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. 2024 Jul;67(7):1413-1426.
doi: 10.1007/s11427-023-2460-0. Epub 2024 Apr 1.

Cytokines-activated nuclear IKKα-FAT10 pathway induces breast cancer tamoxifen-resistance

Xueyan Chen #  1   2 Weilin Wu #  2 Ji-Hak Jeong  2 Matjaz Rokavec  2 Rui Wei  1 Shaolong Feng  2 Werner Schroth  3   4 Hiltrud Brauch  3   4 Shangwei Zhong  5   6 Jun-Li Luo  7   8   9   10
Affiliations

Cytokines-activated nuclear IKKα-FAT10 pathway induces breast cancer tamoxifen-resistance

Xueyan Chen et al. Sci China Life Sci. 2024 Jul.

Abstract

Endocrine therapy that blocks estrogen signaling is the most effective treatment for patients with estrogen receptor positive (ER+) breast cancer. However, the efficacy of agents such as tamoxifen (Tam) is often compromised by the development of resistance. Here we report that cytokines-activated nuclear IKKα confers Tam resistance to ER+ breast cancer by inducing the expression of FAT10, and that the expression of FAT10 and nuclear IKKα in primary ER+ human breast cancer was correlated with lymphotoxin β (LTB) expression and significantly associated with relapse and metastasis in patients treated with adjuvant mono-Tam. IKKα activation or enforced FAT10 expression promotes Tam-resistance while loss of IKKα or FAT10 augments Tam sensitivity. The induction of FAT10 by IKKα is mediated by the transcription factor Pax5, and coordinated via an IKKα-p53-miR-23a circuit in which activation of IKKα attenuates p53-directed repression of FAT10. Thus, our findings establish IKKα-to-FAT10 pathway as a new therapeutic target for the treatment of Tam-resistant ER+ breast cancer.

Keywords: FAT10; Pax5; Tam-resistance; breast cancer; lymphotoxin; nuclear IKKα; nuclear IKKα-FAT0 pathway.

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