Isolation of cDNA for a novel human protein KNP-I that is homologous to the E. coli SCRP-27A protein from the autoimmune polyglandular disease type I (APECED) region of chromosome 21q22.3

Kentaro Nagamine; Jun Kudoh; Shinsei Minoshima; Kazuhiko Kawasaki; Shuichi Asakawa; Fumiaki Ito; Nobuyoshi Shimizu

doi:10.1006/bbrc.1996.1218

Isolation of cDNA for a novel human protein KNP-I that is homologous to the E. coli SCRP-27A protein from the autoimmune polyglandular disease type I (APECED) region of chromosome 21q22.3

Kentaro Nagamine
, Jun Kudoh
, Shinsei Minoshima
, Kazuhiko Kawasaki
, Shuichi Asakawa
, Fumiaki Ito
, Nobuyoshi Shimizu

Anthropology

Research output: Contribution to journal › Article › peer-review

19 Scopus citations

Abstract

We have isolated cDNA clones for a novel human protein KNP-I from fetal brain and bone marrow cDNA libraries. Northern blot analysis indicated that the KNP-I gene is ubiquitously expressed in various human tissues. Significant homology of the KNP-I protein with Escherichia coli anti-sigma cross-reacting protein (SCRP-27A) (44% identity) and zebrafish (Brachydanio rerio) es1 protein (49% identity) suggested that the KNP-I protein may be involved in a basic cellular function. Genomic sequencing revealed that the KNP-I gene consists of seven exons spanning 12 kb. Exon 5 was involved in alternative splicing. The KNP-I gene was mapped between D21S1460 and D21S25 on human chromosome 21q22.3, 26 kb distal to a Not I site of D21S1460. Thus, this novel KNP-I gene could be a candidate gene for autoimmune polyglandular disease type I (APECED) and other disorders mapped to this region.

Original language	English (US)
Pages (from-to)	608-616
Number of pages	9
Journal	Biochemical and Biophysical Research Communications
Volume	225
Issue number	2
DOIs	https://doi.org/10.1006/bbrc.1996.1218
State	Published - Aug 14 1996

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This output contributes to the following UN Sustainable Development Goals (SDGs)

SDG 3 Good Health and Well-being

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Biophysics
Biochemistry
Molecular Biology
Cell Biology

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10.1006/bbrc.1996.1218

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Nagamine, K., Kudoh, J., Minoshima, S., Kawasaki, K., Asakawa, S., Ito, F., & Shimizu, N. (1996). Isolation of cDNA for a novel human protein KNP-I that is homologous to the E. coli SCRP-27A protein from the autoimmune polyglandular disease type I (APECED) region of chromosome 21q22.3. Biochemical and Biophysical Research Communications, 225(2), 608-616. https://doi.org/10.1006/bbrc.1996.1218

@article{837ccef0d70342a9842deb883f1eef43,

title = "Isolation of cDNA for a novel human protein KNP-I that is homologous to the E. coli SCRP-27A protein from the autoimmune polyglandular disease type I (APECED) region of chromosome 21q22.3",

abstract = "We have isolated cDNA clones for a novel human protein KNP-I from fetal brain and bone marrow cDNA libraries. Northern blot analysis indicated that the KNP-I gene is ubiquitously expressed in various human tissues. Significant homology of the KNP-I protein with Escherichia coli anti-sigma cross-reacting protein (SCRP-27A) (44\% identity) and zebrafish (Brachydanio rerio) es1 protein (49\% identity) suggested that the KNP-I protein may be involved in a basic cellular function. Genomic sequencing revealed that the KNP-I gene consists of seven exons spanning 12 kb. Exon 5 was involved in alternative splicing. The KNP-I gene was mapped between D21S1460 and D21S25 on human chromosome 21q22.3, 26 kb distal to a Not I site of D21S1460. Thus, this novel KNP-I gene could be a candidate gene for autoimmune polyglandular disease type I (APECED) and other disorders mapped to this region.",

author = "Kentaro Nagamine and Jun Kudoh and Shinsei Minoshima and Kazuhiko Kawasaki and Shuichi Asakawa and Fumiaki Ito and Nobuyoshi Shimizu",

note = "Funding Information: The authors thank Drs. H. Ichikawa and M. Ohki (National Cancer Center Research Institute, Tokyo, Japan) for the NotI linking clones, Dr. E. Bakker (Leiden University, Leiden, Netherlands) for the D21S25 marker (10.2), and Drs. J. Hazan and J. Weissenbach (Genethon, Evry, France) for the D21S154 marker (IP21K443). This work was supported in part by Grants in Aid for Creative Basic Research (Human Genome Program), Scientific Research on Priority Areas, and Scientific Research from the Ministry of Education, Science and Culture of Japan; the Special Coordination Funds for Promoting Science and Technology from the Science and Technology Agency (STA) of Japan; and Fund for Human Genome Sequencing Project from the Japan Information Center of Science and Technology (JICST).",

year = "1996",

month = aug,

day = "14",

doi = "10.1006/bbrc.1996.1218",

language = "English (US)",

volume = "225",

pages = "608--616",

journal = "Biochemical and Biophysical Research Communications",

issn = "0006-291X",

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number = "2",

}

Nagamine, K, Kudoh, J, Minoshima, S, Kawasaki, K, Asakawa, S, Ito, F & Shimizu, N 1996, 'Isolation of cDNA for a novel human protein KNP-I that is homologous to the E. coli SCRP-27A protein from the autoimmune polyglandular disease type I (APECED) region of chromosome 21q22.3', Biochemical and Biophysical Research Communications, vol. 225, no. 2, pp. 608-616. https://doi.org/10.1006/bbrc.1996.1218

Isolation of cDNA for a novel human protein KNP-I that is homologous to the E. coli SCRP-27A protein from the autoimmune polyglandular disease type I (APECED) region of chromosome 21q22.3. / Nagamine, Kentaro; Kudoh, Jun; Minoshima, Shinsei et al.
In: Biochemical and Biophysical Research Communications, Vol. 225, No. 2, 14.08.1996, p. 608-616.

Research output: Contribution to journal › Article › peer-review

TY - JOUR

T1 - Isolation of cDNA for a novel human protein KNP-I that is homologous to the E. coli SCRP-27A protein from the autoimmune polyglandular disease type I (APECED) region of chromosome 21q22.3

AU - Nagamine, Kentaro

AU - Kudoh, Jun

AU - Minoshima, Shinsei

AU - Kawasaki, Kazuhiko

AU - Asakawa, Shuichi

AU - Ito, Fumiaki

AU - Shimizu, Nobuyoshi

N1 - Funding Information: The authors thank Drs. H. Ichikawa and M. Ohki (National Cancer Center Research Institute, Tokyo, Japan) for the NotI linking clones, Dr. E. Bakker (Leiden University, Leiden, Netherlands) for the D21S25 marker (10.2), and Drs. J. Hazan and J. Weissenbach (Genethon, Evry, France) for the D21S154 marker (IP21K443). This work was supported in part by Grants in Aid for Creative Basic Research (Human Genome Program), Scientific Research on Priority Areas, and Scientific Research from the Ministry of Education, Science and Culture of Japan; the Special Coordination Funds for Promoting Science and Technology from the Science and Technology Agency (STA) of Japan; and Fund for Human Genome Sequencing Project from the Japan Information Center of Science and Technology (JICST).

PY - 1996/8/14

Y1 - 1996/8/14

N2 - We have isolated cDNA clones for a novel human protein KNP-I from fetal brain and bone marrow cDNA libraries. Northern blot analysis indicated that the KNP-I gene is ubiquitously expressed in various human tissues. Significant homology of the KNP-I protein with Escherichia coli anti-sigma cross-reacting protein (SCRP-27A) (44% identity) and zebrafish (Brachydanio rerio) es1 protein (49% identity) suggested that the KNP-I protein may be involved in a basic cellular function. Genomic sequencing revealed that the KNP-I gene consists of seven exons spanning 12 kb. Exon 5 was involved in alternative splicing. The KNP-I gene was mapped between D21S1460 and D21S25 on human chromosome 21q22.3, 26 kb distal to a Not I site of D21S1460. Thus, this novel KNP-I gene could be a candidate gene for autoimmune polyglandular disease type I (APECED) and other disorders mapped to this region.

AB - We have isolated cDNA clones for a novel human protein KNP-I from fetal brain and bone marrow cDNA libraries. Northern blot analysis indicated that the KNP-I gene is ubiquitously expressed in various human tissues. Significant homology of the KNP-I protein with Escherichia coli anti-sigma cross-reacting protein (SCRP-27A) (44% identity) and zebrafish (Brachydanio rerio) es1 protein (49% identity) suggested that the KNP-I protein may be involved in a basic cellular function. Genomic sequencing revealed that the KNP-I gene consists of seven exons spanning 12 kb. Exon 5 was involved in alternative splicing. The KNP-I gene was mapped between D21S1460 and D21S25 on human chromosome 21q22.3, 26 kb distal to a Not I site of D21S1460. Thus, this novel KNP-I gene could be a candidate gene for autoimmune polyglandular disease type I (APECED) and other disorders mapped to this region.

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U2 - 10.1006/bbrc.1996.1218

DO - 10.1006/bbrc.1996.1218

M3 - Article

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AN - SCOPUS:0030583302

SN - 0006-291X

VL - 225

SP - 608

EP - 616

JO - Biochemical and Biophysical Research Communications

JF - Biochemical and Biophysical Research Communications

IS - 2

ER -

Isolation of cDNA for a novel human protein KNP-I that is homologous to the E. coli SCRP-27A protein from the autoimmune polyglandular disease type I (APECED) region of chromosome 21q22.3

Abstract

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