Liver x receptor alpha drives chemoresistance in response to side-chain hydroxycholesterols in triple negative breast cancer

Hutchinson, Samantha A.; Websdale, Alex; Cioccoloni, Giorgia; Røberg-Larsen, Hanne; Lianto, Priscilia; Kim, Baek; Rose, Ailsa; Soteriou, Chrysa; Pramanik, Arindam; Wastall, Laura M; Williams, Bethany; Henn, Madeline A.; Chen, Joy J.; Ma, Liqian; Moore, J. Bernadette; Nelson, Erik R.; Hughes, Tom; Thorne, James L.

doi:10.1038/s41388-021-01720-w

Cited by 26 publications

(20 citation statements)

References 38 publications

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“…To confirm if the protein bands were LXRa variants, we first performed siLXRa treatments in cell lines. Using previously validated (Hutchinson et al, 2021) siRNA duplexes (Origene trisilencers) against LXRa and LXRb, we found that the protein bands predicted by size to be a1, a2, a3, a5, and b1 were all significantly reduced by targeted siRNA in all cell lines tested (all p < 0.05; Figure S10). Note that a4 and b4 were not expressed in cell lines and so could not be validated in this way.…”

Section: Validation Of Isoform Identity Bands Representing Lxr Variants Were Reduced By Targeted Sirnamentioning

confidence: 86%

“…We previously reported that LXRa expression is positively correlated to target gene expression in ER-negative patients who had relapsed and/or died due to their disease (Event patients) but not those who survive (Hutchinson et al, 2021). Here, we tested the hypothesis that differential LXR splice variant expression between cancers may contribute to disease etiology via their ability to control expression of gene targets.…”

Section: Lxr Splice Variants Are Differentially Correlated With Expression Of Target Genes In Event and No Event Patientsmentioning

confidence: 99%

“…The liver x receptors (LXRa/NR1H3; LXRb/NR1H2) are homeostatic regulators of cholesterol metabolism and as such have been suggested as potential therapeutic targets. LXRa activation by hydroxylated cholesterol (oxysterols) has been linked to poor survival by driving multi-drug resistance in patients with TNBC (Hutchinson et al, 2021) and increased metastasis in mouse models (Baek et al, 2017;Nelson et al, 2013). On the other hand, LXRb activation by histamine conjugated oxysterols such as dendrogenin A can induce lethal autophagy in BCa (Poirot and Silvente-Poirot, 2018).…”

Section: Introductionmentioning

confidence: 99%

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Characterization and prognostic value of LXR splice variants in triple-negative breast cancer

et al. 2021

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Activity of liver x receptor (LXR), the homeostatic regulator of cholesterol metabolism, is elevated in triple-negative breast cancer (BCa) relative to other BCa subtypes, driving drug resistance and metastatic gene signatures. The loci encoding LXRa and LXRb produce multiple alternatively spliced proteins, but the true range of variants and their relevance to cancer remain poorly defined. Here, we report seven LXR splice variants, three of which have not previously been reported and five that were prognostic for disease-free survival. Expression of full-length LXRa splice variants was associated with poor prognosis, consistent with a role as an oncogenic driver of triple-negative tumor pathophysiology. Contrary to this was the observation that high expression of truncated LXRa splice variants or any LXRb splice variant was associated with longer survival. These findings indicate that LXR isoform abundance is an important aspect of understanding the link between dysregulated cholesterol metabolism and cancer pathophysiology.

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Section: Validation Of Isoform Identity Bands Representing Lxr Variants Were Reduced By Targeted Sirnamentioning

confidence: 86%

Section: Lxr Splice Variants Are Differentially Correlated With Expression Of Target Genes In Event and No Event Patientsmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

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Characterization and prognostic value of LXR splice variants in triple-negative breast cancer

et al. 2021

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“…In contrast, activation of LXR by LXR agonist inhibited breast cancer cell proliferation in vitro [51]. Interestingly, Hutchinson et al reported that activation of LXR by LXR antagonist contributes to resistance of triple negative breast cancer to epirubicin in vivo [52]. Possibly, the efficacy of specific agents depends on in vitro vs. in vivo methods, tumor type or genotype, or the specific regimen or drug combination evaluated.…”

Section: Discussionmentioning

confidence: 99%

The BET Inhibitor JQ1 Augments the Antitumor Efficacy of Gemcitabine in Preclinical Models of Pancreatic Cancer

Miller

Garcia

Fehling

et al. 2021

Cancers

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Gemcitabine is used to treat pancreatic cancer (PC), but is not curative. We sought to determine whether gemcitabine + a BET bromodomain inhibitor was superior to gemcitabine, and identify proteins that may contribute to the efficacy of this combination. This study was based on observations that cell cycle dysregulation and DNA damage augment the efficacy of gemcitabine. BET inhibitors arrest cells in G1 and allow increases in DNA damage, likely due to inhibition of expression of DNA repair proteins Ku80 and RAD51. BET inhibitors (JQ1 or I-BET762) + gemcitabine were synergistic in vitro, in Panc1, MiaPaCa2 and Su86 PC cell lines. JQ1 + gemcitabine was more effective in vivo than either drug alone in patient-derived xenograft models (P < 0.01). Increases in the apoptosis marker cleaved caspase 3 and DNA damage marker γH2AX paralleled antitumor efficacy. Notably, RNA-seq data showed that JQ1 + gemcitabine selectively inhibited HMGCS2 and APOC1 ~6-fold, compared to controls. These proteins contribute to cholesterol biosynthesis and lipid metabolism, and their overexpression supports tumor cell proliferation. IPA data indicated that JQ1 + gemcitabine selectively inhibited the LXR/RXR activation pathway, suggesting the hypothesis that this inhibition may contribute to the observed in vivo efficacy of JQ1 + gemcitabine.

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“…Leeds teaching Hospitals NHS Trust, Leeds, UK Detoxification and nutrient metabolism are connected in healthy tissues to prevent toxic accumulation of metabolic intermediates and end-products (1) . These pathways also enhance processing of xenobiotics such as anti-cancer drugs (2) . Resistance to anti-cancer drugs remains a major barrier to successful treatment of many cancer types, yet clinical tools that predict which treatment regimen would be most effective at individual patient level remain underdeveloped.…”

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confidence: 99%

Overlap between nutrient metabolism and chemotherapy detoxification in triple negative breast cancer

et al. 2021

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Liver x receptor alpha drives chemoresistance in response to side-chain hydroxycholesterols in triple negative breast cancer

Cited by 26 publications

References 38 publications

Characterization and prognostic value of LXR splice variants in triple-negative breast cancer

Characterization and prognostic value of LXR splice variants in triple-negative breast cancer

The BET Inhibitor JQ1 Augments the Antitumor Efficacy of Gemcitabine in Preclinical Models of Pancreatic Cancer

Overlap between nutrient metabolism and chemotherapy detoxification in triple negative breast cancer

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