Loss of MutL Disrupts CHK2-Dependent Cell-Cycle Control through CDK4/6 to Promote Intrinsic Endocrine Therapy Resistance in Primary Breast Cancer

Haricharan, Svasti; Punturi, Nindo; Singh, Purba; Holloway, Kimberly; Anurag, Meenakshi; Schmelz, Jacob; Schmidt, Cecilia; Lei, Jonathan T.; Suman, Vera J.; Hunt, Kelly K.; Olson, John A.; Hoog, Jeremy; Li, Shunqiang; Huang, Shixia; Edwards, Dean P.; Kavuri, Shyam M.; Bainbridge, Matthew N.; Cynthia, X.; Ellis, Matthew J.

doi:10.1158/2159-8290.cd-16-1179

Cited by 61 publications

(102 citation statements)

References 58 publications

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“…All arms were deprived of estrogen supplementation at randomization. As expected from previous experiments 15 , we observed estrogen independent and fulvestrant resistant growth in MCF7 shMLH1 tumors, and little response to lapatinib alone ( Fig 4A). However, there was striking response with tumor shrinkage to the combination of fulvestrant and lapatinib ( Fig 4A).…”

Section: Her2 Activation Is Required For Endocrine Treatment Resistansupporting

confidence: 90%

“…Since MutL -ER + tumors have a higher mutation load than MutL + tumors 15,19 we tested whether HER2 activation in these tumors occurred via activating mutations 11 . However, frequency of HER2 mutations did not significantly associate with MutL status, if anything appearing lower in MutL -ER + tumors than in MutL + ones ( Fig S2C).…”

Section: Inhibition Of Mismatch Repair Induces Activation Of Her2 In mentioning

confidence: 99%

“…Stable cell lines were maintained in presence of specified antibiotics at recommended concentrations. Growth assays were conducted in triplicate and repeated independently as previously using Alamar blue to identify cell viability 15 . Growth assay results were plotted as fold change in growth from days 1 to 7 and normalized as specified.…”

Section: Cell Lines Mice Crispr Si/shrna Transfection and Growth mentioning

confidence: 99%

“…Defects in the MutL complex of mismatch repair, comprised of MLH1 and PMS2, were recently identified as drivers of endocrine treatment resistance in 15-17% of ER + /HER2breast cancer patients 15,16 . Mismatch repair is a fundamental DNA repair pathway conserved between pro-and eukaryotes, and essential for guarding the genome during cellular replication 17 .…”

Section: Introductionmentioning

confidence: 99%

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Mismatch repair deficiency predicts response to HER2 blockade in HER2-negative breast cancer

Punturi

Şeker

Devarakonda

et al. 2020

Preprint

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One Sentence Summary: Defective mismatch repair activates HER2 in HER2-negative breast cancer cells and renders them susceptible to HER2 inhibitors. Abstract: Estrogen receptor positive (ER + ) breast cancer is a leading cause of cancer-related death globally. Resistance to standard of care endocrine treatment occurs in at least 30% of ER + breast cancer patients resulting in ~40,000 deaths every year in the US alone. Preclinical studies strongly implicate activation of growth factor receptor, HER2 in endocrine treatment resistance of ER + breast cancer that is HER2at diagnosis 1,2 . However, clinical trials of pan-HER inhibitors in ER + /HER2patients have disappointed, likely due to a lack of predictive biomarkers 3-6 . Here we demonstrate that loss of MLH1, a principal mismatch repair gene, causally activates HER2 in ER + /HER2breast cancer upon endocrine treatment. Additionally, we show that HER2 activation is indispensable for endocrine treatment resistant growth of MLH1cells in vitro and in vivo. Consequently, inhibiting HER2 restores sensitivity to endocrine treatment in multiple experimental models including patient-derived xenograft tumors. Patient data from multiple clinical datasets (TCGA, METABRIC, Alliance (Z1031) and E-GEOD-28826) supports an association between MLH1 loss, HER2 upregulation, and sensitivity to trastuzumab in endocrine treatment-resistant ER + /HER2patients. These results provide strong rationale that MLH1 could serve as a first-in-class predictive marker of sensitivity to combinatorial treatment with endocrine drugs and HER inhibitors in endocrine treatment-resistant ER + /HER2breast cancer patients. Implications of this study extend beyond breast cancer to Lynch Syndrome cancers. [Main Text: ]

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Section: Her2 Activation Is Required For Endocrine Treatment Resistansupporting

confidence: 90%

Section: Inhibition Of Mismatch Repair Induces Activation Of Her2 In mentioning

confidence: 99%

Section: Cell Lines Mice Crispr Si/shrna Transfection and Growth mentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

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Mismatch repair deficiency predicts response to HER2 blockade in HER2-negative breast cancer

Punturi

Şeker

Devarakonda

et al. 2020

Preprint

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“…Mutations in PRKDC will potentially produce a defective ATM response/low ATM levels 27 which is interesting in the context of the finding herein that ATM mutations are a potential luminal B driver gene. The significance of a defective ATM pathway as a cause of endocrine resistance is highlighted by the recent finding that dysregulation of the MutL complex (MLH1, PMS1 and PMS2) causes failure of ATM/CHK2-based negative regulation of CDK4/6 28 . Prognostic candidate mutations revealed by the MA12 analysis were different from the UBC TAM series, likely reflecting the different patient profiles and adjuvant treatments illustrated in Figure 2 .…”

Section: Discussionmentioning

confidence: 99%

The prognostic effects of somatic mutations in ER-positive breast cancer

Griffith

Spies

Anurag

et al. 2017

Preprint

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53More than 50 genes are recurrently affected by somatic mutation in estrogen receptor positive 54 (ER+) breast cancer but prognostic effects have not been definitively established. Primary tumor 55DNA was therefore subjected to targeted sequencing from 625 postmenopausal (UBC-TAM 56 series) and 328 premenopausal (MA12 trial) hormone receptor-positive (HR+) patients. 57Independent validation of prognostic interactions was achieved using independent data from the 58 METABRIC study. Associations between MAP3K1 and PIK3CA with luminal A status and TP53 59mutations with Luminal B/non-luminal tumors were observed, validating the methodological 60 approach. In UBC-TAM, NF1 frame-shift nonsense (FS/NS) mutation was validated as a poor 61 outcome driver. For MA12, poor outcome associated with PIK3R1 mutation was similarly 62 validated. DDR1 mutations were strongly associated with poor prognosis in UBC-TAM despite 63 stringent false-discovery correction (q=0.0003). In conclusion, uncommon recurrent somatic 64 mutations should be further explored to create a more complete explanation of the highly 65 variable outcomes that typify ER+ breast cancer.

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Molecular Mechanisms of Endocrine Resistance

Angelis

Veeraraghavan

et al. 2018

Cancer Drug Discovery and Development

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Loss of MutL Disrupts CHK2-Dependent Cell-Cycle Control through CDK4/6 to Promote Intrinsic Endocrine Therapy Resistance in Primary Breast Cancer

Cited by 61 publications

References 58 publications

Mismatch repair deficiency predicts response to HER2 blockade in HER2-negative breast cancer

Mismatch repair deficiency predicts response to HER2 blockade in HER2-negative breast cancer

The prognostic effects of somatic mutations in ER-positive breast cancer

Molecular Mechanisms of Endocrine Resistance

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