Yoshifumi Ogiso scite author profile

We describe four families with affected siblings showing unique clinical features: early-onset (before 1 year of age) progressive diffuse brain atrophy with regression, postnatal microcephaly, postnatal growth retardation, muscle weakness/atrophy, and respiratory failure. By whole-exome sequencing, we identified biallelic TBCD mutations in eight affected individuals from the four families. TBCD encodes TBCD (tubulin folding co-factor D), which is one of five tubulin-specific chaperones playing a pivotal role in microtubule assembly in all cells. A total of seven mutations were found: five missense mutations, one nonsense, and one splice site mutation resulting in a frameshift. In vitro cell experiments revealed the impaired binding between most mutant TBCD proteins and ARL2, TBCE, and β-tubulin. The in vivo experiments using olfactory projection neurons in Drosophila melanogaster indicated that the TBCD mutations caused loss of function. The wide range of clinical severity seen in this neurodegenerative encephalopathy may result from the residual function of mutant TBCD proteins. Furthermore, the autopsied brain from one deceased individual showed characteristic neurodegenerative findings: cactus and somatic sprout formations in the residual Purkinje cells in the cerebellum, which are also seen in some diseases associated with mitochondrial impairment. Defects of microtubule formation caused by TBCD mutations may underlie the pathomechanism of this neurodegenerative encephalopathy.

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An improved intravesical model using human bladder cancer cell lines to optimize gene and other therapies

Watanabe

Shinohara

Sazawa

et al. 2000

Cancer Gene Ther

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Orthotopic implantation of human bladder cancer cells into immunodeficient mice is an important tool for studying the biology and effects of therapy. Nevertheless, the incidence of tumor implantation and growth by transurethral instillation of the human bladder cancer cells into murine bladders has been low or not reproducible. However, using a modified intravesical technique and the human bladder cancer cell lines, KU -7 and UM -UC -2, we have been able to obtain a high and reproducible incidence of superficial bladder tumors. Furthermore, intravesical administration of the LacZ adenovirus vector resulted in significant -galactosidase expression in these bladder tumors as well as the normal urothelium, which was associated with the removal of the glycosoaminoglycan layer. Because this modified technique produces a high incidence of superficial human tumor growth and allows the efficacy of gene transfer to be evaluated, it should be a useful model for the study of intravesical gene therapy for human bladder cancer. Cancer Gene Therapy ( 2000 ) 7, 1575 ± 1580

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Suppression of Pancreatic Cancer by the Dominant NegativerasMutant, N116Y

Shichinohe¹,

Senmaru²,

Furuuchi³

et al. 1996

Journal of Surgical Research

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Induction of Apoptosis by a Dominant Negative H-RAS Mutant (116Y) in K562 Cells

Sakai

Ogiso

Fujita

et al. 1994

Experimental Cell Research

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Fetal hydrops associated with congenital pulmonary myofibroblastic tumor

Horikoshi

Kikuchi

Matsumoto

et al. 2005

J of Obstet and Gynaecol

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We report on a fetus with a congenital pulmonary myofibroblastic tumor, the prenatal detection of which with imaging modalities has not been reported up until now. A 32-year-old woman was referred to our hospital at 29 weeks' gestation because of severe fetal hydrops. Sonograms and magnetic resonance imaging showed a large solid tumor in the left thorax. The fetus died in utero the next day. Autopsy confirmed that the tumor was confined to the lower lobe of the left lung, and circulatory insufficiency from compression by the tumor was considered to be the cause of fetal hydrops and demise. Histologic examination revealed that the tumor was composed of uniform short spindle cells with no atypia and a large number of vessels. In addition, with immunohistochemical studies, the tumor cells were stained for calponin but not for cluster differentiation (CD)-31, CD-34, alpha-smooth muscle actin or S-100.

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Yoshifumi Ogiso

Biallelic TBCD Mutations Cause Early-Onset Neurodegenerative Encephalopathy

An improved intravesical model using human bladder cancer cell lines to optimize gene and other therapies

Suppression of Pancreatic Cancer by the Dominant NegativerasMutant, N116Y

Induction of Apoptosis by a Dominant Negative H-RAS Mutant (116Y) in K562 Cells

Fetal hydrops associated with congenital pulmonary myofibroblastic tumor

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