7 results on '"Shinobu, Ida"'
Search Results
2. Renal function in short‐statured children born small for gestational age and treated with growth hormone
- Author
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Yuri Etani, Yasuko Shoji, Shinobu Ida, Masanobu Kawai, and Mikiko Koizumi
- Subjects
Pediatrics ,medicine.medical_specialty ,Renal function ,Gestational Age ,030204 cardiovascular system & hematology ,Kidney ,Growth hormone ,Short stature ,03 medical and health sciences ,chemistry.chemical_compound ,0302 clinical medicine ,030225 pediatrics ,Humans ,Medicine ,Child ,reproductive and urinary physiology ,Rank correlation ,Creatinine ,Human Growth Hormone ,business.industry ,Infant, Newborn ,Anthropometry ,medicine.disease ,Body Height ,chemistry ,Growth Hormone ,Infant, Small for Gestational Age ,Pediatrics, Perinatology and Child Health ,Gestation ,Small for gestational age ,medicine.symptom ,business - Abstract
BACKGROUND Children born small for gestational age (SGA), particularly when associated with an extremely low birthweight (ELBW), have a higher risk of renal dysfunction. Growth hormone (GH) treatment is used to treat short-statured children born SGA; however, its effects on renal function remain elusive, especially in those born SGA with ELBW. METHODS Short-statured children born SGA (N = 42) were included. Subjects were subdivided into two groups based on their birthweight: the ELBW group (N = 15) with a birthweight of
- Published
- 2021
3. Growth hormone treatment for extremely low birthweight children born small for gestational age
- Author
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Masanobu Kawai, Takatoshi Maeyama, Yasuko Shoji, Yuri Etani, Shinobu Ida, and Shinsuke Onuma
- Subjects
medicine.medical_specialty ,Birth weight ,Gestational Age ,030204 cardiovascular system & hematology ,Growth hormone ,Short stature ,03 medical and health sciences ,Child Development ,0302 clinical medicine ,Japan ,030225 pediatrics ,Internal medicine ,Birth Weight ,Humans ,Medicine ,Human Growth Hormone ,business.industry ,Infant, Newborn ,Infant ,medicine.disease ,Body Height ,Growth hormone treatment ,Low birth weight ,Endocrinology ,Child, Preschool ,Infant, Small for Gestational Age ,Pediatrics, Perinatology and Child Health ,Gh treatment ,Small for gestational age ,medicine.symptom ,business - Abstract
The effectiveness of growth hormone (GH) treatment for height gain in short-stature children born small for gestational age (SGA) with extremely low birthweight (ELBW; birthweight1,000 g) remains largely unknown.In study 1, 35 prepubertal Japanese children born SGA with ELBW were categorized into three groups based on the presence or absence of catch-up growth by age 3 (CU(+) and CU(-), respectively) and GH treatment (GH(+) and GH(-), respectively). Height standard deviation (SD) scores (HT-SDS) in the CU-/GH+ group (n = 19) were compared with those in the age-matched CU+/GH- (n = 9) and CU-/GH- groups (n = 7). In study 2, 66 prepubertal Japanese SGA children treated with GH were divided into three groups by birthweight:1,000 g (n = 19), 1,000-2,000 g (n = 20), and2,000 g (n = 27). Changes in HT-SDS during the initial 3 years of GH treatment were compared among the three groups.In study 1, the mean HT-SDS in the CU-/GH+ group (-1.15 SD) was similar to that in the CU+/GH- group (-1.39 SD) but higher than that in the CU-/GH- group (-2.24 SD). In study 2, GH achieved a height gain of +1.62 SD in the ELBW group, which was similar to that in the other groups (1,000-2,000 g: +1.46 SD,2,000 g: +1.53 SD).Growth hormone treatment in short-stature children born SGA with ELBW increased HT-SDS, which was similar to that in SGA children born with a birthweight ≥1,000 g. These results indicate that GH treatment may be an effective approach to promote adequate growth recovery for short-stature children born SGA with ELBW.
- Published
- 2021
4. Policy statement of enteral nutrition for preterm and very low birthweight infants
- Author
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Nobuo Yoshiike, Shinobu Ida, Toshihiro Ohura, Akihide Sugiyama, Kazue Kawakami, Daisuke Tanaka, Yuko Bito, Chiharu Tsutsumi, Akihisa Okumura, Katsumi Mizuno, Sotaro Mushiake, Toru Kikuchi, Mitsuyoshi Suzuki, Yoshio Hanawa, Kimitaka Takitani, Kazuo Okada, Motoichiro Sakurai, Masanobu Kawai, Mikako Inokuchi, Hiroko Kodama, Mitsuhiko Hara, Hiroaki Inomata, Tatsuya Oguni, Setsuko Ito, Shigetaka Sugihara, Keiichi Uchida, and Toshiaki Shimizu
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medicine.medical_specialty ,Medical staff ,Human milk bank ,Mothers ,030204 cardiovascular system & hematology ,Breast milk ,Guidelines ,03 medical and health sciences ,0302 clinical medicine ,fluids and secretions ,Enteral Nutrition ,Japan ,030225 pediatrics ,medicine ,donor human milk ,Humans ,Infant, Very Low Birth Weight ,Infant Nutritional Physiological Phenomena ,human milk bank ,Milk, Human ,Obstetrics ,business.industry ,Infant, Newborn ,food and beverages ,human milk ,Infant ,Guideline ,Human milk fortifier ,Parenteral nutrition ,Milk Banks ,Pediatrics, Perinatology and Child Health ,exclusive human milk-based diet ,Female ,business ,Infant, Premature - Abstract
For preterm and very low birthweight infants, the mother’s own milk is the best nutrition. Based on the latest information for mothers who give birth to preterm and very low birthweight infants, medical staff should encourage and assist mothers to pump or express and provide their own milk whenever possible.If the supply of maternal milk is insufficient even though they receive adequate support, or the mother’s own milk cannot be given to her infant for any reason, donor human milk should be used.Donors who donate their breast milk need to meet the Guideline of the Japan Human Milk Bank Association.Donor human milk should be provided according to the medical needs of preterm and very low birthweight infants, regardless of their family’s financial status.In the future, it will be necessary to create a system to supply an exclusive human milk‐based diet (EHMD), consisting of human milk with the addition of a human milk‐derived human milk fortifier, to preterm and very low birthweight infants.
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- 2020
5. Male assignment in 5α‐reductase type 2 deficiency with female external genitalia
- Author
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Ayako Konishi, Yuri Etani, Shinobu Ida, Futoshi Matsui, and Masanobu Kawai
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Male ,Hypospadias ,Steroid Metabolism, Inborn Errors ,medicine.medical_specialty ,Disorder of Sex Development, 46,XY ,business.industry ,Female external genitalia ,Disorders of Sex Development ,5α reductase ,Endocrinology ,3-Oxo-5-alpha-Steroid 4-Dehydrogenase ,SRD5A2 ,Internal medicine ,Dihydrotestosterone ,Mutation ,Pediatrics, Perinatology and Child Health ,Humans ,Medicine ,Female ,Genitalia ,business ,medicine.drug - Published
- 2021
6. Esophago-gastric motility and nutritional management in a child with ATR-X syndrome
- Author
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Takahiko Wada, Michinobu Ohno, Kaori Sato, Masataka Takahashi, Shinobu Ida, Yutaka Kanamori, Hisayoshi Kawahara, Katsuhiro Arai, Toshihiko Watanabe, and Yasushi Fuchimoto
- Subjects
medicine.medical_specialty ,Gastric volvulus ,business.industry ,medicine.medical_treatment ,Gastric motility ,Aspiration pneumonia ,medicine.disease ,Gastrostomy ,Gastroenterology ,Gastropexy ,Esophageal motility disorder ,Internal medicine ,Pediatrics, Perinatology and Child Health ,medicine ,Vomiting ,medicine.symptom ,Gastrointestinal function ,business - Abstract
X-linked alpha thalassemia mental retardation (ATR-X) syndrome is an X-linked recessive disorder that often involves gastrointestinal symptoms. Aspiration pneumonia related to gastroesophageal reflux has been reported as the major cause of death, but gastrointestinal function has not been well investigated. The present report describes a child with ATR-X syndrome who suffered from periodical episodes of refractory vomiting. We investigated the function of upper alimentary tract and found that esophago-gastric dysmotility and severe gastric volvulus were the major causes of gastrointestinal symptoms. This child was surgically treated with anterior gastropexy and jejunal alimentation through gastrostomy, and the symptoms were relieved with good weight gain. This report may provide insight into the gastrointestinal function and nutritional management in children with ATR-X syndrome.
- Published
- 2014
7. Prevention of Neonatal HBV Infection with the Combination of HBIG and HBV Vaccine and Its Long-Term Efficacy in Infants Born to HBeAg Positive HBV Carrier Mothers
- Author
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Hitoshi Tajiri, Saburo Kimura, Hyakuji Yabuuchi, Shinobu Ida, Osamu Nose, Kazuo Shimizu, and Kazunori Miki
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Viral Hepatitis Vaccines ,HBEAG POSITIVE ,medicine.medical_specialty ,business.industry ,Group ii ,Infant, Newborn ,Immunoglobulins ,virus diseases ,Hbv carrier ,Hepatitis B ,Gastroenterology ,digestive system diseases ,Titer ,Pregnancy ,Internal medicine ,Carrier State ,Pediatrics, Perinatology and Child Health ,Immunology ,medicine ,Humans ,Female ,Hepatitis B Vaccines ,business ,Maternal-Fetal Exchange ,Immunization Schedule - Abstract
Seventy-three infants born to HBeAg positive HBV carrier mothers were protected from neonatal HBV infection with our standard prevention schedule consisting of two doses of HBIG (0,2 mo) and three doses of HBV vaccine (2, 3, 5 mo). In 62 infants who successfully responded to HBV vaccine with a titer of anti-HBs greater than 2(3), anti-HBs titer was monitored for as long as 48 months (25.6 +/- 11.0 mo) and found to decrease as follows: 5.1 +/- 1.7 at 12 mo., 4.5 +/- 1.8 at 18 mo., 4.2 +/- 1.8 at 24 mo., 4.0 +/- 1.6 at 30 mo., 3.7 +/- 1.7 at 36 mo., 3.2 +/- 2.0 at 48 mo. During the follow-up period, eight HBV events (11.9%) were demonstrated: one case showed an increase of anti-HBs, three showed a reappearance of anti-HBc alone, three showed a reappearance of anti-HBc with increase of anti-HBs, and one became a chronic HBV carrier. All infants were further divided into three groups by their maximal response of anti-HBs to HBV vaccine: Group I (greater than or equal to 2(6)), Group II (2(3)-2(5)), and Group III (2(2) greater than or equal to). Group I sustained a higher titer from 12 to 30 months of age and had less HBV events than G-II and G-III. Our study suggests that acquisition of a high titer of anti-HBs is important in long-term prevention of HBV infection as well as in the neonatal period in infants born to HBeAg positive HBV carrier mothers.
- Published
- 1989
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