Table Info

Table 1.

Mechanisms of endocrine resistance [3]

Resistance pathway	Mechanism	Reference(s)
ER expression and activity loss	Mutations	[32]
	Gene regulation	[33]
	Post-transcriptional modifications (e.g., splice variants, mRNA stability)	[34, 35]
	Post-translational modifications	[36]
Transcriptional machinery of ER	Down-regulation of co-repressors (e.g., NCoR)	[37]
	Over-expression of co-activators (e.g., AIB1)	[38, 39]
	Increased expression of transcriptional factors (e.g., AP-1, SP-1, NFκB)	[40, 41]
Cross-talk between ER and RTKs	EGF/EGFR	[42–44]
	HER2	[44–46]
	IGF1R	[47, 48]
	PI3Ks/Akt	[48–52]
	p44/42 MAPK	[53, 54]
	Stress-induced kinases (JNK, p38 MAPK)	[55]
Cell cycle regulators	Over-expression of positive regulators (e.g., MYC and cyclins E1 and D1)	[56]
	Reduced expression of negative regulators (e.g., p21 and p27)	[57, 58]
	Over-expression of anti-apoptotic molecules (e.g., BCL-XL)	[59]
	Reduced expression of pro-apoptotic molecules (e.g., BCL-2-interacting killer and caspase 9)	[59]

AIB1: amplified in breast 1; Akt: protein kinase B; AP-1: activator protein 1; BCL-2: B-cell lymphoma 2; BCL-XL: B-cell lymphoma-extra large; EGF: epidermal growth factor; EGFR: EGF receptor; IGF1R: insulin growth factor 1 receptor; JNK: c-Jun N-terminal kinase; MAPK: mitogen-activated protein kinase; NCoR: nuclear receptor corepressor; PI3Ks: phosphatidylinositol 3-kinases; SP-1: specificity protein 1

Note. Reprinted from “Biological mechanisms and clinical implications of endocrine resistance in breast cancer,” by Giuliano M, Schifp R, Osborne CK, Trivedi MV. Breast. 2011;20 Suppl 3:S42–9 (https://linkinghub.elsevier.com/retrieve/pii/S0960977611702934). CC BY-NC-ND.

Declarations

Acknowledgments

The authors acknowledge Joana Cavaco Silva for assisting in manuscript revision.

Author contributions

ISP: contributed to the manuscript design and literature analysis, wrote part of the introduction and the NFκB pathway as well as global revision to the article.

CA: contributed to the initial design of the article, wrote Notch pathway and a substantial contribution and regulators of cell cycle apoptosis, as well as to global manuscript revision.

IG: contributed to the manuscript design and literature analysis, wrote part of the introduction and created some figures.

SC: wrote the RANK-RANKL pathway chapter, and full manuscript revision.

TRP: made the revision of TKRs and alternative pathways, made Table 2 and Figures 3 and 4; also contributed to global manuscript revision.

RTS: specially contributed for the initial design of the article, contributed to the conclusion and review the final manuscript.

LC: contributed to conceptualization, design, direction and overall supervision of the manuscript.

All the authors contributed to manuscript revision, read and approved the submitted version.

Conflicts of interest

The authors declare that they have no conflicts of interest.

Ethical approval

Not applicable.

Consent to participate

Not applicable.

Consent to publication

Not applicable.

Availability of data and materials

Not applicable.

Funding

IG is supported by the FCT PhD grant SFRH/BD/139178/2018. The funders had no role in study design, data collection and analysis, decision to publish, or preparation of the manuscript.

Copyright

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