An RNA Interference Screen Identifies Metabolic Regulators NR1D1 and PBP as Novel Survival Factors for Breast Cancer Cells with the ERBB2 Signature

Kourtidis, Antonis; Jain, Ritu; Carkner, Richard; Eifert, Cheryl; Brosnan, M. Julia; Conklin, Douglas S.

doi:10.1158/0008-5472.can-09-1550

Cited by 80 publications

(117 citation statements)

References 42 publications

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“…22 Like Kourtidis et al, 21 we noted that TPD52 knock-down decreased the survival of ERBB2-positive breast cancer cell lines, 22 which were characterized by higher levels of LD staining. 21 Breast and prostate cancers have been shown to accumulate cytoplasmic LDs, [23][24][25] and ERBB2 expression in breast cancer has been associated with a transcriptional program upregulating fatty acid synthase. 26 TPD52 also has a long history of being identified and studied as an androgen-induced gene/ protein, 27,28 and androgen treatment of prostate cancer cells increases cytoplasmic LDs 25 and regulates key anabolic enzymes.…”

Section: Early Evidencesupporting

confidence: 55%

“…Our group reconsidered these and other results following the publication of Kourtidis et al in 2010, which described the reliance of ERBB2-positive breast cancer cell lines upon chromosome 17-encoded regulators of lipid metabolism. 21 At the time, we were analyzing the effects of TPD52 knock-down in breast cell lines. 22 Like Kourtidis et al, 21 we noted that TPD52 knock-down decreased the survival of ERBB2-positive breast cancer cell lines, 22 which were characterized by higher levels of LD staining.…”

Section: Early Evidencementioning

confidence: 99%

“…21 At the time, we were analyzing the effects of TPD52 knock-down in breast cell lines. 22 Like Kourtidis et al, 21 we noted that TPD52 knock-down decreased the survival of ERBB2-positive breast cancer cell lines, 22 which were characterized by higher levels of LD staining. 21 Breast and prostate cancers have been shown to accumulate cytoplasmic LDs, [23][24][25] and ERBB2 expression in breast cancer has been associated with a transcriptional program upregulating fatty acid synthase.…”

Section: Early Evidencementioning

confidence: 99%

“…10 There is therefore no shortage of explanations for why cancer cells might benefit from TPD52 overexpression, but these explanations are relatively generic and would not be expected to favor one cancer cell type over others. Where knock-down studies have been conducted in different breast cell lines, reduced TPD52 expression commonly reduced the survival of ERBB2-positive breast cancer cell lines, 21,22 suggesting a particular function in this cell type. ERBB2-positive breast cancer cell lines are characterized by increased LDs, 21 and ERBB2-positive breast cancers more frequently express proteins associated with lipogenesis or lipid storage.…”

Section: Lipid Droplets and Cancermentioning

confidence: 99%

“…Where knock-down studies have been conducted in different breast cell lines, reduced TPD52 expression commonly reduced the survival of ERBB2-positive breast cancer cell lines, 21,22 suggesting a particular function in this cell type. ERBB2-positive breast cancer cell lines are characterized by increased LDs, 21 and ERBB2-positive breast cancers more frequently express proteins associated with lipogenesis or lipid storage. 48 Increased TPD52 expression could therefore favor the survival of cell lines with increased lipogenic activity by contributing to the increased lipid storage capacity that these cells require.…”

Section: Lipid Droplets and Cancermentioning

confidence: 99%

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Dropping in on the lipid droplet- tumor protein D52 (TPD52) as a new regulator and resident protein

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Section: Early Evidencesupporting

confidence: 55%

Section: Early Evidencementioning

confidence: 99%

Section: Early Evidencementioning

confidence: 99%

Section: Lipid Droplets and Cancermentioning

confidence: 99%

Section: Lipid Droplets and Cancermentioning

confidence: 99%

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Dropping in on the lipid droplet- tumor protein D52 (TPD52) as a new regulator and resident protein

2016

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Circadian clock‐mediated nuclear receptors in cancer

Niu

Táng

2022

Journal Cellular Physiology

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Circadian system coordinates the daily periodicity of physiological and biochemical functions to adapt to environmental changes. Circadian disruption has been identified to increase the risk of cancer and promote cancer progression, but the underlying mechanism remains unclear. And further mechanistic understanding of the crosstalk between clock components and cancer is urgent to achieve clinical anticancer benefits from chronochemotherapy. Recent studies discover that several nuclear receptors regulating circadian clock, also play crucial roles in mediating multiple cancer processes. In this review, we aim to summarize the latest developments of clock-related nuclear receptors in cancer biology and dissect mechanistic insights into how nuclear receptors coordinate with circadian clock to regulate tumorigenesis and cancer treatment. A better understanding of circadian clock-related nuclear receptors in cancer could help prevent tumorigenesis and improve anticancer efficacy.

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TPD52 represents a survival factor inERBB2‐amplified breast cancer cells

Roslan

Bièche

Bright

et al. 2013

Molecular Carcinogenesis

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TPD52 and ERBB2 co-expression has been persistently reported in human breast cancer and animal models of this disease, but the significance of this is unknown. We identified significant positive associations between relative TPD52 and ERBB2 transcript levels in human diagnostic breast cancer samples, and maximal TPD52 expression in the hormone receptor (HR)- and ERBB2-positive sub-group. High-level TPD52 expression was associated with significantly reduced metastasis-free survival, within the overall cohort (log rank test, P = 8.6 × 10(-4), n = 375) where this was an independent predictor of metastasis-free survival (hazard ratio, 2.69, 95% confidence interval 1.59-4.54, P = 2.2 × 10(-4), n = 359), and the HR- and ERBB2-positive sub-group (log rank test, P = 0.035, n = 47). Transient TPD52 knock-down in the ERBB2-amplified breast cancer cell lines SK-BR-3 and BT-474 produced significant apoptosis, both singly and in combination with transient ERBB2 knock-down. Unlike ERBB2 knock-down, transient TPD52 knock-down produced no reduction in pAKT levels in SK-BR-3 or BT-474 cells. We then derived multiple SK-BR-3 cell lines in which TPD52 levels were stably reduced, and measured significant inverse correlations between pERBB2 and TPD52 levels in viable TPD52-depleted and control cell lines, all of which showed similar proliferative capacities. Our results therefore identify TPD52 as a survival factor in ERBB2-amplified breast cancer cells, and suggest complementary cellular functions for TPD52 and ERBB2.

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An RNA Interference Screen Identifies Metabolic Regulators NR1D1 and PBP as Novel Survival Factors for Breast Cancer Cells with the ERBB2 Signature

Cited by 80 publications

References 42 publications

Dropping in on the lipid droplet- tumor protein D52 (TPD52) as a new regulator and resident protein

Dropping in on the lipid droplet- tumor protein D52 (TPD52) as a new regulator and resident protein

Circadian clock‐mediated nuclear receptors in cancer

TPD52 represents a survival factor inERBB2‐amplified breast cancer cells

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