Investigation of the adolescent female breast transcriptome and the impact of obesity.

Breast cancer research : BCR 2020 Vol.22(1) p. 44

Burkholder A, Akrobetu D, Pandiri AR, Ton K, Kim S, Labow BI, Nuzzi LC, Firriolo JM, Schneider SS, Fenton SE, Shaw ND

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Abstract

[BACKGROUND] Early life environmental exposures affect breast development and breast cancer risk in adulthood. The breast is particularly vulnerable during puberty when mammary epithelial cells proliferate exponentially. In overweight/obese (OB) women, inflammation increases breast aromatase expression and estrogen synthesis and promotes estrogen-receptor (ER)-positive breast cancer. In contrast, recent epidemiological studies suggest that obesity during childhood decreases future breast cancer risk. Studies on environmental exposures and breast cancer risk have thus far been limited to animal models. Here, we present the first interrogation of the human adolescent breast at the molecular level and investigate how obesity affects the immature breast.

[METHODS] We performed RNA-seq in 62 breast tissue samples from adolescent girls/young women (ADOL; mean age 17.8 years) who underwent reduction mammoplasty. Thirty-one subjects were non-overweight/obese (NOB; mean BMI 23.4 kg/m) and 31 were overweight/obese (OB; BMI 32.1 kg/m). We also compared our data to published mammary transcriptome datasets from women (mean age 39 years) and young adult mice, rats, and macaques.

[RESULTS] The ADOL breast transcriptome showed limited (30%) overlap with other species, but 88% overlap with adult women for the 500 most highly expressed genes in each dataset; only 43 genes were shared by all groups. In ADOL, there were 120 differentially expressed genes (DEG) in OB compared with NOB samples (p < 0.05). Based on these DEG, Ingenuity Pathway Analysis (IPA) identified the cytokines CSF1 and IL-10 and the chemokine receptor CCR2 as among the most highly activated upstream regulators, suggesting increased inflammation in the OB breast. Classical ER targets (e.g., PR, AREG) were not differentially expressed, yet IPA identified the ER and PR and growth factors/receptors (VEGF, HGF, HER3) and kinases (AKT1) involved in hormone-independent ER activation as activated upstream regulators in OB breast tissue.

[CONCLUSIONS] These studies represent the first investigation of the human breast transcriptome during late puberty/young adulthood and demonstrate that obesity is associated with a transcriptional signature of inflammation which may augment estrogen action in the immature breast microenvironment. We anticipate that these studies will prompt more comprehensive cellular and molecular investigations of obesity and its effect on the breast during this critical developmental window.

추출된 의학 개체 (NER)

유형영어 표현한국어 / 풀이UMLS CUI출처등장
해부 breast 유방 dict 17
해부 mammary 유방 dict 2
시술 reduction mammoplasty 유방성형술 dict 1
해부 mammary epithelial cells scispacy 1
해부 IPA → Ingenuity Pathway Analysis scispacy 1
해부 cellular scispacy 1
약물 estrogen C0014939
estrogens
scispacy 1
약물 NOB C4727454
Bokmal Language
scispacy 1
약물 [BACKGROUND] scispacy 1
약물 DEG → differentially expressed genes scispacy 1
약물 [CONCLUSIONS] scispacy 1
질환 obesity C0028754
Obesity
scispacy 1
질환 breast cancer C0006142
Malignant neoplasm of breast
scispacy 1
질환 inflammation C0021368
Inflammation
scispacy 1
질환 breast aromatase scispacy 1
질환 breast tissue samples scispacy 1
질환 ADOL scispacy 1
질환 IPA → Ingenuity Pathway Analysis scispacy 1
질환 hormone-independent ER scispacy 1
기타 women scispacy 1
기타 estrogen-receptor scispacy 1
기타 human scispacy 1
기타 subjects scispacy 1
기타 mice scispacy 1
기타 rats scispacy 1
기타 macaques scispacy 1
기타 CSF1 scispacy 1
기타 IL-10 scispacy 1
기타 CCR2 scispacy 1
기타 OB breast scispacy 1
기타 AREG scispacy 1
기타 factors/receptors scispacy 1
기타 VEGF scispacy 1
기타 HGF scispacy 1
기타 HER3 scispacy 1
기타 AKT1 scispacy 1
기타 OB breast tissue scispacy 1
기타 human breast scispacy 1

MeSH Terms

Adolescent; Adult; Biomarkers, Tumor; Breast; Breast Neoplasms; Female; Humans; Inflammation; Obesity; Receptors, Estrogen; Risk Factors; Transcriptome; Tumor Microenvironment; Young Adult

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