Your search keyword '"Kuraoka, Isao"' showing total 6 results

1. Mutation spectra of the BRCA1/2 genes in human breast and ovarian cancer and germline.

Author

Koi, Yumiko, Watanabe, Arisa, Kawasaki, Akari, Ideo, Satomi, Matsutani, Nao, Miyashita, Kaname, Shioi, Seijiro, Tokunaga, Eriko, Shimokawa, Mototsugu, Nakatsu, Yoshimichi, Kuraoka, Isao, and Oda, Shinya

Subjects

BRCA genes, BREAST, GERM cells, GENETIC mutation, MISSENSE mutation, SOMATIC cells

Abstract

Annotating genomic sequence alterations is sometimes a difficult decision, particularly in missense variants with uncertain pathogenic significance and also in those presumed as germline pathogenic variants. We here suggest that mutation spectrum may also be useful for judging them. From the public databases, 982 BRCA1/1861 BRCA2 germline missense variants and 294 BRCA1/420 BRCA2 somatic missense variants were obtained. We then compared their mutation spectra, i.e., the frequencies of two transition‐ and four transversion‐type mutations, in each category. Intriguingly, in BRCA1 variants, A:T to C:G transversion, which was relatively frequent in the germline, was extremely rare in somatic, particularly breast cancer, cells (p =.03). Conversely, A:T to T:A transversion was most infrequent in the germline, but not rare in somatic cells. Thus, BRCA1 variants with A:T to T:A transversion may be suspected as somatic, and those with A:T to C:G as being in the germline. These tendencies of mutation spectrum may also suggest the biological and chemical origins of the base alterations. On the other hand, unfortunately, variants of uncertain significance (VUS) were not distinguishable by mutation spectrum. Our findings warrant further and more detailed studies. [ABSTRACT FROM AUTHOR]

Published

2024

2. Inosine-specific ribonuclease activity of natural variants of human endonuclease V.

Author

Kim, Jung In, Tohashi, Kosuke, Iwai, Shigenori, and Kuraoka, Isao

Subjects

INOSINE, RIBONUCLEASES, ENDONUCLEASES, HYDROLYSIS, NITROSATION

Abstract

Adenine bases in DNA, RNA, and nucleotides are deaminated during normal metabolism via hydrolytic and nitrosative reactions. In RNA, the deaminated product inosine is resolved by human endonuclease V, and mice deficient in this enzyme are cancer-prone. We have now produced, purified, and characterized naturally occurring variants of human endonuclease V (V29I, R112Q, K114R, H141Y, and D201N). We found that H141Y, but not other variants, is catalytically impaired, suggesting that individuals homozygous for H141Y may be predisposed to disease. [ABSTRACT FROM AUTHOR]

Published

2016

3. Xeroderma pigmentosum group F protein binds to Eg5 and is required for proper mitosis: implications for XP-F and XFE.

Author

Tan, Li Jing, Saijo, Masafumi, Kuraoka, Isao, Narita, Takashi, Takahata, Chiaki, Iwai, Shigenori, and Tanaka, Kiyoji

Subjects

XERODERMA pigmentosum, PROTEIN binding, MITOSIS, DNA repair, ENDONUCLEASES, GENETIC mutation, LABORATORY rodents

Abstract

The xeroderma pigmentosum group F-cross-complementing rodent repair deficiency group 1 (XPF-ERCC1) complex is a structure-specific endonuclease involved in nucleotide excision repair (NER) and interstrand cross-link (ICL) repair. Patients with XPF mutations may suffer from two forms of xeroderma pigmentosum (XP): XP-F patients show mild photosensitivity and proneness to skin cancer but rarely show any neurological abnormalities, whereas XFE patients display symptoms of severe XP symptoms, growth retardation and accelerated aging. Xpf knockout mice display accelerated aging and die before weaning. These results suggest that the XPF-ERCC1 complex has additional functions besides NER and ICL repair and is essential for development and growth. In this study, we show a partial colocalization of XPF with mitotic spindles and Eg5. XPF knockdown in cells led to an increase in the frequency of abnormal nuclear morphology and mitosis. Similarly, the frequency of abnormal nuclei and mitosis was increased in XP-F and XFE cells. In addition, we showed that Eg5 enhances the action of XPF-ERCC1 nuclease activity. Taken together, these results suggest that the interaction between XPF and Eg5 plays a role in mitosis and DNA repair and offer new insights into the pathogenesis of XP-F and XFE. [ABSTRACT FROM AUTHOR]

Published

2012

4. Mutant Cockayne syndrome group B protein inhibits repair of DNA topoisomerase I-DNA covalent complex.

Author

Horibata, Katsuyoshi, Saijo, Masafumi, Bay, Mui N., Lan, Li, Kuraoka, Isao, Brooks, Philip J., Honma, Masamitsu, Nohmi, Takehiko, Yasui, Akira, and Tanaka, Kiyoji

Subjects

COCKAYNE syndrome, GENETIC mutation, DNA topoisomerases, PHOTOSENSITIZATION, TRANSPOSONS, MESSENGER RNA, DNA repair

Abstract

Two UV-sensitive syndrome patients who have mild photosensitivity without detectable somatic abnormalities lack detectable Cockayne syndrome group B (CSB) protein because of a homozygous null mutation in the CSB gene. In contrast, mutant CSB proteins are produced in CS-B patients with the severe somatic abnormalities of Cockayne syndrome and photosensitivity. It is known that the piggyBac transposable element derived 3 is integrated within the CSB intron 5, and that CSB-piggyBac transposable element derived 3 fusion (CPFP) mRNA is produced by alternative splicing. We found that CPFP or truncated CSB protein derived from CPFP mRNA was stably produced in CS-B patients, and that wild-type CSB, CPFP, and truncated CSB protein interacted with DNA topoisomerase I. We also found that CPFP inhibited repair of a camptothecin-induced topoisomerase I-DNA covalent complex. The inhibition was suppressed by the presence of wild-type CSB, consistent with the autosomal recessive inheritance of Cockayne syndrome. These results suggested that reduced repair of a DNA topoisomerase I-DNA covalent complex because of truncated CSB proteins is involved in the pathogenesis of CS-B. [ABSTRACT FROM AUTHOR]

Published

2011

5. DNA conformation-dependent activities of human mitochondrial RNA polymerase.

Author

Fukuoh, Atsushi, Ohgaki, Kippei, Hatae, Hinako, Kuraoka, Isao, Aoki, Yoshimasa, Uchiumi, Takeshi, Jacobs, Howard T., and Kang, Dongchon

Subjects

DNA, NUCLEIC acids, RNA polymerases, MITOCHONDRIAL DNA, CARRIER proteins

Abstract

Mitochondrial RNA polymerase (POLRMT) is a core protein for mitochondrial DNA (mtDNA) transcription. In addition, POLRMT is assumed to be involved in replication, although its exact role is not yet clearly elucidated. We have found novel properties of human POLRMT using a reconstituted transcription system. Various lengths of RNA molecules were synthesized from templates even without a defined promoter sequence, when we used supercoiled circular double-stranded DNA as a template. This promoter-independent activity was as strong as the promoter-dependent one. Promoter-independent DNA conformation-dependent transcription required TFB2M. On supercoiled templates, the promoter-independent activity was strongly suppressed by a putatively physiological amount of TFAM, while promoter-dependent transcription was inhibited to a lesser extent. These different inhibition patterns by TFAM may be important for prevention of random RNA synthesis in vivo. Promoter-independent activity was also observed on relaxed circular single-stranded DNA, where its activity no longer required TFB2M. RNA synthesis on single-stranded DNA was weakly suppressed by a putatively physiological amount of TFAM but restored by the addition of mitochondrial single-stranded DNA binding protein. We suggest that these properties of POLRMT could explain the characteristic features of mammalian mtDNA transcription and replication. [ABSTRACT FROM AUTHOR]

Published

2009

6. Implications of the zinc-finger motif found in the DNA-binding domain of the human XPA protein.

Author

Morita, Eugene H., Ohkubo, Tadayasu, Kuraoka, Isao, Shirakawa, Masahiro, Tanaka, Kiyoji, and Morikawa, Kosuke

Published

1996