Loss of anti-proliferative effect of all-trans retinoic acid in advanced stage of breast carcinogenesis.
Abstract
[BACKGROUND] Mechanisms by which the inhibitory effect of retinoic acid on tumor growth is attenuated as tumors progress to more advanced stages are unclear.
[MATERIALS AND METHODS] This study utilizes a novel cell culture system of human breast epithelial cells (HBEC). Immortal (M13SV1), weakly tumorigenic (M13SV1-R2), and highly tumorigenic (M13SV1-R2N1) transformed Type I HBEC were derived sequentially from the same parental Type I HBEC (stem cells) developed from reduction mammoplasty of healthy women. Effects of all-trans retinoic acid (AT-RA) on the growth, protein expression of RAR-alpha, beta and gamma, and RARE transcriptional activation were determined.
[RESULTS AND CONCLUSION] AT-RA reduces proliferation rates of immortal and weakly tumorigenic cells, but not highly tumorigenic cells. This loss of response of highly tumorigenic cells to AT-RA is associated with overexpression of p185(c-erbB2/neu). It is not associated with decreased RAR-alpha, beta or gamma expression, or activation by AT-RA; RAR-alpha, beta and gamma are expressed and AT-RA increases RARE transcriptional activity in all cell lines tested in this study.
[MATERIALS AND METHODS] This study utilizes a novel cell culture system of human breast epithelial cells (HBEC). Immortal (M13SV1), weakly tumorigenic (M13SV1-R2), and highly tumorigenic (M13SV1-R2N1) transformed Type I HBEC were derived sequentially from the same parental Type I HBEC (stem cells) developed from reduction mammoplasty of healthy women. Effects of all-trans retinoic acid (AT-RA) on the growth, protein expression of RAR-alpha, beta and gamma, and RARE transcriptional activation were determined.
[RESULTS AND CONCLUSION] AT-RA reduces proliferation rates of immortal and weakly tumorigenic cells, but not highly tumorigenic cells. This loss of response of highly tumorigenic cells to AT-RA is associated with overexpression of p185(c-erbB2/neu). It is not associated with decreased RAR-alpha, beta or gamma expression, or activation by AT-RA; RAR-alpha, beta and gamma are expressed and AT-RA increases RARE transcriptional activity in all cell lines tested in this study.
추출된 의학 개체 (NER)
| 유형 | 영어 표현 | 한국어 / 풀이 | UMLS CUI | 출처 | 등장 |
|---|---|---|---|---|---|
| 해부 | breast
|
유방 | dict | 2 | |
| 시술 | reduction mammoplasty
|
유방성형술 | dict | 1 | |
| 해부 | cell
|
scispacy | 1 | ||
| 해부 | HBEC
→ human breast epithelial cells
|
scispacy | 1 | ||
| 해부 | M13SV1
|
scispacy | 1 | ||
| 해부 | stem cells
|
scispacy | 1 | ||
| 해부 | cells
|
scispacy | 1 | ||
| 해부 | cell lines
|
scispacy | 1 | ||
| 약물 | all-trans retinoic acid
|
C0040845
tretinoin
|
scispacy | 1 | |
| 약물 | retinoic acid
|
C0040845
tretinoin
|
scispacy | 1 | |
| 약물 | AT-RA
→ all-trans retinoic acid
|
C0040845
tretinoin
|
scispacy | 1 | |
| 약물 | [BACKGROUND]
|
scispacy | 1 | ||
| 약물 | [RESULTS AND
|
scispacy | 1 | ||
| 질환 | breast carcinogenesis
|
scispacy | 1 | ||
| 질환 | tumor
|
C0027651
Neoplasms
|
scispacy | 1 | |
| 질환 | tumors
|
C0027651
Neoplasms
|
scispacy | 1 | |
| 질환 | M13SV1-R2
|
scispacy | 1 | ||
| 질환 | M13SV1-R2N1
|
scispacy | 1 | ||
| 기타 | human breast epithelial cells
|
scispacy | 1 | ||
| 기타 | Type I
|
scispacy | 1 | ||
| 기타 | women
|
scispacy | 1 | ||
| 기타 | RAR-alpha
|
scispacy | 1 | ||
| 기타 | beta and
|
scispacy | 1 | ||
| 기타 | RARE
|
scispacy | 1 | ||
| 기타 | beta or gamma
|
scispacy | 1 | ||
| 기타 | beta and gamma
|
scispacy | 1 |
MeSH Terms
Antineoplastic Agents; Breast Neoplasms; Cell Proliferation; Cell Transformation, Neoplastic; Cells, Cultured; Female; Gene Expression Regulation, Neoplastic; Humans; Immunoblotting; Luciferases; Erb-b2 Receptor Tyrosine Kinases; Receptors, Retinoic Acid; Regulatory Elements, Transcriptional; Retinoic Acid Receptor alpha; Transcriptional Activation; Tretinoin; Retinoic Acid Receptor gamma
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