Differentially expressed miRNAs in triple negative breast cancer between African-American and non-Hispanic white women

Sugita, Bruna M.; Gill, Mandeep; Mahajan, A; Duttargi, Anju; Kirolikar, Saurabh; Almeida, Rodrigo Coutinho de; Regis, Kenny; Oluwasanmi, Olusayo L.; Marchi, Fábio Albuquerque; Marian, Cătălin; Makambi, Kepher H.; Kallakury, Bhaskar; Sheahan, Laura; Cavalli, Iglenir João; Ribeiro, Enilze Maria de Souza Fonseca; Madhavan, Subha; Boca, Simina M.; Gusev, Yuriy; Cavalli, Luciane R.

doi:10.18632/oncotarget.13024

Cited by 46 publications

(87 citation statements)

References 76 publications

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“…This 20patient subset included 6 TNBC patients and 14 NTN patients. Principal component analysis (PCA) of 3000 AIMs overlaid with self-reported ethnicity of our cases showed separation of distinct ancestral populations [22] when merged with two populations from the 1000 Genomes Project: African descent (AFR) and ad mixed American (AMR) (Fig. 3c).…”

Section: Esrrb Does Not Have Copy Number Loss In Tnbcmentioning

confidence: 89%

“…Next, we sought to determine if the observed decrease in ESRRB mRNA expression found in TNBC/BLBC may be due to copy number loss. We approached this by analyzing an independent, 106-patient cohort of Caucasian (CW) and African American (AA) patients with TNBC and non TNBC (NTN) using array comparative genomic hybridization (aCGH) as previously described by Sugita, et al [22]. ESRRB copy number was calculated and defined as deletion, loss, gain, or amplification, and demographic information was analyzed for associations with ESRRB copy number changes ( Fig.…”

Section: Esrrb Does Not Have Copy Number Loss In Tnbcmentioning

confidence: 99%

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The orphan nuclear receptor estrogen-related receptor beta (ERRβ) in triple-negative breast cancer

Fernandez

Geng

Chaldekas

et al. 2019

Preprint

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PurposeTriple negative breast cancer (TNBC)/ basal-like breast cancer (BLBC) is a highly aggressive form of breast cancer prevalent in African-American (AA) women. We previously reported that a small molecule agonist ligand for the orphan nuclear receptor estrogen-related receptor beta (ERRβ or ESRRB) has growth inhibitory and anti-mitotic activity in TNBC cell lines. In this study, we evaluate the association of ESRRB mRNA, copy number levels, and protein expression with demographic, clinicopathological, and gene expression features in breast tumor clinical specimens. Methods ESRRB mRNA level expression and clinical associations were analyzed usingRNAseq data. Array-based comparative genomic hybridization determined ESRRB copy number in AA and Caucasian women. Transcription factor activity was measured using promoter-reporter luciferase assays in TNBC cell lines. Semi-automatic quantification of immunohistochemistry measured ERRβ protein expression on a 150patient tissue microarray series. ResultsESRRB mRNA expression is significantly lower in TNBC/BLBC vs. other breast cancer subtypes. There is no evidence of ESRRB copy number loss. ESRRB mRNA expression is correlated with the expression of genes associated with neuroactive ligand-receptor interaction, metabolic pathways, and deafness. These genes contain G/C-rich transcription factor binding motifs. The ESRRB message is alternatively spliced into three isoforms, which we show have different transcription factor activity in basal-like vs. other TNBC cell lines. We further show that the ERRβ2 and ERRβsf isoforms are broadly expressed in breast tumors at the protein level. ConclusionsDecreased ESRRB mRNA expression, and distinct patterns of ERRβ isoform subcellular localization and transcription factor activity are key features in TNBC/BLBC. KeywordsTriple negative breast cancer Basal-like breast cancer Molecular subtypes Estrogen-related receptor beta ABBREVIATIONS TNBC Triple negative breast cancer BLBC Basal-like breast cancer AA African-American ESRRB Estrogen related receptor beta IHC Immunohistochemistry ER Estrogen receptor PR progesterone receptor HER2 human epidermal growth factor two CW Caucasian/White NR Nuclear receptor(s) ONR Orphan nuclear receptor

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Section: Esrrb Does Not Have Copy Number Loss In Tnbcmentioning

confidence: 89%

Section: Esrrb Does Not Have Copy Number Loss In Tnbcmentioning

confidence: 99%

The orphan nuclear receptor estrogen-related receptor beta (ERRβ) in triple-negative breast cancer

Fernandez

Geng

Chaldekas

et al. 2019

Preprint

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“…A genome-wide analysis of CNAs conducted in different types of cancer revealed that a specific tumor type presents 17% of regions with amplifications and 16% of deletions, compared with <0.5% in normal samples (40). The patterns of these somatic tumor alterations, as CNVs, may also vary within ethnic groups (35,41). The majority of the studies assessing these alterations, in addition to their gene and epigenetic expression profiles, are in White European and African American patients with breast cancer (35,(40)(41)(42)(43)(44)(45).…”

Section: Discussionmentioning

confidence: 99%

“…The patterns of these somatic tumor alterations, as CNVs, may also vary within ethnic groups (35,41). The majority of the studies assessing these alterations, in addition to their gene and epigenetic expression profiles, are in White European and African American patients with breast cancer (35,(40)(41)(42)(43)(44)(45). Few studies have been performed in patients from Sub-Saharan countries (24,25).…”

Section: Discussionmentioning

confidence: 99%

“…DNA was isolated using the standard phenol-chlorophorm method as was previously described (32). Normal (reference) DNA was prepared from the peripheral blood of a pool of multiple healthy female donors, as previously described (35,36). Equal amounts of tumor and reference genomic DNA (300-500 ng) were digested and enzymatically labeled using the SureTag Complete DNA Labeling kit (Agilent Technologies, Inc.) and hybridized to the arrays, according to the manufacture's protocols.…”

Section: Methodsmentioning

confidence: 99%

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Patterns of copy number alterations in primary breast tumors of South African patients and their impact on functional cellular pathways

et al. 2018

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Breast cancer is the most common and the leading cause of female mortality among South African (SA) women. Several non-biological and biological risk factors may be attributed to their observed high mortality rate; however, the molecular profiles associated with their breast tumors are poorly characterized. The present study examined the patterns of genome-wide copy number alterations (CNAs) and their potential impact on functional cellular pathways targeted by cancer driver genes in patients with breast cancer from the Western Cape region of SA. Array-comparative genomic hybridization analysis, performed in 28 cases of invasive breast cancer, revealed a mean number of 8.68±6.18 CNAs per case, affecting primarily the Xp22.3 and 6p21-p25 cytobands (57.14% of the cases), followed by 19p13.3-p13.11 (35.7%), 2p25.3-p24.3, 4p16.3-p15.3, 8q11.1-q24.3 and 16 p13.3-p11.2 (32.14%). Functional enrichment analysis of genes and microRNA targets mapped in these affected cytobands revealed critical cancer-associated pathways, including fatty acid biosynthesis and metabolism, extracellular matrix-receptor interaction, hippo and tumor protein p53 signaling pathways, which are regulated by known cancer genes, including CCND1, CDKN1A, MAPK1, MDM2, TP53 and SMAD2. An inverse correlation was observed among the number of CNAs and tumor size and grade; CNAs on the 4p and 6p cytobands were also inversely correlated with tumor grade. No association was observed in the number of CNAs and/or the affected cytobands and the different ethnic groups of the SA patients, indicating that their tumor genome is affected by CNAs, irrespectively of their genetic descent. Additional genomic tumor profiling in SA and other Sub-Saharan African patients with breast cancer is required to determine the associations of the CNAs observed with prognosis and clinical outcome.

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Identification of dysregulated miRNAs in triple negative breast cancer: A meta‐analysis approach

Naorem

Venkatesan

2018

Journal Cellular Physiology

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Triple negative breast cancer (TNBC) is an aggressive subtype of breast cancer with poor clinical outcomes and lack of approved targeted therapy. Dysregulated microRNAs (miRNAs) have been considered a promising biomarker, which plays an important role in the tumorigenesis of human cancer. Due to the increase in miRNA profiling datasets of TNBC, a proper analysis is required for studying. Therefore, this study used meta‐analysis to amalgamate ten miRNA profiling studies of TNBC. By the robust rank aggregation method, metasignatures of six miRNAs (4 upregulated: hsa‐miR‐135b‐5p, hsa‐miR‐18a‐5p, hsa‐miR‐9‐5p and hsa‐miR‐522‐3p; 2 downregulated: hsa‐miR‐190b and hsa‐miR‐449a) were obtained. The gene ontology analysis revealed that target genes regulated by miRNAs were associated with processes like the regulation of transcription, DNA dependent, and signal transduction. Also, it is noted from the pathway analysis that signaling and cancer pathways were associated with the progression of TNBC. A Naïve Bayes‐based classifier built with miRNA signatures discriminates TNBC and non‐TNBC samples in test data set with high diagnostic sensitivity and specificity. From the analysis carried out by the study, it is suggested that the identified miRNAs are of great importance in improving the diagnostics and therapeutics for TNBC.

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Differentially expressed miRNAs in triple negative breast cancer between African-American and non-Hispanic white women

Cited by 46 publications

References 76 publications

The orphan nuclear receptor estrogen-related receptor beta (ERRβ) in triple-negative breast cancer

The orphan nuclear receptor estrogen-related receptor beta (ERRβ) in triple-negative breast cancer

Patterns of copy number alterations in primary breast tumors of South African patients and their impact on functional cellular pathways

Identification of dysregulated miRNAs in triple negative breast cancer: A meta‐analysis approach

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