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Fetal Therapy Model of Myelomeningocele with Three-Dimensional Skin Using Amniotic Fluid Cell-Derived Induced Pluripotent Stem Cells

Author: Aikou Okamoto
Akihiro Umezawa
Haruhiko Sago
Hidenori Akutsu
Jurii Karibe
Kazuhiro Kajiwara
Kohji Okamura
Norimasa Ihara
Osamu Samura
Seiji Wada
Shuji Takada
Tomohiro Tanemoto
Tomoyuki Kawasaki
Yoshie Oishi
Yu Ikemoto
Publication venue: 'Elsevier BV'
Publication date: 01/06/2017
Field of study

Myelomeningocele (MMC) is a congenital disease without genetic abnormalities. Neurological symptoms are irreversibly impaired after birth, and no effective treatment has been reported to date. Only surgical repairs have been reported so far. In this study, we performed antenatal treatment of MMC with an artificial skin using induced pluripotent stem cells (iPSCs) generated from a patient with Down syndrome (AF-T21-iPSCs) and twin-twin transfusion syndrome (AF-TTTS-iPSCs) to a rat model. We manufactured three-dimensional skin with epidermis generated from keratinocytes derived from AF-T21-iPSCs and AF-TTTS-iPSCs and dermis of human fibroblasts and collagen type I. For generation of epidermis, we developed a protocol using Y-27632 and epidermal growth factor. The artificial skin was successfully covered over MMC defect sites during pregnancy, implying a possible antenatal surgical treatment with iPSC technology

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ATM Regulates Adipocyte Differentiation and Contributes to Glucose Homeostasis

Author: Akio Yasuda
Hatsume Uno
Jinhua Piao
Masataka Sugimoto
Masatoshi Takagi
Norimasa Ihara
Rina Nishi
Saori Kakei
Sayaka Kanai
Setsuko Hasegawa
Shuki Mizutani
Takayoshi Suganami
Toshiaki Shimizu
Yasutomi Kamei
Yoshifumi Tamura
Yoshihiro Ogawa
Publication venue: 'Elsevier BV'
Publication date: 01/02/2015
Field of study

Ataxia-telangiectasia (A-T) patients occasionally develop diabetes mellitus. However, only limited attempts have been made to gain insight into the molecular mechanism of diabetes mellitus development in A-T patients. We found that Atm−/− mice were insulin resistant and possessed less subcutaneous adipose tissue as well as a lower level of serum adiponectin than Atm+/+ mice. Furthermore, in vitro studies revealed impaired adipocyte differentiation in Atm−/− cells caused by the lack of induction of C/EBPα and PPARγ, crucial transcription factors involved in adipocyte differentiation. Interestingly, ATM was activated by stimuli that induced differentiation, and the binding of ATM to C/EBPβ and p300 was involved in the transcriptional regulation of C/EBPα and adipocyte differentiation. Thus, our study sheds light on the poorly understood role of ATM in the pathogenesis of glucose intolerance in A-T patients and provides insight into the role of ATM in glucose metabolism

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