Estrogen receptor α K303R mutation reorganizes its binding to forkhead box protein A1 regions and induces chromatin opening

Nakadai, Tomoyoshi; Yang, Liying; Kumegawa, Kohei; Maruyama, Reo

doi:10.1007/s11033-022-08089-3

Mol Biol Rep

2022

DOI: 10.1007/s11033-022-08089-3

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Estrogen receptor α K303R mutation reorganizes its binding to forkhead box protein A1 regions and induces chromatin opening

Tomoyoshi Nakadai

Liying Yang

Kohei Kumegawa

et al.

Abstract: Background Estrogen receptor alpha (ERα) is a frequently mutated gene in breast cancer (BC). While many studies have investigated molecular dysregulation by hotspot mutations at Y537 and D538, which exhibit an estrogen-independent constitutively active phenotype, the functional abnormalities of other mutations remain obscure. The K303R mutation in primary invasive BC has been implicated with endocrine resistance, tumor size, and lymph node positivity. However, the impact of the K303R mutation on … Show more

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2024

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Estrogen Receptor Alpha Mutations, Truncations, Heterodimers, and Therapies

Hancock,

Gertz,

Jeselsohn

et al. 2024

Endocrinology

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Annual breast cancer (BCa) deaths have declined since its apex in 1989 concomitant with widespread adoption of hormone therapies that target estrogen receptor alpha (ERα), the prominent nuclear receptor expressed in ∼80% of BCa. However, up to ∼50% of ER + patients with high-risk disease experience post endocrine therapy relapse and metastasis to distant organs. The vast majority of BCa mortality occurs in this setting, highlighting the inadequacy of current therapies. Genomic abnormalities to ESR1, the gene encoding ERα, emerge under prolonged selective pressure to enable endocrine therapy resistance. These genetic lesions include focal gene amplifications, hotspot missense mutations in the ligand binding domain, truncations, fusions, and complex interactions with other nuclear receptors. Tumor cells utilize aberrant ERα activity to proliferate, spread and evade therapy in BCa as well as other cancers. Cutting edge studies on ERα structural and transcriptional relationships are being harnessed to produce new therapies that have shown benefits in patients with ESR1 hotspot mutations. In this review we discuss the history of ERα, current research unlocking unknown aspects of ERα signaling including the structural basis for receptor antagonism, and future directions of ESR1 investigation. In addition, we discuss the development of endocrine therapies from their inception to present day and survey new avenues of drug development to improve pharmaceutical profiles, targeting, and efficacy.

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Estrogen Receptor Alpha Mutations, Truncations, Heterodimers, and Therapies

Hancock,

Gertz,

Jeselsohn

et al. 2024

Endocrinology

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show abstract

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Estrogen receptor α K303R mutation reorganizes its binding to forkhead box protein A1 regions and induces chromatin opening

Cited by 1 publication

References 44 publications

Estrogen Receptor Alpha Mutations, Truncations, Heterodimers, and Therapies

Estrogen Receptor Alpha Mutations, Truncations, Heterodimers, and Therapies

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