The Drosophila ortholog of breast cancer metastasis suppressor gene, dBrms1, is critical for developmental timing through regulating ecdysone signaling

Shilin Song; Yuan Yuan; Jinfeng Lu; Qi Li; Zuoyan Zhu; Qichang Fan; Youfang Xue; Zhi Chun Lai; Wenxia Zhang

doi:10.1016/j.ydbio.2013.05.012

The Drosophila ortholog of breast cancer metastasis suppressor gene, dBrms1, is critical for developmental timing through regulating ecdysone signaling

Shilin Song, Yuan Yuan, Jinfeng Lu, Qi Li, Zuoyan Zhu, Qichang Fan, Youfang Xue, Zhi Chun Lai, Wenxia Zhang

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

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Abstract

BRMS1 was first discovered as a human breast carcinoma metastasis suppressor gene. However, the mechanism of BRMS1 in tumor metastasis and its developmental role remain unclear. In this paper, we first report the identification of the Drosophila ortholog of human BRMS1, dBrms1. Through a genetic approach, the role of dBrms1 during development has been investigated. We found that dBrms1 is an essential gene and loss of dBrms1 function results in lethality at early developmental stages. dBrms1mutants displayed phenotypes such as developmental delay and failure to initiate metamorphosis. Further analysis suggests that these phenotypes are contributed by defective ecdysone signaling and expression of target genes of the ecdysone pathway. Therefore, dBrms1 is required for growth control by acting as a modulator of ecdysone signaling in Drosophila and is required for metamorphosis for normal development.

Original language	English (US)
Pages (from-to)	344-350
Number of pages	7
Journal	Developmental biology
Volume	380
Issue number	2
DOIs	https://doi.org/10.1016/j.ydbio.2013.05.012
State	Published - Aug 15 2013

All Science Journal Classification (ASJC) codes

Molecular Biology
Developmental Biology
Cell Biology

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10.1016/j.ydbio.2013.05.012

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title = "The Drosophila ortholog of breast cancer metastasis suppressor gene, dBrms1, is critical for developmental timing through regulating ecdysone signaling",

abstract = "BRMS1 was first discovered as a human breast carcinoma metastasis suppressor gene. However, the mechanism of BRMS1 in tumor metastasis and its developmental role remain unclear. In this paper, we first report the identification of the Drosophila ortholog of human BRMS1, dBrms1. Through a genetic approach, the role of dBrms1 during development has been investigated. We found that dBrms1 is an essential gene and loss of dBrms1 function results in lethality at early developmental stages. dBrms1mutants displayed phenotypes such as developmental delay and failure to initiate metamorphosis. Further analysis suggests that these phenotypes are contributed by defective ecdysone signaling and expression of target genes of the ecdysone pathway. Therefore, dBrms1 is required for growth control by acting as a modulator of ecdysone signaling in Drosophila and is required for metamorphosis for normal development.",

author = "Shilin Song and Yuan Yuan and Jinfeng Lu and Qi Li and Zuoyan Zhu and Qichang Fan and Youfang Xue and Lai, {Zhi Chun} and Wenxia Zhang",

note = "Funding Information: We thank Dr. Renjie Jiao for fly strains, Dr. Xun Huang for his help and the idea of feeding flies with ecdysone, Dr. Xinhua Lin for the pCaSpeR4 vector, the Bloomington Drosophila Stock Center for fly strains, and Gu Chun for participating part of work. This research was supported by the National Natural Science Foundation of China (Grant no. 30270186 and 30771058 ). ",

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doi = "10.1016/j.ydbio.2013.05.012",

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AU - Song, Shilin

AU - Yuan, Yuan

AU - Lu, Jinfeng

AU - Li, Qi

AU - Zhu, Zuoyan

AU - Fan, Qichang

AU - Xue, Youfang

AU - Lai, Zhi Chun

AU - Zhang, Wenxia

N1 - Funding Information: We thank Dr. Renjie Jiao for fly strains, Dr. Xun Huang for his help and the idea of feeding flies with ecdysone, Dr. Xinhua Lin for the pCaSpeR4 vector, the Bloomington Drosophila Stock Center for fly strains, and Gu Chun for participating part of work. This research was supported by the National Natural Science Foundation of China (Grant no. 30270186 and 30771058 ).

PY - 2013/8/15

Y1 - 2013/8/15

N2 - BRMS1 was first discovered as a human breast carcinoma metastasis suppressor gene. However, the mechanism of BRMS1 in tumor metastasis and its developmental role remain unclear. In this paper, we first report the identification of the Drosophila ortholog of human BRMS1, dBrms1. Through a genetic approach, the role of dBrms1 during development has been investigated. We found that dBrms1 is an essential gene and loss of dBrms1 function results in lethality at early developmental stages. dBrms1mutants displayed phenotypes such as developmental delay and failure to initiate metamorphosis. Further analysis suggests that these phenotypes are contributed by defective ecdysone signaling and expression of target genes of the ecdysone pathway. Therefore, dBrms1 is required for growth control by acting as a modulator of ecdysone signaling in Drosophila and is required for metamorphosis for normal development.

AB - BRMS1 was first discovered as a human breast carcinoma metastasis suppressor gene. However, the mechanism of BRMS1 in tumor metastasis and its developmental role remain unclear. In this paper, we first report the identification of the Drosophila ortholog of human BRMS1, dBrms1. Through a genetic approach, the role of dBrms1 during development has been investigated. We found that dBrms1 is an essential gene and loss of dBrms1 function results in lethality at early developmental stages. dBrms1mutants displayed phenotypes such as developmental delay and failure to initiate metamorphosis. Further analysis suggests that these phenotypes are contributed by defective ecdysone signaling and expression of target genes of the ecdysone pathway. Therefore, dBrms1 is required for growth control by acting as a modulator of ecdysone signaling in Drosophila and is required for metamorphosis for normal development.

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The Drosophila ortholog of breast cancer metastasis suppressor gene, dBrms1, is critical for developmental timing through regulating ecdysone signaling

Abstract

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