Recapitulation of prostate tissue cell type-specific transcriptomes by an in vivo primary prostate tissue xenograft model

Gross, Nelson T.; Wang, Jianmin; Fiandalo, Michael V.; Gomez, Eduardo Cortes; Watts, Anica; Godoy, Alejandro; Smith, Gary J.; Wu, Yue

doi:10.1371/journal.pone.0233899

Cited by 2 publications

(2 citation statements)

References 85 publications

(103 reference statements)

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“…Therefore, the race-specific associations of genetic variations in SLCO2A1 and SLCO5A1 are aligned with both transporters being the predominant SLCO transporters expressed in prostate cancer tissue, and their cell type-specific expression in prostate cancer endothelial cells and epithelial cells. The cell type-specific expression of SLCO2A1 and SLCO5A1 in prostate tissue is supported by our recent report of RNA sequencing data generated from prostate epithelial cells and endothelial cells isolated from fresh clinical specimens of prostate tissue (38). However, knowledge on the biological functions and substrates of SLCO2A1 and SLCO5A1 in human prostate tissue is scant.…”

Section: Discussionmentioning

confidence: 89%

Differential Associations of SLCO Transporters with Prostate Cancer Aggressiveness between African Americans and European Americans

Tang

Zhu

Wang

et al. 2021

Cancer Epidemiology, Biomarkers &Amp; Prevention

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Background: Androgen receptor signaling is crucial to prostate cancer aggressiveness. Members of the solute carrier family of the organic anion transporting peptides (SLCO) are potential regulators of androgen availability in prostate tissue. It remains unknown whether genetic variations in SLCOs contribute to the differences in prostate cancer aggressiveness in African Americans (AA) and European Americans (EA).Methods: SNPs in 11 SLCO members were selected, with addition of 139 potentially functional SNPs and 128 ancestry informative markers. A total of 1,045 SNPs were genotyped and analyzed in 993 AAs and 1,057 EAs from the North Carolina-Louisiana Prostate Cancer Project. Expression and cellular localization of SLCOs were examined using qRT-PCR, IHC, and in situ RNA hybridization in independent sets of prostate cancer cases.Results: Significant associations with prostate cancer characteristics were found for SNPs in SLCO2A1 and SLCO5A1. The associations differed by race (P interaction < 0.05). SNPs in SLCO2A1 were associated with reduced tumor aggressiveness and low Gleason score in AAs; whereas, SNPs in SLCO5A1 were associated with high clinical stage in EAs. In prostate tissue, SLCO2A1 and SLCO5A1 were the most expressed SLCOs at the mRNA level and were expressed predominantly in prostate endothelial and epithelial cells at the protein level, respectively.Conclusions: SLCO2A1 and SLCO5A1 play important but different roles in prostate cancer aggressiveness in AAs versus EAs.Impact: The finding calls for consideration of racial differences in biomarker studies of prostate cancer and for investigations on functions of SLCO2A1 and SLCO5A1 in prostate cancer.

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Section: Discussionmentioning

confidence: 89%

Differential Associations of SLCO Transporters with Prostate Cancer Aggressiveness between African Americans and European Americans

Tang

Zhu

Wang

et al. 2021

Cancer Epidemiology, Biomarkers &Amp; Prevention

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“…On immunofluorescence, there were significantly more blood vessels in orthotopic prostate tumors compared to subcutaneous tumors. These data indicate that the microenvironment at the orthotopic site and cellular-environmental interaction facilitated tumorigenesis of LNCaP cells ( 29 ).…”

Section: Discussionmentioning

confidence: 92%

Comparison of tumor angiogenesis in subcutaneous and orthotopic LNCaP mouse models using contrast-enhanced ultrasound imaging

Liu¹,

Zhu²,

Ye³

et al. 2021

Transl Cancer Res TCR

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Background: Understanding angiogenesis in prostate cancer is essential. LNCaP prostate xenograft tumors are androgen responsive and closely mimic clinical disease. Orthotopic animal models replicate aspects of the cancer microenvironment and are more clinically relevant than subcutaneous models.Comparative studies investigating angiogenesis using contrast-enhanced ultrasound (CEUS) imaging in subcutaneous and orthotopic mouse models of prostate cancer have not been performed.Methods: Tumor microcirculation and perfusion in subcutaneous and orthotopic LNCaP xenograft Balb/c athymic nude mice models were compared by investigating microbubble wash-in with CEUS. Results:The take rate of subcutaneous and orthotopic tumors were 58.3% and 68.2%, respectively.On CEUS, orthotopic prostate tumors enhanced more rapidly than subcutaneous tumors. Mean arrivaltime (Atm) for subcutaneous tumors, orthotopic prostate tumors, and kidney were 4.21±1.86, 1.72±0.79, and 0.73±0.12 s, respectively. Mean Atm was significantly longer for subcutaneous tumors compared to orthotopic prostate tumors or kidney (P<0.01). Mean time to peak enhancement (TtoPk) for subcutaneous tumors, orthotopic prostate tumors, and kidney were 38.56±13.23, 12.39±7.17, and 3.74±1.41 s, respectively. Mean TtoPk were significantly shorter for orthotopic prostate tumors and kidney compared to subcutaneous tumors (P<0.01). Mean wash-in area under the curve (WiAuC) for subcutaneous tumors, orthotopic

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Recapitulation of prostate tissue cell type-specific transcriptomes by an in vivo primary prostate tissue xenograft model

Cited by 2 publications

References 85 publications

Differential Associations of SLCO Transporters with Prostate Cancer Aggressiveness between African Americans and European Americans

Differential Associations of SLCO Transporters with Prostate Cancer Aggressiveness between African Americans and European Americans

Comparison of tumor angiogenesis in subcutaneous and orthotopic LNCaP mouse models using contrast-enhanced ultrasound imaging

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