated number of initial patient visits per year and birth prevalence of congenital limb deficiency in Japan. Our results will contribute to establishing the disease concept and grades of severity of congenital limb deficiency. Electronic supplementary material The online version of this article (10.1186/s12891-018-2195-3) contains supplementary material, which is available to authorized users.

Published

2018

162. Molecular and clinical analyses of two patients with UPD(16)mat detected by screening 94 patients with Silver-Russell syndrome phenotype of unknown aetiology

Author

Tsutomu Ogata, Tomoko Fuke, Junko Nishioka, Masayo Kagami, Kazuki Yamazawa, Takanobu Inoue, Hideaki Yagasaki, Satoshi Narumi, Maki Fukami, Keiko Matsubara, Akira Oka, Akie Nakamura, and Kazuhiko Nakabayashi

Subjects

0301 basic medicine, Adult, Male, Pathology, medicine.medical_specialty, Adolescent, 030105 genetics & heredity, Gene mutation, 03 medical and health sciences, Young Adult, maternal uniparental disomy of chromosome 16, Chromosome 16, parasitic diseases, Genetics, medicine, Humans, Genetic Predisposition to Disease, Child, Exome, Genetics (clinical), Genetic Association Studies, Genetic testing, medicine.diagnostic_test, business.industry, Silver–Russell syndrome, Infant, znf597, silver-russell syndrome, DNA Methylation, Uniparental Disomy, medicine.disease, Phenotype, 030104 developmental biology, Hypospadias, Child, Preschool, netchine-harbison clinical scoring system, Female, Epigenetics, business, Chromosomes, Human, Pair 16, SNP array, Transcription Factors

Abstract

BackgroundRecently, a patient with maternal uniparental disomy of chromosome 16 (UPD(16)mat) presenting with Silver-Russell syndrome (SRS) phenotype was reported. SRS is characterised by growth failure and dysmorphic features.ObjectiveTo clarify the prevalence of UPD(16)mat in aetiology-unknown patients with SRS phenotype and phenotypic differences between UPD(16)mat and SRS.MethodsWe studied 94 patients with SRS phenotype of unknown aetiology. Sixty-three satisfied the Netchine-Harbison clinical scoring system (NH-CSS) criteria, and 25 out of 63 patients showed both protruding forehead and relative macrocephaly (clinical SRS). The remaining 31 patients met only three NH-CSS criteria, but were clinically suspected as having SRS. To detect UPD(16)mat, we performed methylation analysis for the ZNF597:TSS-differentially methylated region (DMR) on chromosome 16 and subsequently performed microsatellite, SNP array and exome analyses in the patients with hypomethylated ZNF597:TSS-DMR.ResultsWe identified two patients (2.1%) with a mixture of maternal isodisomy and heterodisomy of chromosome 16 in 94 aetiology-unknown patients with SRS phenotype. Both patients exhibited preterm birth and prenatal and postnatal growth failure. The male patient had ventricular septal defect and hypospadias. Whole-exome sequencing detected no gene mutations related to their phenotypes.ConclusionWe suggest considering genetic testing for UPD(16)mat in SRS phenotypic patients without known aetiology.

Published

2018

163. Partial androgen insensitivity syndrome caused by a deep intronic mutation creating an alternative splice acceptor site of the AR gene

Author

Yasuko Fujisawa, Tsutomu Ogata, Shinichi Nakashima, Hiroyuki Ono, Reiko Horikawa, Kazuhiko Nakabayashi, Hirotomo Saitsu, Kumiko Yanagi, Maki Fukami, and Yumiko Ohkubo

Subjects

Male, 0301 basic medicine, Science, Nonsense-mediated decay, Article, 03 medical and health sciences, 0302 clinical medicine, medicine, Humans, Coding region, splice, RNA, Messenger, Gene, Family Health, Messenger RNA, 030219 obstetrics & reproductive medicine, Multidisciplinary, Whole Genome Sequencing, Chemistry, Gene Expression Profiling, Wild type, RNA, Androgen-Insensitivity Syndrome, medicine.disease, Molecular biology, Nonsense Mediated mRNA Decay, 030104 developmental biology, Receptors, Androgen, Mutation, Medicine, Androgen insensitivity syndrome, RNA Splice Sites

Abstract

Although partial androgen insensitivity syndrome (PAIS) is caused by attenuated responsiveness to androgens, androgen receptor gene (AR) mutations on the coding regions and their splice sites have been identified only in AR (NM_000044.4:c.2450−42 G > A). This variant created the splice acceptor motif that was accompanied by pyrimidine-rich sequence and two candidate branch sites. Consistent with this, reverse transcriptase (RT)-PCR experiments for cycloheximide-treated lymphoblastoid cell lines revealed a relatively large amount of aberrant mRNA produced by the newly created splice acceptor site and a relatively small amount of wildtype mRNA produced by the normal splice acceptor site. Furthermore, most of the aberrant mRNA was shown to undergo nonsense mediated decay (NMD) and, if a small amount of aberrant mRNA may have escaped NMD, such mRNA was predicted to generate a truncated AR protein missing some functional domains. These findings imply that the deep intronic mutation creating an alternative splice acceptor site resulted in the production of a relatively small amount of wildtype AR mRNA, leading to PAIS.

Published

2018

164. Spectrum of mutations and genotype–phenotype analysis in Noonan syndrome patients with RIT1 mutations

Author

Tsutomu Ogata, Sixto García-Miñaur, Nobuhiko Okamoto, Shion Hayashi, Atsushi Watanabe, Ohsuke Migita, Pablo Lapunzina, Masato Yokozawa, Hiroshi Suzumura, Hirofumi Ohashi, Fernando Santos-Simarro, Seiji Mizuno, Tetsuya Niihori, Yoko Aoki, Akihiko Nakahara, Yusuke Nakano, Shin Ichi Inoue, Ayumi Ohmori, Yoichi Matsubara, Tatsunori Hokosaki, Shigeo Kure, Hiroshi Kawame, Kenji Kurosawa, Hirofumi Sawada, Aya Mima, and Masako Yaoita

Subjects

Heart Defects, Congenital, Male, 0301 basic medicine, Pathology, medicine.medical_specialty, Hydrops Fetalis, Protein Tyrosine Phosphatase, Non-Receptor Type 11, RASopathy, Biology, medicine.disease_cause, Chylothorax, Short stature, Atrial septal defects, Proto-Oncogene Proteins p21(ras), 03 medical and health sciences, Genetics, medicine, Humans, Genetic Association Studies, Genetics (clinical), Mutation, Noonan Syndrome, Infant, Newborn, Hypertrophic cardiomyopathy, Infant, Exons, medicine.disease, Pleural Effusion, PTPN11, 030104 developmental biology, Gene Expression Regulation, Child, Preschool, ras Proteins, Noonan syndrome, Female, KRAS, medicine.symptom, Nuchal Translucency Measurement, SOS1 Protein

Abstract

RASopathies are autosomal dominant disorders caused by mutations in more than 10 known genes that regulate the RAS/MAPK pathway. Noonan syndrome (NS) is a RASopathy characterized by a distinctive facial appearance, musculoskeletal abnormalities, and congenital heart defects. We have recently identified mutations in RIT1 in patients with NS. To delineate the clinical manifestations in RIT1 mutation-positive patients, we further performed a RIT1 analysis in RASopathy patients and identified 7 RIT1 mutations, including two novel mutations, p.A77S and p.A77T, in 14 of 186 patients. Perinatal abnormalities, including nuchal translucency, fetal hydrops, pleural effusion, or chylothorax and congenital heart defects, are observed in all RIT1 mutation-positive patients. Luciferase assays in NIH 3T3 cells demonstrated that the newly identified RIT1 mutants, including p.A77S and p.A77T, and the previously identified p.F82V, p.T83P, p.Y89H, and p.M90I, enhanced Elk1 transactivation. Genotype-phenotype correlation analyses of previously reported NS patients harboring RIT1, PTPN11, SOS1, RAF1, and KRAS revealed that hypertrophic cardiomyopathy (56 %) was more frequent in patients harboring a RIT1 mutation than in patients harboring PTPN11 (9 %) and SOS1 mutations (10 %). The rates of hypertrophic cardiomyopathy were similar between patients harboring RIT1 mutations and patients harboring RAF1 mutations (75 %). Short stature (52 %) was less prevalent in patients harboring RIT1 mutations than in patients harboring PTPN11 (71 %) and RAF1 (83 %) mutations. These results delineate the clinical manifestations of RIT1 mutation-positive NS patients: high frequencies of hypertrophic cardiomyopathy, atrial septal defects, and pulmonary stenosis; and lower frequencies of ptosis and short stature.

Published

2015

165. Risk assessment of medically assisted reproduction and advanced maternal ages in the development of Prader-Willi syndrome due to UPD(15)mat

Author

Nobuyuki Murakami, Keiko Matsubara, Tsutomu Ogata, Masayo Kagami, Toshiro Nagai, and Maki Fukami

Subjects

0301 basic medicine, congenital, hereditary, and neonatal diseases and abnormalities, medicine.medical_specialty, media_common.quotation_subject, medicine.medical_treatment, Population, Biology, Logistic regression, 03 medical and health sciences, 0302 clinical medicine, Genetics, medicine, Advanced maternal age, Young adult, education, Genetics (clinical), media_common, Gynecology, education.field_of_study, 030219 obstetrics & reproductive medicine, Assisted reproductive technology, nutritional and metabolic diseases, medicine.disease, Uniparental disomy, nervous system diseases, 030104 developmental biology, Reproduction, Risk assessment

Abstract

Recent studies have suggested that disomic oocyte-mediated uniparental disomy 15 (UPD(15)mat) is increased in patients with Prader-Willi syndrome (PWS) born after medically assisted reproduction (MAR). However, it remains unknown whether the increase is primarily due to MAR procedure itself or advanced maternal childbearing ages as a predisposing factor for the disomic oocyte production. To examine this matter, we studied 122 naturally conceived PWS patients (PWS-NC group) and 13 MAR-conceived patients (PWS-MAR group). The relative frequency of disomic oocyte-mediated UPD(15)mat was significantly higher in PWS-MAR group than in PWS-NC group (7/13 vs 20/122, p = 0.0045), and the maternal childbearing ages were significantly higher in PWS-MAR group than in PWS-NC group [median (range), 38 (26-45) vs 30 (19-42), p = 0.0015]. However, the logistic regression analysis revealed no significant association between the occurrence of disomic oocyte-mediated UPD(15)mat and MAR, after adjusting for childbearing age (p = 0.25). Consistent with this, while the frequency of assisted reproductive technology (ART)-conceived livebirths was higher in the PWS patients than in the Japanese general population (6.4% vs 1.1%, p = 0.00018), the distribution of childbearing ages was significantly skewed to the increased ages in the PWS patients (p < 2.2 × 10(-16) ). These results argue against a positive association of MAR procedure itself with the development of UPD(15)mat.

Published

2015

166. Kagami–Ogata syndrome: a clinically recognizable upd(14)pat and related disorder affecting the chromosome 14q32.2 imprinted region

Author

Tsutomu Ogata and Masayo Kagami

Subjects

0301 basic medicine, medicine.medical_specialty, Chromosome Disorders, Review, Biology, Genomic Imprinting, 03 medical and health sciences, Genetics, medicine, Humans, Abnormalities, Multiple, Epigenetics, Imprinting (psychology), Genetics (clinical), Chromosomes, Human, Pair 14, MEG3, Cytogenetics, Syndrome, Uniparental Disomy, medicine.disease, Uniparental disomy, Phenotype, 030104 developmental biology, Statistical genetics, embryonic structures, Medical genetics, Chromosome Deletion, Genomic imprinting

Abstract

Human chromosome 14q32.2 carries paternally expressed genes including DLK1 and RTL1, and maternally expressed genes including MEG3 and RTL1as, along with the germline-derived DLK1-MEG3 intergenic differentially methylated region (IG-DMR) and the postfertilization-derived MEG3-DMR. Consistent with this, paternal uniparental disomy 14 (upd(14)pat), and epimutations (hypermethylations) and microdeletions affecting the IG-DMR and/or the MEG3-DMR of maternal origin, result in a unique phenotype associated with characteristic face, a small bell-shaped thorax with coat-hanger appearance of the ribs, abdominal wall defects, placentomegaly and polyhydramnios. Recently, the name ‘Kagami–Ogata syndrome' (KOS) has been approved for this clinically recognizable disorder. Here, we review the current knowledge about KOS. Important findings include the following: (1) the facial ‘gestalt' and the increased coat-hanger angle constitute pathognomonic features from infancy through childhood/puberty; (2) the unmethylated IG-DMR and MEG3-DMR of maternal origin function as the imprinting control centers in the placenta and body respectively, with a hierarchical interaction regulated by the IG-DMR for the methylation pattern of the MEG3-DMR in the body; (3) RTL1 expression level becomes ~2.5 times increased in the absence of functional RTL1as-encoded microRNAs that act as a trans-acting repressor for RTL1; (4) excessive RTL1 expression and absent MEG expression constitute the primary underlying factor for the phenotypic development; and (5) upd(14)pat accounts for approximately two-thirds of KOS patients, and epimutations and microdeletions are identified with a similar frequency. Furthermore, we refer to diagnostic and therapeutic implications.

Published

2015

167. Testicular dysgenesis/regression without campomelic dysplasia in patients carrying missense mutations and upstream deletion of <scp>SOX</scp> 9

Author

Yoichi Matsubara, Yuko Katoh-Fukui, Maki Igarashi, Ken Ichirou Morohashi, Erina Suzuki, Kazuhiko Nakabayashi, Keisuke Nagasaki, Tsutomu Ogata, Mami Miyado, Toshiro Nagai, Kenichiro Hata, Shuji Takada, Takashi Baba, Keiko Hayashi, Takayoshi Tsuchiya, Arisa Igarashi, Reiko Horikawa, and Maki Fukami

Subjects

Genetics, endocrine system, Mutation, Original Articles, SOX9, testis, Sex reversal, Biology, medicine.disease, medicine.disease_cause, Campomelic dysplasia, Dysplasia, Cancer research, medicine, Missense mutation, Original Article, deletion, enhancer, mutation, Haploinsufficiency, Molecular Biology, Exome, Genetics (clinical)

Abstract

SOX9 haploinsufficiency underlies campomelic dysplasia (CD) with or without testicular dysgenesis. Current understanding of the phenotypic variability and mutation spectrum of SOX9 abnormalities remains fragmentary. Here, we report three patients with hitherto unreported SOX9 abnormalities. These patients were identified through molecular analysis of 33 patients with 46,XY disorders of sex development (DSD). Patients 1–3 manifested testicular dysgenesis or regression without CD. Patients 1 and 2 carried probable damaging mutations p.Arg394Gly and p.Arg437Cys, respectively, in the SOX9 C‐terminal domain but not in other known 46,XY DSD causative genes. These substitutions were absent from ~120,000 alleles in the exome database. These mutations retained normal transactivating activity for the Col2a1 enhancer, but showed impaired activity for the Amh promoter. Patient 3 harbored a maternally inherited ~491 kb SOX9 upstream deletion that encompassed the known 32.5 kb XY sex reversal region. Breakpoints of the deletion resided within nonrepeat sequences and were accompanied by a short‐nucleotide insertion. The results imply that testicular dysgenesis and regression without skeletal dysplasia may be rare manifestations of SOX9 abnormalities. Furthermore, our data broaden pathogenic SOX9 abnormalities to include C‐terminal missense substitutions which lead to target‐gene‐specific protein dysfunction, and enhancer‐containing upstream microdeletions mediated by nonhomologous end‐joining.

Published

2015

168. Rare pseudoautosomal copy-number variations involving SHOX and/or its flanking regions in individuals with and without short stature

Author

Maki, Fukami, Yasuhiro, Naiki, Koji, Muroya, Takashi, Hamajima, Shun, Soneda, Reiko, Horikawa, Tomoko, Jinno, Momori, Katsumi, Akie, Nakamura, Yumi, Asakura, Masanori, Adachi, Tsutomu, Ogata, Susumu, Kanzaki, and M, Fukami

Subjects

Male, DNA Copy Number Variations, 5' Flanking Region, Pseudoautosomal region, Alu element, Dwarfism, Biology, Osteochondrodysplasias, Young Adult, Exon, Gene Frequency, Short Stature Homeobox Protein, Gene Duplication, Gene duplication, Genetics, Humans, 3' Flanking Region, Copy-number variation, Child, Growth Disorders, Genetics (clinical), Sequence Deletion, Homeodomain Proteins, Breakpoint, Infant, Middle Aged, Case-Control Studies, Child, Preschool, Female, Human genome

Abstract

Pseudoautosomal region 1 (PAR1) contains SHOX, in addition to seven highly conserved non-coding DNA elements (CNEs) with cis-regulatory activity. Microdeletions involving SHOX exons 1-6a and/or the CNEs result in idiopathic short stature (ISS) and Leri-Weill dyschondrosteosis (LWD). Here, we report six rare copy-number variations (CNVs) in PAR1 identified through copy-number analyzes of 245 ISS/LWD patients and 15 unaffected individuals. The six CNVs consisted of three microduplications encompassing SHOX and some of the CNEs, two microduplications in the SHOX 3'-region affecting one or four of the downstream CNEs, and a microdeletion involving SHOX exon 6b and its neighboring CNE. The amplified DNA fragments of two SHOX-containing duplications were detected at chromosomal regions adjacent to the original positions. The breakpoints of a SHOX-containing duplication resided within Alu repeats. A microduplication encompassing four downstream CNEs was identified in an unaffected father-daughter pair, whereas the other five CNVs were detected in ISS patients. These results suggest that microduplications involving SHOX cause ISS by disrupting the cis-regulatory machinery of this gene and that at least some of microduplications in PAR1 arise from Alu-mediated non-allelic homologous recombination. The pathogenicity of other rare PAR1-linked CNVs, such as CNE-containing microduplications and exon 6b-flanking microdeletions, merits further investigation.

Published

2015

169. Comprehensive clinical studies in 34 patients with molecularly defined UPD(14)pat and related conditions (Kagami–Ogata syndrome)

Author

Kenji Kurosawa, Kentaro Matsuoka, Tsutomu Ogata, Masayo Kagami, Osamu Miyazaki, and Fumitoshi Ishino

Subjects

Male, Thorax, Hepatoblastoma, Pediatrics, medicine.medical_specialty, Polyhydramnios, Beckwith-Wiedemann Syndrome, Adolescent, Developmental Disabilities, Birth weight, Gestational Age, Kaplan-Meier Estimate, Biology, Article, Craniofacial Abnormalities, Genomic Imprinting, Pregnancy, Pathognomonic, Intellectual Disability, Intellectual disability, Genetics, medicine, Humans, Abnormalities, Multiple, Child, Genetics (clinical), Chromosomes, Human, Pair 14, Philtrum, Infant, Newborn, Infant, Gestational age, Anatomy, Uniparental Disomy, medicine.disease, medicine.anatomical_structure, Child, Preschool, Female

Abstract

Paternal uniparental disomy 14 (UPD(14)pat) and epimutations and microdeletions affecting the maternally derived 14q32.2 imprinted region lead to a unique constellation of clinical features such as facial abnormalities, small bell-shaped thorax with a coat-hanger appearance of the ribs, abdominal wall defects, placentomegaly, and polyhydramnios. In this study, we performed comprehensive clinical studies in patients with UPD(14)pat (n=23), epimutations (n=5), and microdeletions (n=6), and revealed several notable findings. First, a unique facial appearance with full cheeks and a protruding philtrum and distinctive chest roentgenograms with increased coat-hanger angles to the ribs constituted the pathognomonic features from infancy through childhood. Second, birth size was well preserved, with a median birth length of ±0 SD (range, −1.7 to +3.0 SD) and a median birth weight of +2.3 SD (range, +0.1 to +8.8 SD). Third, developmental delay and/or intellectual disability was invariably present, with a median developmental/intellectual quotient of 55 (range, 29–70). Fourth, hepatoblastoma was identified in three infantile patients (8.8%), and histological examination in two patients showed a poorly differentiated embryonal hepatoblastoma with focal macrotrabecular lesions and well-differentiated hepatoblastoma, respectively. These findings suggest the necessity of an adequate support for developmental delay and periodical screening for hepatoblastoma in the affected patients, and some phenotypic overlap between UPD(14)pat and related conditions and Beckwith–Wiedemann syndrome. On the basis of our previous and present studies that have made a significant contribution to the clarification of underlying (epi)genetic factors and the definition of clinical findings, we propose the name ‘Kagami–Ogata syndrome' for UPD(14)pat and related conditions.

Published

2015

170. A 45,X/46,XY DSD (Disorder of Sexual Development) case with an extremely uneven distribution of 46,XY cells between lymphocytes and gonads

Author

Michiyo Okada, Takumi Akashi, Risa Nomura, Kenichi Kashimada, Michiko Kajiwara, Masaki Sekine, Tsutomu Ogata, Kentaro Miyai, Makoto Ono, Iichiro Onishi, Shuki Mizutani, and Mana Sato

Subjects

Genetics, education.field_of_study, endocrine system, Endocrinology, Diabetes and Metabolism, Population, XY karyotype, Fish analysis, Biology, Peripheral blood, FISH (fluorescence in situ hybridization), Andrology, Endocrinology, mosaicism, chimerism, SRY, Pediatrics, Perinatology and Child Health, Original Article, Development of the gonads, education, 45,X/46,XY DSD (disorder of sexual development)

Abstract

In 45,X/46,XY DSDs, the proportion of the two cell lineages is uneven in different organs and tissues, and 45,X and 46,XY cells can be found throughout the body. The gonadal development of 45,X/46,XY patients depends on the population of 46,XY cells in the gonads and the clinical features are variable. We had a 45,X/46,XY DSD patient whose 46,XY population in peripheral blood was extremely low, less than 0.2%, and was not detected by FISH analysis. However, the patient showed bilateral testicular development and more than 50% of the cells in the gonads had the 46,XY karyotype. This case suggests that a drastically imbalanced distribution could occur in 45,X/46,XY DSD cases.

Published

2015

171. Detecting copy-number variations in whole-exome sequencing data using the eXome Hidden Markov Model: an ‘exome-first’ approach

Author

Ichiro Kuki, Yoshio Makita, Ryoko Fukai, Yoshinori Tsurusaki, Atsushi Araki, Tsutomu Ogata, Mitsuko Nakashima, Megumi Nukui, Satoko Miyatake, Eriko Koshimizu, Eri Imagawa, Noriko Miyake, Naomichi Matsumoto, Hirotomo Saitsu, Chihiro Ohba, and Atsushi Fujita

Subjects

Male, medicine.medical_specialty, DNA Copy Number Variations, Methyl-CpG-Binding Protein 2, MECP2 duplication syndrome, Biology, Sensitivity and Specificity, Gigantism, Chromosome Breakpoints, Intellectual Disability, Chromosome Duplication, Genetics, medicine, Humans, Exome, Copy-number variation, Genetics (clinical), Exome sequencing, Oligonucleotide Array Sequence Analysis, Sequence Deletion, Brain Diseases, Models, Genetic, Sotos syndrome, Intracellular Signaling Peptides and Proteins, Computational Biology, High-Throughput Nucleotide Sequencing, Nuclear Proteins, Histone-Lysine N-Methyltransferase, medicine.disease, Markov Chains, Statistical genetics, Overgrowth syndrome, Histone Methyltransferases, Medical genetics, Female, Atrophy, Algorithms

Abstract

Whole-exome sequencing (WES) is becoming a standard tool for detecting nucleotide changes, and determining whether WES data can be used for the detection of copy-number variations (CNVs) is of interest. To date, several algorithms have been developed for such analyses, although verification is needed to establish if they fit well for the appropriate purpose, depending on the characteristics of each algorithm. Here, we performed WES CNV analysis using the eXome Hidden Markov Model (XHMM). We validated its performance using 27 rare CNVs previously identified by microarray as positive controls, finding that the detection rate was 59%, or higher (89%) with three or more targets. XHMM can be effectively used, especially for the detection of >200 kb CNVs. XHMM may be useful for deletion breakpoint detection. Next, we applied XHMM to genetically unsolved patients, demonstrating successful identification of pathogenic CNVs: 1.5–1.9-Mb deletions involving NSD1 in patients with unknown overgrowth syndrome leading to the diagnosis of Sotos syndrome, and 6.4-Mb duplication involving MECP2 in affected brothers with late-onset spasm and progressive cerebral/cerebellar atrophy confirming the clinical suspect of MECP2 duplication syndrome. The possibility of an ‘exome-first’ approach for clinical genetic investigation may be considered to save the cost of multiple investigations.

Published

2015

172. Human Chorionic Gonadotropin Stimulation Test in Prepubertal Children with Micropenis Can Accurately Predict Leydig Cell Function in Pubertal or Postpubertal Adolescents

Author

Satoshi Narumi, Nobutake Matsuo, Makoto Anzo, Shinya Tamai, Naoaki Hori, Tsutomu Kamimaki, Tomohiro Ishii, Tsutomu Ogata, Mikako Inokuchi, Hironori Shibata, Seiji Sato, Naoko Amano, Goro Sasaki, and Tomonobu Hasegawa

Subjects

Male, endocrine system, medicine.medical_specialty, Adolescent, Hormone Replacement Therapy, Endocrinology, Diabetes and Metabolism, Gonadotropin-releasing hormone, Human chorionic gonadotropin, Gonadotropin-Releasing Hormone, Follicle-stimulating hormone, Endocrinology, Asian People, Prepuberty, Internal medicine, Hormone replacement therapy (male-to-female), Humans, Medicine, Testosterone, Child, Retrospective Studies, Leydig cell, urogenital system, business.industry, Puberty, Infant, Leydig Cells, Micropenis, Placental Lactogen, medicine.disease, Stimulation, Chemical, medicine.anatomical_structure, Child, Preschool, Pediatrics, Perinatology and Child Health, Follicle Stimulating Hormone, Genital Diseases, Male, business, hormones, hormone substitutes, and hormone antagonists, Penis

Abstract

Background/Aim: To evaluate the accuracy of the human chorionic gonadotropin (hCG) stimulation test in children with micropenis in predicting later Leydig cell function. Methods: We conducted a retrospective investigation of testosterone response to a 3-day hCG test (3,000 IU/m2/day) in prepuberty to indicate the need for hormone replacement therapy (HRT) in adolescence. Results: Fifty Japanese boys (range, 0.8-15.4 years of age; median, 8.9) with micropenis were enrolled. Thirty-four spontaneously developed puberty and preserved the ability of testosterone production (group 1), while 16 did not develop any pubertal signs without HRT (group 2). Serum testosterone levels after the hCG test (post-hCG T) in group 2 (range, Conclusions: The hCG test in prepubertal children with micropenis can be useful for predicting Leydig cell function in pubertal or postpubertal adolescents. The post-hCG T cut-off level of 1.1 ng/ml is recommended to screen for those who will likely require HRT for pubertal development.

Published

2015

173. SOX3 Overdosage Permits Normal Sex Development in Females with Random X Inactivation

Author

Momori Katsumi, Yoko Izumi, Maki Fukami, Hitoshi Mikami, Maki Igarashi, Tsutomu Ogata, and Mami Miyado

Subjects

Male, Embryology, Gonad, Endocrinology, Diabetes and Metabolism, Gene Dosage, Biology, Gene dosage, Genome, X-inactivation, chemistry.chemical_compound, X Chromosome Inactivation, Gene duplication, medicine, Humans, Disorders of sex development, Gene Rearrangement, Genetics, Genome, Human, SOXB1 Transcription Factors, Sexual Development, medicine.disease, Phenotype, Molecular biology, medicine.anatomical_structure, chemistry, Child, Preschool, Female, DNA, Developmental Biology

Abstract

Submicroscopic duplications involving SOX3 and/or its flanking regions have been identified in 46,XX individuals both with and without disorders of sex development, raising the question whether SOX3 overdosage is sufficient to induce testicular development in genetically female individuals. Here, we report a mother-daughter pair with female phenotypes and random X inactivation. The individuals carry complex X chromosomal rearrangements leading to a copy number gain of genomic regions involving SOX3 and its upstream region. The amplified DNA fragments were detected at Xq27. These results provide evidence that SOX3 overdosage permits normal sex development in 46,XX individuals with random X inactivation.

Published

2015

174. Growth hormone deficiency in monozygotic twins with autosomal dominant pseudohypoparathyroidism type Ib

Author

Masayo Kagami, Keiko Matsubara, Shinichiro Sano, Tsutomu Ogata, Maki Fukami, and Hiromi Iwata

Subjects

musculoskeletal diseases, medicine.medical_specialty, Endocrinology, Diabetes and Metabolism, Mothers, Dwarfism, Syntaxin 16, Biology, Short stature, Growth hormone deficiency, Exon, Endocrinology, Japan, Internal medicine, Diseases in Twins, medicine, GNAS complex locus, Humans, Dwarfism, Pituitary, Pseudohypoparathyroidism, Human Growth Hormone, Twins, Monozygotic, DNA Methylation, medicine.disease, Differentially methylated regions, Child, Preschool, biology.protein, Female, STX16, Chromosome Deletion, medicine.symptom

Abstract

Pseudohypoparathyroidism (PHP) is associated with compromised signal transductions via PTH receptor (PTH-R) and other G-protein-coupled receptors including GHRH-R. To date, while GH deficiency (GHD) has been reported in multiple patients with PHP-Ia caused by mutations on the maternally expressed GNAS coding regions and in two patients with sporadic form of PHP-Ib accompanied by broad methylation defects of maternally derived GNAS differentially methylated regions (DMRs), it has not been identified in a patient with an autosomal dominant form of PHP-Ib (AD-PHP-Ib) accompanied by an STX16 microdeletion and an isolated loss of methylation (LOM) at exon A/B-DMR. We studied 5 4/12-year-old monozygotic twins with short stature (both -3.4 SD) and GHD (peak GH values

Published

2015

175. Loss of imprinting of the human-specific imprinted gene ZNF597 causes prenatal growth retardation and dysmorphic features: implications for phenotypic overlap with Silver-Russell syndrome.

Author

Kazuki Yamazawa, Takanobu Inoue, Yoshihiro Sakemi, Toshinori Nakashima, Hironori Yamashita, Kaduki Khono, Hideki Fujita, Keisuke Enomoto, Kazuhiko Nakabayashi, Kenichiro Hata, Moeko Nakashima, Tatsuo Matsunaga, Akie Nakamura, Keiko Matsubara, Tsutomu Ogata, and Masayo Kagami

Abstract

Background ZNF597, encoding a zinc-finger protein, is the human-specific maternally expressed imprinted gene located on 16p13.3. The parent-of-origin expression of ZNF597 is regulated by the ZNF597:TSS-DMR, of which only the paternal allele acquires methylation during postimplantation period. Overexpression of ZNF597 may contribute to some of the phenotypes associated with maternal uniparental disomy of chromosome 16 (UPD(16)mat), and some patients with UPD(16)mat presenting with Silver-Russell syndrome (SRS) phenotype have recently been reported. Methods A 6-year-old boy presented with prenatal growth restriction, macrocephaly at birth, forehead protrusion in infancy and clinodactyly of the fifth finger. Methylation, expression, microsatellite marker, single nucleotide polymorphism array and trio whole-exome sequencing analyses were conducted. Results Isolated hypomethylation of the ZNF597:TSS-DMR and subsequent loss of imprinting and overexpression of ZNF597 were confirmed in the patient. Epigenetic alterations, such as UPD including UPD(16) mat and other methylation defects, were excluded. Pathogenic sequence or copy number variants affecting his phenotypes were not identified, indicating that primary epimutation occurred postzygotically. Conclusion We report the first case of isolated ZNF597 imprinting defect, showing phenotypic overlap with SRS despite not satisfying the clinical SRS criteria. A novel imprinting disorder entity involving the ZNF597 imprinted domain can be speculated. [ABSTRACT FROM AUTHOR]

Published

2021

176. Long-term Effect of Aromatase Inhibition in Aromatase Excess Syndrome.

Author

Gerhard Binder, Akie Nakamura, Roland Schweizer, Tsutomu Ogata, Maki Fukami, Keisuke Nagasaki, Binder, Gerhard, Nakamura, Akie, Schweizer, Roland, Ogata, Tsutomu, Fukami, Maki, and Nagasaki, Keisuke

Subjects

PRECOCIOUS puberty, AROMATASE, MAGNETIC resonance imaging, OLDER people, MEDICAL ethics, MEDICAL sciences, LUTEINIZING hormone releasing hormone, STATURE, CHILD development, TIME, RETROSPECTIVE studies, INFERTILITY, AROMATASE inhibitors, INBORN errors of metabolism, GYNECOMASTIA, PHARMACODYNAMICS

Abstract

Context: Aromatase excess syndrome (AEXS) is a very rare disorder characterized by prepubertal gynecomastia, bone age acceleration, and early growth arrest. Heterozygote submicroscopic rearrangements within the promotor of CYP19A1 result in overexpression of aromatase and enhanced aromatization of androgens.Objective: The objective was to study long-term treatment effects of an aromatase inhibitor.Methods: Data from 7 boys with AEXS were retrospectively collected. Genetic analysis revealed upstream of CYP19A1 a 165 901 bp deletion in 4 German cousins, a 198 662 bp deletion in 2 Japanese brothers, and a 387 622 bp tandem duplication in a Japanese boy.Results: All boys developed prepubertal gynecomastia, at median 9.0 years of age (range: 7.0-11.0). Height was +1.20 standard deviation score (SDS) (-0.24 to +1.98); predicted adult height was -1.29 SDS (-3.29 to +1.09). Four boys were treated with 1.0 mg of anastrozole daily, while 3 reached adult height untreated. Treatment with anastrozole was stopped after 5.6 years (4.0-6.8). Three treated boys exceeded their prognosis by 2.4, 6.9, and 8.1 cm, while 1 untreated boy fell below the prognosis by 8.6 cm. One treated with a low dose and 2 untreated reached their prognosis. Adult heights were -0.91 SDS with anastrozole (-2.86 to -0.29) and -0.15 SDS without (-2.31 to -0.03). Distance to target height was -0.22 SDS with anastrozole (-1.72 to +0.52) and +0.54 SDS without (+0.23 to +1.30).Conclusion: Spontaneous growth in AEXS varied, even in the same family. Our data suggest that early started, long-term inhibition by anastrozole promotes adult height in boys with AEXS. [ABSTRACT FROM AUTHOR]

Published

2021

177. Role of Imprinting Disorders in Short Children Born SGA and Silver-Russell Syndrome Spectrum.

Author

Tomoko Fuke, Akie Nakamura, Takanobu Inoue, Sayaka Kawashima, Kaori Isono Hara, Keiko Matsubara, Shinichiro Sano, Kazuki Yamazawa, Maki Fukami, Tsutomu Ogata, Masayo Kagami, Fuke, Tomoko, Nakamura, Akie, Inoue, Takanobu, Kawashima, Sayaka, Hara, Kaori Isono, Matsubara, Keiko, Sano, Shinichiro, Yamazawa, Kazuki, and Fukami, Maki

Subjects

PITUITARY dwarfism, CHROMOSOME duplication, FETAL growth retardation, DNA copy number variations, PATIENT compliance, COMPARATIVE genomic hybridization, RESEARCH, SEQUENCE analysis, CRANIOFACIAL abnormalities, RESEARCH methodology, SILVER-Russell syndrome, CASE-control method, GENETIC disorders, MEDICAL cooperation, EVALUATION research, HUMAN growth hormone, MULTIPLE human abnormalities, COMPARATIVE studies, GENES, CYTOGENETICS, SMALL for gestational age, DWARFISM, PHENOTYPES, DISEASE complications

Abstract

Background: (Epi)genetic disorders associated with small-for-gestational-age with short stature (SGA-SS) include imprinting disorders (IDs). Silver-Russell syndrome (SRS) is a representative ID in SGA-SS and has heterogenous (epi)genetic causes.Subjects and Methods: To clarify the contribution of IDs to SGA-SS and the molecular and phenotypic spectrum of SRS, we recruited 269 patients with SGA-SS, consisting of 103 and 166 patients referred to us for genetic testing for SGA-SS and SRS, respectively. After excluding 20 patients with structural abnormalities detected by comparative genomic hybridization analysis using catalog array, 249 patients were classified into 3 subgroups based on the Netchine-Harbison clinical scoring system (NH-CSS), SRS diagnostic criteria. We screened various IDs by methylation analysis for differentially methylated regions (DMRs) related to known IDs. We also performed clinical analysis.Results: These 249 patients with SGA-SS were classified into the "SRS-compatible group" (n = 148), the "non-SRS with normocephaly or relative macrocephaly at birth group" (non-SRS group) (n = 94), or the "non-SRS with relative microcephaly at birth group" (non-SRS with microcephaly group) (n = 7). The 44.6% of patients in the "SRS-compatible group," 21.3% of patients in the "non-SRS group," and 14.3% in the "non-SRS with microcephaly group" had various IDs. Loss of methylation of the H19/IGF2:intergenic-DMR and uniparental disomy chromosome 7, being major genetic causes of SRS, was detected in 30.4% of patients in the "SRS-compatible group" and in 13.8% of patients in the "non-SRS group."Conclusion: We clarified the contribution of IDs as (epi)genetic causes of SGA-SS and the molecular and phenotypic spectrum of SRS. Various IDs constitute underlying factors for SGA-SS, including SRS. [ABSTRACT FROM AUTHOR]

Published

2021

178. Insulin resistant diabetes mellitus in SHORT syndrome: case report and literature review.

Author

Yohei Masunaga, Yasuko Fujisawa, Mayumi Muramatsu, Hiroyuki Ono, Takanobu Inoue, Maki Fukami, Masayo Kagami, Hirotomo Saitsu, and Tsutomu Ogata

Published

2021

179. STX2 is a causative gene for nonobstructive azoospermia

Author

Hideo Nakai, Maki Fukami, Hiromichi Ishikawa, Yoshihiko Ueda, Tsutomu Ogata, Mami Miyado, Yoshitomo Kobori, Kazuki Saito, Shigeru Nakamura, Yoko Tanaka, Atsumi Yoshida, Akie Nakamura, Momori Katsumi, and Hiroshi Okada

Subjects

0301 basic medicine, Infertility, Adult, Male, Loss of Heterozygosity, Syntaxin 1, Biology, urologic and male genital diseases, Frameshift mutation, Andrology, 03 medical and health sciences, Mice, fluids and secretions, 0302 clinical medicine, Multinucleate, STX2, hemic and lymphatic diseases, Complementary DNA, Testis, Genetics, medicine, Animals, Humans, Spermatogenesis, Genetics (clinical), Azoospermia, 030219 obstetrics & reproductive medicine, Wild type, bacterial infections and mycoses, medicine.disease, 030104 developmental biology, Mutation, Mutation testing, bacteria

Abstract

STX2 encodes a sulfoglycolipid transporter. Although Stx2 nullizygosity is known to cause spermatogenic failure in mice, STX2 mutations have not been identified in humans. Here, we performed STX2 mutation analysis for 131 Japanese men clinically diagnosed with nonobstructive azoospermia. As a result, we identified a homozygous frameshift mutation [c.8_12delACCGG, p.(Asp3Alafs*8)] in one patient. The mutation-positive patient exhibited loss-of-heterozygosity for 58.4 Mb genomic regions involving STX2, suggesting possible parental consanguinity. The patient showed azoospermia, relatively small testes, and a mildly elevated follicle stimulating hormone level, but no additional clinical features. Testicular histology of the patient showed universal maturation arrest and multinucleated spermatocytes, which have also been observed in mice lacking Stx2. PCR-based cDNA screening revealed wildtype STX2 expression in various tissues including the testis. Our results indicate that STX2 nullizygosity results in nonsyndromic maturation arrest with multinucleated spermatocytes, and accounts for a small fraction of cases with nonobstructive azoospermia.

Published

2017

180. Protein-altering variants of PTPN2 in childhood-onset Type 1A diabetes

Author

T. Kikuchi, Shin Amemiya, Adolescent Diabetes, Tsutomu Ogata, Kohji Okamura, Ikuma Musha, Kazuhiko Nakabayashi, Misako Okuno, Tomoyuki Kawamura, Yukihide Momozawa, Tatsuhiko Urakami, Nobuyuki Kikuchi, Tadayuki Ayabe, K. Shiga, Michiaki Kubo, Maki Fukami, Akira Ohtake, Akie Nakamura, Ichiro Yokota, Junichi Suzuki, and Shigetaka Sugihara

Subjects

0301 basic medicine, Male, Adolescent, Endocrinology, Diabetes and Metabolism, Population, Mutation, Missense, Single-nucleotide polymorphism, Human leukocyte antigen, Polymorphism, Single Nucleotide, Frameshift mutation, 03 medical and health sciences, Open Reading Frames, Endocrinology, HLA Antigens, Diabetes mellitus, Internal Medicine, medicine, Missense mutation, Humans, Genetic Predisposition to Disease, RNA, Messenger, Allele, education, Child, Frameshift Mutation, Exome, Genetics, education.field_of_study, Protein Tyrosine Phosphatase, Non-Receptor Type 2, business.industry, Infant, medicine.disease, 030104 developmental biology, Diabetes Mellitus, Type 1, Child, Preschool, Female, business

Abstract

AIM To examine the contribution of PTPN2 coding variants to the risk of childhood-onset Type 1A diabetes. METHODS PTPN2 mutation analysis was carried out for 169 unrelated Japanese people with childhood-onset Type 1A diabetes. We searched for coding variants that were absent or extremely rare in the general population and were scored as damaging by multiple in silico programs. We performed mRNA analysis and three-dimensional structural prediction of the detected variants, when possible. We also examined possible physical links between these variants and previously reported risk SNPs as well as clinical information from variant-positive children. RESULTS One frameshift variant (p.Q286Yfs*24) and two probably damaging missense substitutions (p.C232W and p.R350Q) were identified in one child each. Of these, p.Q286Yfs*24 and p.C232W were hitherto unreported, while p.R350Q accounted for 2/121,122 alleles of the exome datasets. The p.Q286Yfs*24 variant did not encode stable mRNA, and p.C232W appeared to affect the structure of the tyrosine-protein phosphatase domain. The three variants were physically unrelated to known risk SNPs. The variant-positive children manifested Type 1A diabetes without additional clinical features and invariably carried risk human leukocyte antigen alleles. CONCLUSIONS The results provide the first indication that PTPN2 variants contribute to the risk of Type 1A diabetes, independently of known risk SNPs. PTPN2 coding variants possibly induce non-specific Type 1A diabetes phenotypes in individuals with human leukocyte antigen-mediated disease susceptibility. Our findings warrant further validation.

Published

2017

181. Efficacy and safety of two doses of Norditropin

Author

Keiichi, Ozono, Tsutomu, Ogata, Reiko, Horikawa, Yoichi, Matsubara, Yoshihisa, Ogawa, Keiji, Nishijima, and Susumu, Yokoya

Subjects

Male, Dose-Response Relationship, Drug, Human Growth Hormone, Noonan Syndrome, Body Height, Drug Administration Schedule, Treatment Outcome, Asian People, Double-Blind Method, Japan, Child, Preschool, Humans, Female, Child, Follow-Up Studies

Abstract

This randomized double-blind multicenter trial (NCT01927861) evaluated the growth-promoting effect and safety of Norditropin

Published

2017

182. Phenotypic Variation in 46,XX Disorders of Sex Development due to the NR5A1 p.R92W Variant: A Sibling Case Report and Literature Review

Author

Kei, Takasawa, Maki, Igarashi, Makoto, Ono, Akira, Takemoto, Shuji, Takada, Atsuyuki, Yamataka, Tsutomu, Ogata, Tomohiro, Morio, Maki, Fukami, and Kenichi, Kashimada

Subjects

Male, Heterozygote, Disorder of Sex Development, 46,XY, Phenotype, Siblings, Mutation, Missense, Humans, Female, Steroidogenic Factor 1, Pedigree

Abstract

Recently, a heterozygous missense mutation in NR5A1, p.R92W, was identified as a cause of 46,XX testicular/ovo-testicular disorders of sexual development (DSD). We report a sibling pair with 46,XX DSD due to an NR5A1 mutation with distinct phenotypes, including external and internal genitalia and gonads, for whom different rearing sexes were selected. Thus, the phenotypes of p.R92W vary, even within a family. The father of the patients showed oligozoospermia with the p.R92W mutation, suggesting that in 46,XY individuals, the mutation would cause various gonadal phenotypes. We review and discuss the general role of the R92W mutation in sexual development.

Published

2017

183. Two patients with MIRAGE syndrome lacking haematological features: role of somatic second-site reversion SAMD9 mutations

Author

Angela Huebner, Katrin Koehler, Tsutomu Ogata, Hirohito Shima, Klaus Mohnike, Yumiko Nomura, Akira Satoh, Markus Schuelke, Ramona Jühlen, Kazuhiko Sugimoto, Satoshi Narumi, and Maki Fukami

Subjects

0301 basic medicine, Adrenal disorder, Biology, medicine.disease_cause, Germline, 03 medical and health sciences, symbols.namesake, 0302 clinical medicine, X Chromosome Inactivation, Genetics, medicine, Missense mutation, Humans, Allele, Skewed X-inactivation, Genetics (clinical), Sanger sequencing, Mutation, Intracellular Signaling Peptides and Proteins, Infant, Proteins, medicine.disease, Molecular biology, 030104 developmental biology, 030220 oncology & carcinogenesis, Child, Preschool, Myelodysplastic Syndromes, symbols, Congenital disorder, Adrenal Insufficiency

Abstract

BackgroundMyelodysplasia, infection, restriction of growth, adrenal hypoplasia, genital phenotypes and enteropathy (MIRAGE) syndrome is a recently described congenital disorder caused by heterozygous SAMD9 mutations. The phenotypic spectrum of the syndrome remains to be elucidated.Methods and resultsWe describe two unrelated patients who showed manifestations compatible with MIRAGE syndrome, with the exception of haematological features. Leucocyte genomic DNA samples were analysed with next-generation sequencing and Sanger sequencing, revealing the patients to have two de novoSAMD9 mutations on the same allele (patient 1 p.[Gln695*; Ala722Glu] and patient 2 p.[Gln39*; Asp769Gly]). In patient 1, p.Gln695* was absent in genomic DNA extracted from hair follicles, implying that the non-sense mutation was acquired somatically. In patient 2, with the 46,XX karyotype, skewed X chromosome inactivation pattern was found in leucocyte DNA, suggesting monoclonality of cells in the haematopoietic system. In vitro expression experiments confirmed the growth-restricting capacity of the two missense mutant SAMD9 proteins that is a characteristic of MIRAGE-associated SAMD9 mutations.ConclusionsAcquisition of a somatic nonsense SAMD9 mutation in the cells of the haematopoietic system might revert the cellular growth repression caused by the germline SAMD9 mutations (ie, second-site reversion mutations). Unexpected lack of haematological features in the two patients would be explained by the reversion mutations.

Published

2017

184. Gain-of-function mutations in G-protein-coupled receptor genes associated with human endocrine disorders

Author

Maki Igarashi, Tsutomu Ogata, Mami Miyado, Maki Fukami, and Erina Suzuki

Subjects

0301 basic medicine, medicine.medical_specialty, Endocrinology, Diabetes and Metabolism, 030209 endocrinology & metabolism, Biology, medicine.disease_cause, Endocrine System Diseases, G Protein-Coupled Receptor Gene, Germline, Frameshift mutation, Receptors, G-Protein-Coupled, 03 medical and health sciences, 0302 clinical medicine, Endocrinology, Internal medicine, medicine, Humans, Receptor, Gene, G protein-coupled receptor, Mutation, Phenotype, 030104 developmental biology, Gain of Function Mutation

Abstract

The human genome encodes more than 700 G-protein-coupled receptors (GPCRs), many of which are involved in hormone secretion. To date, more than 100 gain-of-function (activating) mutations in at least ten genes for GPCRs, in addition to several loss-of-function mutations, have been implicated in human endocrine disorders. Previously reported gain-of-function GPCR mutations comprise various missense substitutions, frameshift mutations, intragenic inframe deletions and copy-number gains. Such mutations appear in both germline and somatic tumour cells, and lead to various hormonal abnormalities reflecting excessive receptor activity. Phenotypic consequences of these mutations include distinctive endocrine syndromes, as well as relatively common hormonal abnormalities. Such mutations encode hyperfunctioning receptors with increased constitutive activity, broadened ligand specificity, increased ligand sensitivity and/or delayed receptor desensitization. Furthermore, recent studies proposed a paradoxical gain-of-function mechanism caused by inactive GPCR mutants. Molecular diagnosis of GPCR activating mutations serves to improve the clinical management of mutation-positive patients. This review aims to introduce new aspects regarding gain-of-function mutations in GPCR genes associated with endocrine disorders.

Published

2017

185. Functional missense and splicing variants in the retinoic acid catabolizing enzyme CYP26C1 in idiopathic short stature

Author

Nadine H Hauer, Christian Thiel, Maki Fukami, Lonny Juergensen, David Hassel, Gudrun A. Rappold, Tsutomu Ogata, Yasuhiro Naiki, Birgit Weiss, Antonino Montalbano, and Ralph Roeth

Subjects

0301 basic medicine, Adult, Male, Adolescent, RNA Splicing, Population, Retinoic acid, Mutation, Missense, Biology, Quantitative trait locus, Short stature, Article, 03 medical and health sciences, symbols.namesake, chemistry.chemical_compound, Cell Line, Tumor, Genetics, medicine, Missense mutation, Animals, Humans, Exome, education, Child, Dwarfism, Pituitary, Genetics (clinical), Cytochrome P450 Family 26, Zebrafish, Sanger sequencing, education.field_of_study, medicine.disease, Idiopathic short stature, 030104 developmental biology, chemistry, symbols, Female, medicine.symptom

Abstract

Height is a complex quantitative trait with a high heritability. Short stature is diagnosed when height is significantly below the average of the general population for that person’s age and sex. We have recently found that the retinoic acid degrading enzyme CYP26C1 modifies SHOX deficiency phenotypes toward more severe clinical manifestations. Here, we asked whether damaging variants in CYP26C1 alone could lead to short stature. We performed exome and Sanger sequencing to analyze 856 individuals with short stature where SHOX deficiency was previously excluded. Three different damaging missense variants and one splicing variant were identified in six independent individuals; the functional significance of the identified variants was tested in vitro or in vivo using zebrafish as a model. The genetic and functional data reported here indicate that CYP26C1 represents a novel gene underlying growth disorders and that damaging variants in the absence of SHOX variants can lead to short stature.

Published

2017

186. Efficacy and safety of octreotide for the treatment of congenital hyperinsulinism: a prospective, open-label clinical trial and an observational study in Japan using a nationwide registry

Author

Osamu Arisaka, Hironori Nishibori, Tohru Yorifuji, Yuki Hosokawa, Tsutomu Ogata, Rie Kawakita, Keiichi Ozono, Toshimi Sairenchi, Yukihiro Hasegawa, Susumu Yokoya, Michiya Masue, and Satoshi Kusuda

Subjects

Blood Glucose, Male, medicine.medical_specialty, Endocrinology, Diabetes and Metabolism, Octreotide, 030209 endocrinology & metabolism, Hypoglycemia, 03 medical and health sciences, 0302 clinical medicine, Endocrinology, Japan, 030225 pediatrics, Internal medicine, medicine, Humans, Prospective Studies, Registries, Adverse effect, Blood glucose monitoring, medicine.diagnostic_test, business.industry, Remission Induction, Infant, Newborn, Infant, medicine.disease, Clinical trial, Treatment Outcome, Anesthesia, Congenital hyperinsulinism, Observational study, Congenital Hyperinsulinism, Female, Open label, business, Somatostatin, medicine.drug

Abstract

Octreotide, a long-acting somatostatin analog, has been used for treating hypoglycemia caused by congenital hyperinsulinism (CHI). However, octreotide has not been evaluated in clinical trials and has not been approved in any developed country. We aimed to test the efficacy and safety of octreotide for diazoxide-unresponsive CHI through a combination of a single-arm, open-label clinical trial (SCORCH study) and an observational study to collect data on the clinical course of patients treated off-label in Japan (SCORCH registry). In the SCORCH study, 5 patients were stabilized (blood glucose > 45 mg/dL) by hypertonic glucose infusion, and treated by continuous subcutaneous octreotide infusion at a dose of 5-25 μg/kg/day. Continuous blood glucose monitoring was performed between -24 and +48 hours. In 3 patients, a clinically meaningful rise in blood glucose was achieved and therapy was continued. The glucose infusion was gradually decreased and stopped after 5, 11, and 174 days, respectively. In one case, remission of CHI was reached after 606 days and octreotide was discontinued. The SCORCH registry included 19 diazoxide-unresponsive patients treated by subcutaneous octreotide, by continuous infusion or multiple daily injections. Of the 17 patients treated with hypertonic glucose infusion, the infusion rate was reduced after 4 weeks to less than 50% in 11 patients (64.7%) and stopped in 9 (52.9%). During the combined observation period of 695.4 patient-months in both studies, no severe adverse events related to octreotide were observed. In conclusion, subcutaneous octreotide injection was effective and well tolerated in the majority of patients with diazoxide-unresponsive CHI.

Published

2017

187. Knockout of Murine Mamld1 Impairs Testicular Growth and Daily Sperm Production but Permits Normal Postnatal Androgen Production and Fertility

Author

Kazuki Saito, Shigeru Nakamura, Kenji Miyado, Maki Fukami, Tsutomu Ogata, Mami Miyado, Momori Katsumi, and Kaoru Yoshida

Subjects

0301 basic medicine, Male, Serum, Time Factors, lcsh:Chemistry, Mice, Spermatocytes, Testosterone, lcsh:QH301-705.5, Spectroscopy, Sperm motility, Mice, Knockout, Sperm Count, Gene Expression Regulation, Developmental, Dihydrotestosterone, General Medicine, Seminiferous Tubules, Spermatozoa, Computer Science Applications, Seminiferous tubule, medicine.anatomical_structure, Phenotype, Knockout mouse, Androgens, Sperm Motility, Female, medicine.drug, medicine.medical_specialty, endocrine system, medicine.drug_class, androgen, Biology, testis, Catalysis, Article, knockout mouse, mutation, reproduction, Inorganic Chemistry, Andrology, 03 medical and health sciences, Hypergonadotropic hypogonadism, Internal medicine, medicine, Animals, Humans, Physical and Theoretical Chemistry, Molecular Biology, Models, Genetic, urogenital system, Organic Chemistry, Androstenedione, Androgen, medicine.disease, Spermatogonia, Mice, Inbred C57BL, 030104 developmental biology, Endocrinology, Fertility, lcsh:Biology (General), lcsh:QD1-999, Microscopy, Electron, Scanning, Spermatogenesis, Transcription Factors

Abstract

MAMLD1 has been implicated in testicular function in both human and mouse fetuses. Although three patients with MAMLD1 mutations were reported to have hypergonadotropic hypogonadism in their teens, the functional significance of MAMLD1 in the postnatal testis remains unclear. Here, we analyzed the phenotype of Mamld1 knockout (KO) male mice at reproductive ages. The reproductive organs of KO male mice were morphologically unremarkable, except for relatively small testes. Seminiferous tubule size and number of proliferating spermatogonia/spermatocytes were reduced in the KO testis. Daily sperm production of KO mice was mildly attenuated, whereas total sperm counts in epididymal semen remained normal. Sperm motility and morphology, as well as androgen levels in serum and testicular tissues and the number of pups born from cross-mated wildtype (WT) female mice, were comparable between WT and KO male mice. These results indicate that MAMLD1 contributes to the maintenance of postnatal testicular growth and daily sperm production but is dispensable for androgen biosynthesis and fertility. MAMLD1 likely plays supporting roles in multiple and continuous steps of male reproduction.

Published

2017

188. Nomenclature of primary amenorrhea: A proposal document of the Japan Society of Obstetrics and Gynecology committee for the redefinition of primary amenorrhea

Author

Makio, Shozu, Hiroshi, Ishikawa, Reiko, Horikawa, Hideya, Sakakibara, Shun-Ichiro, Izumi, Takashi, Ohba, Yasushi, Hirota, Tsutomu, Ogata, Yutaka, Osuga, and Koji, Kugu

Subjects

Menarche, Adolescent, Japan, Gynecology, Terminology as Topic, Humans, Female, Amenorrhea, Societies, Medical

Abstract

The aim of this study was to provide medical terms to describe the condition of a girl who should be evaluated for primary amenorrhea in order to facilitate intervention at an appropriate time.We performed a literature and clinical guidelines search for recent practices with regard to menarche and discussed relevant cases that had been experienced by committee members. Additionally, we theoretically reviewed medical terms defined in the Glossary Book of Obstetrics and Gynecology in Japan (Japan Society of Obstetrics and Gynecology, 3rd edition).The committee for the redefinition of primary amenorrhea proposed the introduction of two terms and the deletion of one term that had been defined by the Japan Society of Obstetrics and Gynecology, instead of changing the age definition of primary amenorrhea. 'Delayed menarche' was introduced to describe a condition in which a girl has never experienced cyclic menstruation (menarche) by 15-17 years of age. 'Late menarche' was also introduced to describe a condition in which a girl has experienced menarche at 15 years of age or older. 'Delayed menstruation,' which was defined as a condition in which a girl experiences menarche at 15-18 years of age, was deleted.The new terms 'delayed menarche' and 'late menarche' were introduced, and the term 'delayed menstruation' was deleted. The new system might help in the early detection and appropriate treatment of primary amenorrhea.

Published

2017

189. Safety and efficacy of treatment with asfotase alfa in patients with hypophosphatasia: Results from a Japanese clinical trial

Author

Atsushi Watanabe, Toshihiro Tajima, Keisuke Nagasaki, Toshimi Michigami, Tsutomu Ogata, Katsusuke Yamamoto, Toru Kikuchi, Takuo Kubota, Masayuki Kokaji, Ikuma Fujiwara, Hiroshi Mochizuki, Keiichi Ozono, Koji Tatebayashi, Satoshi Okada, Taichi Kitaoka, and Shuichi Yatsuga

Subjects

0301 basic medicine, Adult, Male, medicine.medical_specialty, Adolescent, Endocrinology, Diabetes and Metabolism, Recombinant Fusion Proteins, Hypophosphatasia, Gene mutation, 03 medical and health sciences, Young Adult, 0302 clinical medicine, Endocrinology, Japan, Internal medicine, medicine, Humans, Respiratory function, Hypocalcaemia, Adverse effect, Child, business.industry, Infant, Newborn, ALPL, Infant, medicine.disease, Alkaline Phosphatase, Clinical trial, Hyperphosphatemia, Survival Rate, 030104 developmental biology, Treatment Outcome, Asfotase alfa, Child, Preschool, Immunoglobulin G, Mutation, Calcium, Female, business, 030217 neurology & neurosurgery

Abstract

SummaryObjective Hypophosphatasia (HPP) is a rare skeletal disease characterized by hypomineralization and low alkaline phosphatase activity. Asfotase alfa (AA) has been recently developed to treat HPP complications. This study evaluated its safety and efficacy in Japan. Design Open-label, multicentre, prospective trial. Patients were enrolled in 11 hospitals from June 2014 to July 2015. Patients Thirteen patients (9 females, 4 males) ages 0 days to 34 years at baseline were enrolled and treated with AA (2 mg/kg three times weekly subcutaneously in all but one patient). All had ALPL gene mutations. HPP forms were perinatal (n=6), infantile (n=5), childhood (n=1) and adult (n=1). Measurements Safety determined from adverse events (AEs) and laboratory data was the primary outcome measure. Efficacy was assessed as a secondary outcome measure from overall survival, respiratory status, rickets severity and gross motor development. Results Injection site reactions were the most frequent AEs. Serious AEs possibly related to treatment were convulsion and hypocalcaemia observed in a patient with the perinatal form. In addition, hypercalcaemia and/or hyperphosphatemia was observed in three patients with the infantile form and a low-calcium and/or low-phosphate formula was given to these patients. With respect to efficacy, all patients survived and the radiographic findings, developmental milestones and respiratory function improved. Conclusion Asfotase alfa therapy improved skeletal, respiratory and physical symptoms with a few serious AEs in patients with HPP. Our results add support to the safety and efficacy of AA therapy for HPP patients.

Published

2017

190. Validation of auxological reference values for Japanese children with Noonan syndrome and comparison with growth in children with Turner syndrome

Author

Satoru Sakazume, Susumu Yokoya, Tsutomu Ogata, Tomonobu Hasegawa, Toshiro Nagai, Tsuyoshi Isojima, and Toshio Nakanishi

Subjects

Pediatrics, medicine.medical_specialty, Endocrinology, Diabetes and Metabolism, Turner syndrome, 030209 endocrinology & metabolism, growth pattern, 03 medical and health sciences, 0302 clinical medicine, Endocrinology, growth chart, 030225 pediatrics, medicine, Noonan syndrome, validation, Growth chart, business.industry, Longitudinal growth, Significant difference, medicine.disease, Confidence interval, Clinical Practice, Reference values, Pediatrics, Perinatology and Child Health, Original Article, business

Abstract

We recently published growth references for Japanese individuals with Noonan syndrome (NS). However, it is uncertain whether these references can be used to evaluate the longitudinal growth of children with NS. In addition, these charts did not include detailed values suitable for clinical practice, and they did not include weight-for-height (WFH) charts. In the present study, we validated the references and established new WFH charts for children with NS. In addition, we investigated the growth patterns of these children by comparing them with those of children with Turner syndrome (TS), as well as with those of the normal population. To validate our reference values, we enrolled 32 subjects from our previous study with data available at both a younger (≤ 5 yr) and an older age (≥ 15 yr). We then investigated longitudinal changes in NS-specific standard deviation scores (SDSs) for height in these subjects. There was no significant difference between the initial and later SDSs (mean difference: –0.12, 95% confidence interval: –0.26–0.023, P = 0.10), suggesting that the references could be applied in clinical practice. We also confirmed that the growth patterns of children with NS in each index are significantly different from those of children with TS. In conclusion, we confirmed auxological reference values for Japanese children with NS.

Published

2017

191. Genetic heterogeneity of patients with suspected Silver-Russell syndrome: genome-wide copy number analysis in 82 patients without imprinting defects

Author

Kazuki Yamazawa, Tomoko Fuke, Zenro Kizaki, Yoshika Matsukura, Hisakazu Nakajima, Keiko Matsubara, Takanobu Inoue, Tsutomu Ogata, Akira Oka, Maki Fukami, Chie Harashima, Seiji Mizuno, Akie Nakamura, Masayo Kagami, Kumi Tsumura, Shinichiro Sano, and Tatsuji Hasegawa

Subjects

0301 basic medicine, Male, Pathogenic copy number variation, lcsh:QH426-470, DNA Copy Number Variations, Heart Diseases, Developmental Disabilities, Williams syndrome, Copy number analysis, Short Report, lcsh:Medicine, 030105 genetics & heredity, Biology, Bioinformatics, 4p microdeletion syndrome, Epigenesis, Genetic, Mosaic trisomy 18, 03 medical and health sciences, Genetic Heterogeneity, Genomic Imprinting, Young Adult, parasitic diseases, Genetics, medicine, Humans, Copy-number variation, Global developmental delay, Child, Molecular Biology, Genetics (clinical), Comparative Genomic Hybridization, Genetic heterogeneity, Silver–Russell syndrome, lcsh:R, Brachydactyly, Netchine-Harbison clinical scoring system, Infant, DNA Methylation, medicine.disease, lcsh:Genetics, Silver-Russell Syndrome, 19q13.11 deletion syndrome, 030104 developmental biology, Array comparative genomic hybridization, Child, Preschool, Female, Trisomy, Developmental Biology, Congenital disorder

Abstract

Background Silver-Russell syndrome (SRS) is a rare congenital disorder characterized by pre- and postnatal growth failure and dysmorphic features. Recently, pathogenic copy number variations (PCNVs) and imprinting defects other than hypomethylation of the H19-differentially methylated region (DMR) and maternal uniparental disomy chromosome 7 have been reported in patients with the SRS phenotype. This study aimed to clarify the frequency and clinical features of patients with SRS phenotype caused by PCNVs. Methods We performed array comparative genomic hybridization analysis using a catalog array for 54 patients satisfying the Netchine-Harbison clinical scoring system (NH-CSS) (SRS-compatible) and for 28 patients presenting with three NH-CSS items together with triangular face and/or fifth finger clinodactyly and/or brachydactyly (SRS-like) without abnormal methylation levels of 9 DMRs related to known imprinting disorders. We then investigated the clinical features of patients with PCNVs. Results Three of the 54 SRS-compatible patients (5.6%) and 2 of the 28 SRS-like patients (7.1%) had PCNVs. We detected 3.5 Mb deletion in 4p16.3, mosaic trisomy 18, and 3.77–4.00 Mb deletion in 19q13.11-12 in SRS-compatible patients, and 1.41–1.97 Mb deletion in 7q11.23 in both SRS-like patients. Congenital heart diseases (CHDs) were identified in two patients and moderate to severe global developmental delay was observed in four patients. Conclusions Of the patients in our study, 5.6% of SRS-compatible and 7.1% of SRS-like patients had PCNVs. All PCNVs have been previously reported for genetic causes of contiguous deletion syndromes or mosaic trisomy 18. Our study suggests patients with PCNVs, who have a phenotype resembling SRS, show a high tendency towards CHDs and/or apparent developmental delay.

Published

2017

192. Diagnosis and management of Silver-Russell syndrome: first international consensus statement

Author

Frédéric Brioude, I. Karen Temple, Jet Bliek, Adda Grimberg, Thomas Eggermann, Gudrun E. Moore, Agnès Linglart, Klaus Mohnike, Zeynep Tümer, Edith Said, Ana Pinheiro Machado Canton, Renuka P Dias, Oluwakemi Lokulo-Sodipe, Madeleine D. Harbison, Meropi Toumba, Gerhard Binder, Béatrice Dubern, Anita C. S. Hokken-Koelega, Jennifer Salem, Deborah J G Mackay, Susan M. O’Connell, Miriam Elbracht, Irène Netchine, Justin H Davies, David Monk, Silvia Russo, Emma Wakeling, Mohamad Maghnie, Isabelle Oliver Petit, Krystyna H. Chrzanowska, Eloise Giabicani, Philip Murray, Masayo Kagami, Alexander A. L. Jorge, Tsutomu Ogata, Karen Grønskov, Pediatrics, North West london hospitals NHS Trust, Centre de Recherche Saint-Antoine (UMRS893), Université Pierre et Marie Curie - Paris 6 (UPMC)-Institut National de la Santé et de la Recherche Médicale (INSERM), MAGIC Foundation, Department of Clinical Genetics, University of Amsterdam [Amsterdam] (UvA), CHU Trousseau [APHP], Assistance publique - Hôpitaux de Paris (AP-HP) (AP-HP)-Sorbonne Université (SU), Unité de Recherche en Epidémiologie Nutritionnelle (UREN), Institut National de la Santé et de la Recherche Médicale (INSERM)-Université Sorbonne Paris Cité (USPC)-Université Paris 13 (UP13)-Conservatoire National des Arts et Métiers [CNAM] (CNAM)-Institut National de la Recherche Agronomique (INRA), Assistance publique - Hôpitaux de Paris (AP-HP) (AP-HP), Institut National de la Santé et de la Recherche Médicale (INSERM), Sorbonne Université (SU), Clinical genetic clinic, Copenhagen University Hospital, Erasmus University Medical Center [Rotterdam] (Erasmus MC), Service d'endocrinologie pédiatrique [CHU Bicêtre], Université Paris-Sud - Paris 11 (UP11)-Assistance publique - Hôpitaux de Paris (AP-HP) (AP-HP), Fetal Growth and Developmental Group, University College of London [London] (UCL), Department of Endocrinology and Metabolism, National Research Institute for Child Health and Development, Department of Pediatrics and Medical Genetics, St. Luke's Hospital, Service de néphrologie et pédiatrie générale [CHU Trousseau], Université Pierre et Marie Curie - Paris 6 (UPMC)-Assistance publique - Hôpitaux de Paris (AP-HP) (AP-HP)-CHU Trousseau [APHP], Assistance publique - Hôpitaux de Paris (AP-HP) (AP-HP)-Sorbonne Université (SU)-Sorbonne Université (SU), Icahn School of Medicine at Mount Sinai [New York] (MSSM), Human Genetics and Genomic Medicine group, Faculty of Medicine, Université Paris 13 (UP13)-Institut National de la Recherche Agronomique (INRA)-Conservatoire National des Arts et Métiers [CNAM] (CNAM), HESAM Université - Communauté d'universités et d'établissements Hautes écoles Sorbonne Arts et métiers université (HESAM)-HESAM Université - Communauté d'universités et d'établissements Hautes écoles Sorbonne Arts et métiers université (HESAM)-Université Sorbonne Paris Cité (USPC)-Institut National de la Santé et de la Recherche Médicale (INSERM), Centre de Recherche Saint-Antoine (CR Saint-Antoine), Institut National de la Santé et de la Recherche Médicale (INSERM)-Université Pierre et Marie Curie - Paris 6 (UPMC), Université Paris 13 (UP13)-Institut National de la Recherche Agronomique (INRA)-Conservatoire National des Arts et Métiers [CNAM] (CNAM)-Université Sorbonne Paris Cité (USPC)-Institut National de la Santé et de la Recherche Médicale (INSERM), Assistance publique - Hôpitaux de Paris (AP-HP) (APHP), Université Paris-Sud - Paris 11 (UP11)-Assistance publique - Hôpitaux de Paris (AP-HP) (APHP), Université Pierre et Marie Curie - Paris 6 (UPMC)-Assistance publique - Hôpitaux de Paris (AP-HP) (APHP)-CHU Trousseau [APHP], and Human Genetics

Subjects

0301 basic medicine, medicine.medical_specialty, Pediatrics, Internationality, Endocrinology, Diabetes and Metabolism, Gonadotropin-Releasing Hormone/therapeutic use, Human Growth Hormone/therapeutic use, MESH: Disease Management, law.invention, Gonadotropin-Releasing Hormone, 03 medical and health sciences, Endocrinology, Randomized controlled trial, law, Internal medicine, MESH: Gonadotropin-Releasing Hormone, medicine, MESH: Human Growth Hormone, Humans, Silver-Russell Syndrome/diagnosis, Motor skill, [SDV.MHEP.PED]Life Sciences [q-bio]/Human health and pathology/Pediatrics, MESH: Humans, Human Growth Hormone, business.industry, Adrenarche, Disease Management, [SDV.MHEP.EM]Life Sciences [q-bio]/Human health and pathology/Endocrinology and metabolism, medicine.disease, 3. Good health, Diabetes and Metabolism, Growth hormone treatment, Natural history, Silver-Russell Syndrome, 030104 developmental biology, MESH: Silver-Russell Syndrome, Speech delay, MESH: Internationality, Small for gestational age, medicine.symptom, business, Psychosocial

Abstract

International audience; This Consensus Statement summarizes recommendations for clinical diagnosis, investigation and management of patients with Silver-Russell syndrome (SRS), an imprinting disorder that causes prenatal and postnatal growth retardation. Considerable overlap exists between the care of individuals born small for gestational age and those with SRS. However, many specific management issues exist and evidence from controlled trials remains limited. SRS is primarily a clinical diagnosis; however, molecular testing enables confirmation of the clinical diagnosis and defines the subtype. A 'normal' result from a molecular test does not exclude the diagnosis of SRS. The management of children with SRS requires an experienced, multidisciplinary approach. Specific issues include growth failure, severe feeding difficulties, gastrointestinal problems, hypoglycaemia, body asymmetry, scoliosis, motor and speech delay and psychosocial challenges. An early emphasis on adequate nutritional status is important, with awareness that rapid postnatal weight gain might lead to subsequent increased risk of metabolic disorders. The benefits of treating patients with SRS with growth hormone include improved body composition, motor development and appetite, reduced risk of hypoglycaemia and increased height. Clinicians should be aware of possible premature adrenarche, fairly early and rapid central puberty and insulin resistance. Treatment with gonadotropin-releasing hormone analogues can delay progression of central puberty and preserve adult height potential. Long-term follow up is essential to determine the natural history and optimal management in adulthood.

Published

2017

193. Comprehensive and quantitative multilocus methylation analysis reveals the susceptibility of specific imprinted differentially methylated regions to aberrant methylation in Beckwith–Wiedemann syndrome with epimutations

Author

Yoshio Makita, Kazuhiko Nakabayashi, Tsutomu Ogata, Yuhei Hamasaki, Makoto Migita, Nobuhiko Okamoto, Kosuke Jozaki, Hitomi Yatsuki, Keiko Matsubara, Toshiyuki Maeda, Kenichiro Hata, Muneaki Matsuo, Hidefumi Tonoki, Hidenobu Soejima, Kenichi Nishioka, Hirofumi Ohashi, Rika Kosaki, Tsunehiro Mukai, Fumio Takada, Yasufumi Ohtsuka, Keiichiro Joh, and Ken Higashimoto

Subjects

Male, congenital, hereditary, and neonatal diseases and abnormalities, Beckwith-Wiedemann Syndrome, Adolescent, Beckwith–Wiedemann syndrome, Biology, medicine.disease_cause, medicine, multiple methylation defects, Humans, Genetic Predisposition to Disease, Original Research Article, Allele, Child, Alleles, Genetics (clinical), Regulation of gene expression, Genetics, Mutation, DNA methylation, Gene Expression Profiling, Infant, Newborn, Infant, DNA, medicine.disease, genomic imprinting, differentially methylated region, Gene expression profiling, Differentially methylated regions, Gene Expression Regulation, Child, Preschool, Spectrometry, Mass, Matrix-Assisted Laser Desorption-Ionization, Female, Genomic imprinting

Abstract

Purpose: Expression of imprinted genes is regulated by DNA methylation of differentially methylated regions (DMRs). Beckwith–Wiedemann syndrome is an imprinting disorder caused by epimutations of DMRs at 11p15.5. To date, multiple methylation defects have been reported in Beckwith–Wiedemann syndrome patients with epimutations; however, limited numbers of DMRs have been analyzed. The susceptibility of DMRs to aberrant methylation, alteration of gene expression due to aberrant methylation, and causative factors for multiple methylation defects remain undetermined. Methods: Comprehensive methylation analysis with two quantitative methods, matrix-assisted laser desorption/ionization mass spectrometry and bisulfite pyrosequencing, was conducted across 29 DMRs in 54 Beckwith–Wiedemann syndrome patients with epimutations. Allelic expressions of three genes with aberrant methylation were analyzed. All DMRs with aberrant methylation were sequenced. Results: Thirty-four percent of KvDMR1–loss of methylation patients and 30% of H19DMR–gain of methylation patients showed multiple methylation defects. Maternally methylated DMRs were susceptible to aberrant hypomethylation in KvDMR1–loss of methylation patients. Biallelic expression of the genes was associated with aberrant methylation. Cis-acting pathological variations were not found in any aberrantly methylated DMR. Conclusion: Maternally methylated DMRs may be vulnerable to DNA demethylation during the preimplantation stage, when hypomethylation of KvDMR1 occurs, and aberrant methylation of DMRs affects imprinted gene expression. Cis-acting variations of the DMRs are not involved in the multiple methylation defects.

Published

2014

194. Cytochrome P450 oxidoreductase deficiency: Rare congenital disorder leading to skeletal malformations and steroidogenic defects

Author

Tsutomu Ogata and Maki Fukami

Subjects

Genetics, medicine.medical_specialty, Antley–Bixler syndrome, business.industry, Virilization, medicine.disease, Compound heterozygosity, Endocrinology, CYP17A1, Internal medicine, Pediatrics, Perinatology and Child Health, medicine, Missense mutation, Congenital adrenal hyperplasia, medicine.symptom, Congenital Malformation Syndrome, business, Congenital disorder

Abstract

Cytochrome P450 oxidoreductase (POR) deficiency (PORD) is a newly characterized disorder. PORD is caused by homozygous or compound heterozygous mutations in POR encoding an electron donor for several microsomal enzymes such as CYP21A2, CYP17A1, CYP19A1, CYP51A1, and CYP26A1-C1. Molecular defects of PORD include a Japanese founder mutation p.R457H, as well as various missense, nonsense, frameshift, and splice-site mutations and exonic deletions. PORD leads to unique skeletal malformations referred to as Antley-Bixler syndrome, in addition to 46,XX and 46,XY disorders of sex development, pubertal failure, adrenal dysfunction, and maternal virilization during pregnancy. Such clinical features are ascribable to impaired activities of the POR-dependent microsomal enzymes. PORD represents one form of congenital adrenal hyperplasia, although it can occur as a congenital malformation syndrome and a disorder of sex development. Phenotypic severity of PORD is highly variable and only partly depends on the residual activity of the mutant proteins. It is possible that PORD remains undiagnosed in several patients. Detailed hormonal assessment and molecular analysis are useful for diagnosis of PORD.

Published

2014

195. Clinical and molecular studies in four patients with SRY-positive 46,XX testicular disorders of sex development: implications for variable sex development and genomic rearrangements

Author

Fumio Takada, Shinichi Nakashima, Hideki Kawamura, Maki Fukami, Maki Igarashi, Tsutomu Ogata, and Akira Ohishi

Subjects

Adult, Male, medicine.medical_specialty, DNA End-Joining Repair, Testicular Disorder, 46, XX Testicular Disorders of Sex Development, Biology, Translocation, Genetic, Young Adult, Pregnancy, X Chromosome Inactivation, Molecular genetics, Genetics, medicine, Humans, Genes, sry, Homologous Recombination, Genetics (clinical), Chromosomes, Human, X, Comparative Genomic Hybridization, Chromosomes, Human, Y, Infant, Newborn, Cytogenetics, Infant, Human genetics, Testis determining factor, Genetic epidemiology, Statistical genetics, Child, Preschool, Medical genetics, Female

Abstract

We report four patients with SRY-positive 46,XX testicular disorders of sex development (46,XX-TDSD) (cases 1-4). Case 1 exhibited underdeveloped external genitalia with hypospadias, case 2 manifested micropenis and cases 3 and 4 showed normal external genitalia. The Xp;Yp translocations occurred between the X- and the Y-differential regions in case 1, between PRKX and inverted PRKY in case 2 and between the X-chromosomal short arm pseudoautosomal region and the Y-differential regions in cases 3 and 4. The distance of the Yp breakpoint from SRY was ~0.75 Mb in case 1, ~6.5 Mb in case 2, ~2.3 Mb in case 3 and ~72 kb in case 4. The Xp;Yp translocation occurred within an 87-bp homologous segment of PRKX and PRKY in case 2, and between non-homologous regions with addition of an 18-bp sequence of unknown origin in case 4. X-inactivation analysis revealed random inactivation in cases 1-4. The results argue against the notion that undermasculinization in 46,XX-TDSD is prone to occur when translocated Yp materials are small (100 kb of the Y-differential region), and imply that the Xp;Yp translocations result from several mechanisms including non-allelic homologous recombination and non-homologous end joining.

Published

2014

196. Early vitamin K deficiency bleeding in a neonate associated with maternal Crohn’s disease

Author

Akira Ohishi, Shinichi Nakashima, Tsutomu Ogata, and Shigeo Iijima

Subjects

Adult, medicine.medical_specialty, Pediatrics, Anemia, Disease, Gastroenterology, Crohn Disease, Pregnancy, Internal medicine, Humans, Medicine, Neonatology, Crohn's disease, business.industry, Infant, Newborn, Obstetrics and Gynecology, Gestational age, Vitamin K Deficiency Bleeding, medicine.disease, Pregnancy Complications, Purpura, Pediatrics, Perinatology and Child Health, Gestation, Female, medicine.symptom, business

Abstract

We report herein a case of early vitamin K deficiency bleeding (VKDB) in a neonate associated with maternal Crohn's disease. A female neonate was born at 37 weeks' gestation and weighed 2778 g. She developed broad purpura on her back on day 1. Laboratory data showed anemia, prolonged coagulation time and elevated protein induced by vitamin K absence or antagonist-II. Early VKDB has not been reported in a neonate born from mother with active Crohn's disease. It is essential to give vitamin K selectively as soon as possible after birth to prevent early VKDB in neonates.

Published

2014

197. Understanding the pathological manifestations of aromatase excess syndrome: lessons for clinical diagnosis

Author

Maki Fukami, Tsutomu Ogata, and Makio Shozu

Subjects

medicine.medical_specialty, endocrine system, Aromatase inhibitor, CYP19A1 mutation, biology, Aromatase excess syndrome, gynecomastia, business.industry, medicine.drug_class, Endocrinology, Diabetes and Metabolism, Bone age, Review, medicine.disease, aromatase excess syndrome, Endocrinology, Gynecomastia, Estrogen, Internal medicine, Gene duplication, biology.protein, Medicine, Aromatase, business, Pathological

Abstract

CYP19A1 Aromatase excess syndrome is characterized by pre- or peripubertal onset of gynecomastia due to estrogen excess because of a gain-of-function mutation in the aromatase gene (CYP19A1). Subchromosomal recombination events including duplication, deletion, and inversion has been identified. The latter two recombinations recruit novel promoters for CYP19A1 through a unique mechanism. Gynecomastia continues for life, and although the general condition is well preserved, it may cause psychological issues. Minor symptoms (variably advanced bone age and short adult height), if present, are exclusively because of estrogen excess. Serum estradiol levels are elevated in 48% of affected males, but are not necessarily useful for diagnosis. Molecular analysis of CYP19A1 mutations is mandatory to confirm aromatase excess syndrome diagnosis. Furthermore, the use of an aromatase inhibitor can ameliorate gynecomastia.

Published

2014

198. Mutation spectrum and phenotypic variation in nine patients with SOX2 abnormalities

Author

Maki Fukami, Junichi Suzuki, Shun Soneda, Koji Muroya, Sumito Dateki, Shinichiro Sano, Toshiro Nagai, Yukiyo Yamamoto, Hiroshi Wada, Reiko Saito, Tsutomu Ogata, Noriyuki Azuma, Tatsuhiko Urakami, and Akira Endo

Subjects

Male, Alu element, Biology, medicine.disease_cause, Microphthalmia, Frameshift mutation, Young Adult, Transactivation, Alu Elements, Genetics, medicine, Humans, Missense mutation, Eye Abnormalities, Child, Genetic Association Studies, Genetics (clinical), Gene Rearrangement, Homeodomain Proteins, Mutation, Anophthalmia, SOXB1 Transcription Factors, Infant, Newborn, Infant, Gene rearrangement, medicine.disease, Molecular biology, Phenotype, Gonadotropins, Pituitary, Female, sense organs

Abstract

Multiple mutations in SOX2 have been identified in patients with ocular anomalies and/or pituitary dysfunction. Here, we identified SOX2 abnormalities in nine patients. The molecular defects included one missense, one nonsense and four frameshift mutations, and three submicroscopic deletions involving SOX2. Three of the six mutations and all deletions were hitherto unreported. The breakpoints determined in one deletion were located within Alu repeats and accompanied by an overlap of 11 bp. Three of the six mutations encoded SOX2 proteins that lacked in vitro transactivation activity for the HESX1 promoter, whereas the remaining three generated proteins with ∼15-∼20% of transactivation activity. All cases manifested ocular anomalies of various severities, together with several complications including arachnoid cyst and hamartoma. There was no apparent correlation between the residual activity and clinical severity. The results indicate that molecular defects in SOX2 are highly variable and include Alu repeat-mediated genomic rearrangements. Our data provide further evidence for wide phenotypic variation of SOX2 abnormalities and the lack of genotype-phenotype correlation in patients carrying SOX2 lesions.

Published

2014

199. Identification and Functional Characterization of Two Novel NPR2 Mutations in Japanese Patients With Short Stature

Author

Tokuo Mukai, Yoshiya Ito, Susumu Yokoya, Toshiaki Tanaka, Tomonobu Hasegawa, Satoshi Narumi, Tsutomu Ogata, and Naoko Amano

Subjects

Male, medicine.medical_specialty, Endocrinology, Diabetes and Metabolism, DNA Mutational Analysis, Clinical Biochemistry, Long bone, Mutation, Missense, Dwarfism, Context (language use), Dominant-Negative Mutation, Biology, medicine.disease_cause, Biochemistry, Short stature, Endocrinology, Asian People, Internal medicine, Chlorocebus aethiops, medicine, Animals, Humans, Endochondral ossification, Genetic Association Studies, Mutation, Biochemistry (medical), Molecular Bases of Disease, medicine.disease, NPR2, Pedigree, medicine.anatomical_structure, Dysplasia, COS Cells, Female, medicine.symptom, Receptors, Atrial Natriuretic Factor

Abstract

C-type natriuretic peptide-natriuretic peptide receptor B (NPR-B) signaling is critical for endochondral ossification, which is responsible for longitudinal growth in limbs and vertebrae. Biallelic NPR2 mutations cause acromesomelic dysplasia, type Maroteaux, which is bone dysplasia characterized by severe short stature and short limbs. A monoallelic NPR2 mutation has been suggested to mildly impair long bone growth.The goal of this study was to identify and characterize NPR2 mutations among Japanese patients with short stature.We enrolled 101 unrelated Japanese patients with short stature. NPR2 and NPPC were sequenced, and the identified variants were characterized in vitro.In two subjects, we identified two novel heterozygous NPR2 mutations (R110C and Q417E) causing a loss of C-type natriuretic peptide-dependent cGMP generation capacities and having dominant-negative effects. R110C was defective in trafficking from the endoplasmic reticulum to the Golgi apparatus. In contrast, Q417E showed clear cell surface expression.We identified heterozygous NPR2 mutations in 2% of Japanese patients with short stature. Our in vitro findings indicate that NPR2 mutations have a dominant negative effect, and their dominant-negative mechanisms vary corresponding to the molecular pathogenesis of the mutations.

Published

2014

200. Hemodynamic assessment in a child with renovascular hypertension using time-resolved three-dimensional cine phase-contrast MRI

Author

Yasuo Takehara, Harumi Sakahara, Satoru Iwashima, Masataka Sugiyama, Tsutomu Ogata, Tetsuya Wakayama, Shuhei Yamashita, Takamichi Ishikawa, Kevin M. Johnson, and Oliver Wieben

Subjects

medicine.medical_specialty, Percutaneous, medicine.diagnostic_test, business.industry, Phase contrast microscopy, Hemodynamics, Magnetic resonance imaging, medicine.disease, Renovascular hypertension, law.invention, Stenosis, Renal angioplasty, law, Internal medicine, Renal blood flow, cardiovascular system, medicine, Cardiology, Radiology, Nuclear Medicine and imaging, cardiovascular diseases, Radiology, business, circulatory and respiratory physiology

Abstract

Renovascular hypertension (RVH) is an important cause of hypertension in children. It is essential to assess the hemodynamics of RVH lesions in detail. We herein report the case of a 9-year-old female with RVH caused by left renal artery stenosis in which the hemodynamics of the lesions were assessed with time-resolved three-dimensional cine phase-contrast MRI (3D cine PC MRI) with a vastly undersampled 3D radial projection imaging trajectory before and after percutaneous transluminal renal angioplasty (PTRA). The utility of 3D cine PC MRA for diagnosing RVH and evaluating the renal blood flow pre- and post-PTRA is presented. J. Magn. Reson. Imaging 2015;41:165–168. © 2014 Wiley Periodicals, Inc.

Published

2014