Human breast progenitor cell numbers are regulated by WNT and TBX3.
Abstract
[BACKGROUND] Although human breast development is mediated by hormonal and non-hormonal means, the mechanisms that regulate breast progenitor cell activity remain to be clarified. This limited understanding of breast progenitor cells has been due in part to the lack of appropriate model systems to detect and characterize their properties.
[METHODS] To examine the effects of WNT signaling and TBX3 expression on progenitor activity in the breast, primary human mammary epithelial cells (MEC) were isolated from reduction mammoplasty tissues and transduced with lentivirus to overexpress WNT1 or TBX3 or reduce expression of their cognate receptors using shRNA. Changes in progenitor activity were quantified using characterized assays. We identified WNT family members expressed by cell populations within the epithelium and assessed alterations in expression of WNT family ligands by MECs in response to TBX3 overexpression and treatment with estrogen and progesterone.
[RESULTS] Growth of MECs on collagen gels resulted in the formation of distinct luminal acinar and basal ductal colonies. Overexpression of TBX3 in MECs resulted in increased ductal colonies, while shTBX3 expression diminished both colony types. Increased WNT1 expression led to enhanced acinar colony formation, shLRP6 decreased both types of colonies. Estrogen stimulated the formation of acinar colonies in control MEC, but not shLRP6 MEC. Formation of ductal colonies was enhanced in response to progesterone. However, while shLRP6 decreased MEC responsiveness to progesterone, shTBX3 expression did not alter this response.
[CONCLUSIONS] We identified two phenotypically distinguishable lineage-committed progenitor cells that contribute to different structural elements and are regulated via hormonal and non-hormonal mechanisms. WNT signaling regulates both types of progenitor activity. Progesterone favors the expansion of ductal progenitor cells, while estrogen stimulates the expansion of acinar progenitor cells. Paracrine WNT signaling is stimulated by estrogen and progesterone, while autocrine WNT signaling is induced by the embryonic T-box transcription factor TBX3.
[METHODS] To examine the effects of WNT signaling and TBX3 expression on progenitor activity in the breast, primary human mammary epithelial cells (MEC) were isolated from reduction mammoplasty tissues and transduced with lentivirus to overexpress WNT1 or TBX3 or reduce expression of their cognate receptors using shRNA. Changes in progenitor activity were quantified using characterized assays. We identified WNT family members expressed by cell populations within the epithelium and assessed alterations in expression of WNT family ligands by MECs in response to TBX3 overexpression and treatment with estrogen and progesterone.
[RESULTS] Growth of MECs on collagen gels resulted in the formation of distinct luminal acinar and basal ductal colonies. Overexpression of TBX3 in MECs resulted in increased ductal colonies, while shTBX3 expression diminished both colony types. Increased WNT1 expression led to enhanced acinar colony formation, shLRP6 decreased both types of colonies. Estrogen stimulated the formation of acinar colonies in control MEC, but not shLRP6 MEC. Formation of ductal colonies was enhanced in response to progesterone. However, while shLRP6 decreased MEC responsiveness to progesterone, shTBX3 expression did not alter this response.
[CONCLUSIONS] We identified two phenotypically distinguishable lineage-committed progenitor cells that contribute to different structural elements and are regulated via hormonal and non-hormonal mechanisms. WNT signaling regulates both types of progenitor activity. Progesterone favors the expansion of ductal progenitor cells, while estrogen stimulates the expansion of acinar progenitor cells. Paracrine WNT signaling is stimulated by estrogen and progesterone, while autocrine WNT signaling is induced by the embryonic T-box transcription factor TBX3.
추출된 의학 개체 (NER)
| 유형 | 영어 표현 | 한국어 / 풀이 | UMLS CUI | 출처 | 등장 |
|---|---|---|---|---|---|
| 해부 | breast
|
유방 | dict | 5 | |
| 시술 | reduction mammoplasty
|
유방성형술 | dict | 1 | |
| 해부 | breast progenitor cell
|
scispacy | 1 | ||
| 해부 | breast progenitor cells
|
scispacy | 1 | ||
| 해부 | tissues
|
scispacy | 1 | ||
| 해부 | cell populations
|
scispacy | 1 | ||
| 해부 | epithelium
|
scispacy | 1 | ||
| 해부 | MECs
|
scispacy | 1 | ||
| 해부 | MEC
→ mammary epithelial cells
|
scispacy | 1 | ||
| 해부 | lineage-committed progenitor cells
|
scispacy | 1 | ||
| 해부 | progenitor
|
scispacy | 1 | ||
| 해부 | ductal progenitor cells
|
scispacy | 1 | ||
| 해부 | acinar progenitor cells
|
scispacy | 1 | ||
| 해부 | mammary
|
유방 | dict | 1 | |
| 합병증 | acinar colony
|
scispacy | 1 | ||
| 약물 | MEC
→ mammary epithelial cells
|
scispacy | 1 | ||
| 약물 | estrogen
|
C0014939
estrogens
|
scispacy | 1 | |
| 약물 | progesterone
|
C0033308
progesterone
|
scispacy | 1 | |
| 약물 | luminal
|
C0524462
Luminal region
|
scispacy | 1 | |
| 약물 | [BACKGROUND]
|
scispacy | 1 | ||
| 약물 | [RESULTS] Growth
|
scispacy | 1 | ||
| 약물 | [CONCLUSIONS]
|
scispacy | 1 | ||
| 질환 | shLRP6
|
scispacy | 1 | ||
| 질환 | MEC
→ mammary epithelial cells
|
scispacy | 1 | ||
| 질환 | luminal acinar
|
scispacy | 1 | ||
| 질환 | basal ductal colonies
|
scispacy | 1 | ||
| 질환 | MECs
|
scispacy | 1 | ||
| 질환 | ductal colonies
|
scispacy | 1 | ||
| 질환 | acinar colonies
|
scispacy | 1 | ||
| 질환 | shLRP6 MEC
|
scispacy | 1 | ||
| 기타 | Human breast progenitor cell
|
scispacy | 1 | ||
| 기타 | WNT
|
scispacy | 1 | ||
| 기타 | TBX3
|
scispacy | 1 | ||
| 기타 | human breast
|
scispacy | 1 | ||
| 기타 | human mammary epithelial cells
|
scispacy | 1 | ||
| 기타 | lentivirus
|
scispacy | 1 | ||
| 기타 | WNT1
|
scispacy | 1 | ||
| 기타 | collagen
|
scispacy | 1 | ||
| 기타 | shTBX3
|
scispacy | 1 | ||
| 기타 | shLRP6
|
scispacy | 1 |
MeSH Terms
Animals; Breast; Cell Line, Tumor; Cell Proliferation; Collagen; Epithelial Cells; Estrogens; Female; Humans; Lentivirus; Ligands; Low Density Lipoprotein Receptor-Related Protein-6; Mice; Mice, Inbred NOD; Mice, SCID; Phenotype; Primary Cell Culture; Progesterone; RNA, Small Interfering; Signal Transduction; Stem Cells; T-Box Domain Proteins; Wnt Proteins
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