HMGA2 is regulated by LIN28 and BRCA1 in human placental cells†

West, Rachel C.; McWhorter, Erin S.; Ali, Asghar; Goetzman, L N; Russ, Jennifer E.; Gonzalez-Berrios, C L; Anthony, Russell V.; Bouma, Gerrit J.; Winger, Quinton A.

doi:10.1093/biolre/ioy183

Cited by 16 publications

(42 citation statements)

References 45 publications

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“…Furthermore, knockdown of LIN28B resulted in significantly increased levels of let‐7c, e,f, and g . This is similar to West et al (), showing let‐7c was higher in LIN28B KD cells, although it was not statistically significant. To determine if AR possibly is regulated by let‐7′s, ACH‐3P cells were transfected with synthetic let‐7 mimics.…”

Section: Discussionsupporting

confidence: 89%

“…Specifically, knockdown of LIN28A in mouse trophoblast stem cells leads to their differentiation into trophoblast giant cells, whereas LIN28A knockdown in ACH‐3P cells leads to increased syncytialization (Seabrook et al, ). Because then, we found that LIN28B in fact is the predominant LIN28 homolog expressed in human first‐trimester placenta, localized to the cytotrophoblast cells, and present in commonly used human trophoblast cell lines (West et al, ). This was also recently confirmed by Canfield et al ().…”

Section: Discussionmentioning

confidence: 96%

“…Similar to LIN28B, AR is not present in the differentiated syncytiotrophoblast layer, which is positive for hCG, but appears to localize to trophoblast cells right beneath the syncytiotrophoblast layer. These possibly are cytotrophoblast cells, based on a similar localization pattern as LIN28B (West et al, ). Furthermore, AR is localized to the stromal cells confirming previous reports describing AR localization to the decidua and villous stromal cells (Horie et al, ; Yoshida, Ikeda, & Aihara, ).…”

Section: Discussionmentioning

confidence: 98%

“…Knockdown of LIN28B in ACH‐3P cells leads to differentiation towards syncytiotrophoblast, with increased levels of ERVW‐1 and secretion of hCG (West et al, ). This study revealed that knockdown of LIN28B leads to significantly lower levels of AR mRNA and protein, suggesting LIN28B either directly or through let‐7 miRNAs regulates AR abundance in trophoblast cells.…”

Section: Discussionmentioning

confidence: 99%

“…This is contrary to our previous observation when LIN28A was knocked down in ACH‐3P cells, which revealed an increase in LGALS13 (Seabrook et al, ). However, complete abolishment of both LIN28A and LIN28B in ACH‐3P cells also leads to a decrease in LGALS13 (West et al, ), suggesting regulation of this gene is more complex, which is not surprising considering its localization in not only syncytiotrophoblast but also extravillous trophoblast.…”

Section: Discussionmentioning

confidence: 99%

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LIN28B regulates androgen receptor in human trophoblast cells through Let‐7c

McWhorter

West

Russ

et al. 2019

Molecular Reproduction Devel

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LIN28B is an RNA‐binding protein necessary for maintaining pluripotency in stem cells and plays an important role in trophoblast cell differentiation. LIN28B action on target gene function often involves the Let‐7 miRNA family. Previous work in cancer cells revealed that LIN28 through Let‐7 miRNA regulates expression of androgen receptor (AR). Considering the similarities between cancer and trophoblast cells, we hypothesize that LIN28B also is necessary for the presence of AR in human trophoblast cells. The human first‐trimester trophoblast cell line, ACH‐3P was used to evaluate the regulation of AR by LIN28B, and a LIN28B knockdown cell line was constructed using lentiviral‐based vectors. LIN28B knockdown in ACH‐3P cells resulted in significantly decreased levels of AR and increased levels of Let‐7 miRNAs. Moreover, treatment of ACH‐3P cells with Let‐7c mimic, but not Let‐7e or Let‐7f, resulted in a significant reduction in LIN28B and AR. Finally, forskolin‐induced syncytialization and Let‐7c treatment both resulted in increased expression of syncytiotrophoblast marker ERVW‐1 and a significant decrease in AR in ACH‐3P. These data reveal that LIN28B regulates AR levels in trophoblast cells likely through its inhibitory actions on let‐7c, which may be necessary for trophoblast cell differentiation into the syncytiotrophoblast.

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Section: Discussionsupporting

confidence: 89%

Section: Discussionmentioning

confidence: 96%

Section: Discussionmentioning

confidence: 98%

Section: Discussionmentioning

confidence: 99%

Section: Discussionmentioning

confidence: 99%

See 3 more Smart Citations

LIN28B regulates androgen receptor in human trophoblast cells through Let‐7c

McWhorter

West

Russ

et al. 2019

Molecular Reproduction Devel

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BRCA1 regulates HMGA2 levels in the Swan71 trophoblast cell line

West

Russ

Bouma

et al. 2019

Molecular Reproduction Devel

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During early placental development, tumor suppressors and oncogenes work synergistically to regulate cell proliferation and differentiation in a restrained manner compared with the uncontrollable growth in cancer. One example of this partnership is the regulation of the oncofetal protein HMGA2 by BRCA1. BRCA1 forms a repressor complex with ZNF350 and CtIP to bind to the promoter of HMGA2, preventing transcription. Chromatin immunoprecipitation determined BRCA1 forms this repressor complex in human trophoblast cells, suggesting a role in the placenta. Furthermore, miR‐182 has been shown to target BRCA1 mRNA in ovarian cancer cells, blocking the formation of the BRCA1 repressor complex and allowing increased transcription of HMGA2. miR‐182 was one of the first miRNAs described as elevated in the serum and placentas of preeclamptic women. Therefore, we hypothesized that BRCA1 is essential for normal trophoblast cell development. We used CRISPR‐Cas9 genome editing and miR‐182 overexpression to decrease BRCA1 protein in the Swan71 cell line. HMGA2 was significantly increased in the BRCA1 KO and miR‐182 overexpressing cells compared to controls. We also determined that BRCA1 repressor complex binding to HMGA2 was significantly reduced in BRCA1 KO and miR‐182 overexpressing cells compared with controls, leading us to conclude that increased HMGA2 was because of decreased binding of the BRCA1 repressor complex. Finally, we found that the caspase activity was significantly higher in BRCA1 KO and miR‐182 overexpressing cells suggesting an increased amount of apoptosis. These data suggest that BRCA1 is an important regulator of the oncofetal protein HMGA2 and promotes cell survival in human placental cells.

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