Hiromitsu Okano scite author profile

Hiromitsu Okano

5Publications

159Citation Statements Received

39Citation Statements Given

How they've been cited

398

153

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Affiliations

Kyushu University, National Hospital Organization Kyushu Cancer Center, Niigata University

Publications

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Establishment and characterization of an erythropoietin-dependent subline, UT-7/Epo, derived from human leukemia cell line, UT-7

Komatsu

Yamamoto

Fujita

et al. 1993

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UT-7 is a human leukemic cell line capable of growing in interleukin-3 (IL-3), granulocyte/macrophage colony-stimulating factor (GM-CSF), or erythropoietin (Epo) (Komatsu et al, Cancer Res 51:341, 1991). To study the effect of Epo on proliferation and differentiation of UT-7, we maintained the UT-7 cell culture for more than 6 months in the presence of Epo. As a result, a subline, UT-7/Epo, was established. The growth of UT-7/Epo could be supported by Epo but not by GM-CSF or IL-3. UT- 7/Epo showed a greater level of heme content and ratio of benzidine- positive staining cells than did UT-7. Butyric acid promoted the synthesis of hemoglobin in UT-7/Epo, but not UT-7. Further, the mRNA concentrations of the c-myb oncogene and GM-CSF receptor beta-subunit were decreased substantially in UT-7/Epo cells. These findings showed that UT-7/Epo cells had progressed further in erythroid development than UT-7 cells, and suggested that long-term culture in Epo had promoted this differentiation. Whereas availability of the Epo receptor (Epo-R) for binding of Epo was reduced in UT-7/Epo cells compared with UT-7 cells, the Epo-R showed a similar affinity for Epo. This observation suggested that change(s) in postreceptor signaling step might be involved in the establishment and maintenance of the UT-7/Epo phenotype.

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Homozygous deletions and point mutations of the Ikaros gene in γ-ray-induced mouse thymic lymphomas

et al. 1999

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Our previous genome-wide analysis of allelic loss for thymic lymphomas that were induced by g-irradiation in F 1 hybrid mice between BALB/c and MSM strains suggested the centromeric region on chromosome 11 as a site harboring a tumor suppressor gene. Interestingly, to this region the mouse Ikaros gene was mapped which was postulated to participate in oncogenic process from the study of Ikaros knockout mice. Here we show ®ne allelic loss mapping in the vicinity of Ikaros in 191 lymphomas, indicating that the critical region of allelic loss was centered at the Ikaros locus. PCR analysis revealed that nine lymphomas failed to give PCR-ampli®cation for either of two exon primer pairs, indicative of homozygous deletion. Six and ®ve mutations were detected in the N-terminal zinc ®nger domain and the activation domain of Ikaros, respectively, and six of the eleven were frameshift or nonsense mutations that resulted in truncation of Ikaros protein. The results strongly suggest a direct role for Ikaros in development of mouse thymic lymphomas. This provides the experimental basis for further analysis of Ikaros mutations in human cancer.

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Establishment and characterization of an erythropoietin-dependent subline, UT-7/Epo, derived from human leukemia cell line, UT-7

et al. 1993

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Current status of nanostructured tungsten-based materials development

et al. 2014

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Content of reticulocyte hemoglobin is a reliable tool for determining iron deficiency in dialysis patients

Tsuchiya

Okano²,

Teramura³

et al. 2003

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Hiromitsu Okano

Establishment and characterization of an erythropoietin-dependent subline, UT-7/Epo, derived from human leukemia cell line, UT-7

Homozygous deletions and point mutations of the Ikaros gene in γ-ray-induced mouse thymic lymphomas

Establishment and characterization of an erythropoietin-dependent subline, UT-7/Epo, derived from human leukemia cell line, UT-7

Current status of nanostructured tungsten-based materials development

Content of reticulocyte hemoglobin is a reliable tool for determining iron deficiency in dialysis patients

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