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Stephen Green

Researcher at French Institute of Health and Medical Research

Publications -  27
Citations -  10313

Stephen Green is an academic researcher from French Institute of Health and Medical Research. The author has contributed to research in topics: Estrogen receptor & Receptor. The author has an hindex of 22, co-authored 27 publications receiving 10196 citations.

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Human oestrogen receptor cDNA: sequence, expression and homology to v-erb-A

TL;DR: Cloned and sequenced the complete complementary DNA of the oestrogen receptor (ER) present in the breast cancer cell line MCF-7 and found extensive homology between the ER and the erb-A protein of the oncogenic avian erythroblastosis virus.
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Functional domains of the human estrogen receptor.

TL;DR: Deletion of most or all of the hormone-binding domain leads to only about 5% constitutive transcriptional activity, yet these mutants appear to bind efficiently to an ERE in vivo.
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Nuclear receptors enhance our understanding of transcription regulation

TL;DR: Receptors for retinoic acid, vitamin D3 and the steroid and thyroid hormones belong to a family of ligand-activated enhancer-binding factors which are composed of a number of functional domains required for ligand and DNA binding, nuclear translocation, dimerization and trans -activation of transcription.
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Cloning of the human estrogen receptor cDNA.

TL;DR: Results demonstrate that the clones isolated correspond to the ER mRNA sequence, and use of lambda OR8 as a hybridization probe revealed a single poly(A)+ RNA band of approximately equal to 6.2 kilobase pairs in the ER-containing human breast cancer cell lines MCF-7 and T47D.
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The chicken oestrogen receptor sequence: homology with v-erbA and the human oestrogen and glucocorticoid receptors.

TL;DR: A chicken oviduct cDNA clone containing the complete open reading frame of the oestrogen receptor (ER) has been isolated and sequenced, indicating that c‐erbA, the cellular counterpart of v‐erbB, belongs to a multigene family of transcriptional regulatory proteins which bind steroid‐related ligands.