Expanding the Prostate Cancer Cell Line Repertoire with ACRJ-PC28, an AR-negative Neuroendocrine Cell Line Derived From an African-Caribbean Patient

Prostate cancer cell lines from diverse backgrounds are important to addressing disparities in prostate cancer incidence and mortality rates among Black men. ACRJ-PC28 was developed from a transrectal needle biopsy and established via inactivation of the CDKN2A locus and simultaneous expression of h...

Descripción completa

Detalles Bibliográficos
Autores principales: Valentine, Henkel, Aiken, William, Morrison, Belinda, Zhao, Ziran, Fowle, Holly, Wasserman, Jason S., Thompson, Elon, Chin, Warren, Young, Mark, Clarke, Shannique, Gibbs, Denise, Harrison, Sharon, McLaughlin, Wayne, Kwok, Tim, Jin, Fang, Campbell, Kerry S., Horvath, Anelia, Thompson, Rory, Lee, Norman H., Zhou, Yan, Graña, Xavier, Ragin, Camille, Badal, Simone
Formato: Online Artículo Texto
Lenguaje:English
Publicado: American Association for Cancer Research 2022
Materias:
Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9836004/
https://www.ncbi.nlm.nih.gov/pubmed/36643868
http://dx.doi.org/10.1158/2767-9764.CRC-22-0245
_version_ 1784868776571830272
author Valentine, Henkel
Aiken, William
Morrison, Belinda
Zhao, Ziran
Fowle, Holly
Wasserman, Jason S.
Thompson, Elon
Chin, Warren
Young, Mark
Clarke, Shannique
Gibbs, Denise
Harrison, Sharon
McLaughlin, Wayne
Kwok, Tim
Jin, Fang
Campbell, Kerry S.
Horvath, Anelia
Thompson, Rory
Lee, Norman H.
Zhou, Yan
Graña, Xavier
Ragin, Camille
Badal, Simone
author_facet Valentine, Henkel
Aiken, William
Morrison, Belinda
Zhao, Ziran
Fowle, Holly
Wasserman, Jason S.
Thompson, Elon
Chin, Warren
Young, Mark
Clarke, Shannique
Gibbs, Denise
Harrison, Sharon
McLaughlin, Wayne
Kwok, Tim
Jin, Fang
Campbell, Kerry S.
Horvath, Anelia
Thompson, Rory
Lee, Norman H.
Zhou, Yan
Graña, Xavier
Ragin, Camille
Badal, Simone
author_sort Valentine, Henkel
collection PubMed
description Prostate cancer cell lines from diverse backgrounds are important to addressing disparities in prostate cancer incidence and mortality rates among Black men. ACRJ-PC28 was developed from a transrectal needle biopsy and established via inactivation of the CDKN2A locus and simultaneous expression of human telomerase. Characterization assays included growth curve analysis, immunoblots, IHC, three-dimensional cultures, immunofluorescence imaging, confocal microscopy, flow cytometry, whole-genome sequencing (WGS), and RNA sequencing (RNA-seq). ACRJ-PC28 has been passaged more than 40 times in vitro over 10 months with a doubling time of 45 hours. Short tandem repeat profiling confirmed the novelty and human origin of the cell line. RNA-seq confirmed the expression of prostate specific genes alpha-methylacyl-CoA racemase (AMACR) and NKX3.1 and neuroendocrine specific markers synaptophysin and enolase 2 (ENO2) and IHC confirmed the presence of AMACR. Immunoblots indicated the cell line is of basal-luminal type; expresses p53 and pRB and is androgen receptor (AR) negative. WGS confirmed the absence of exonic mutations and the presence of intronic variants that appear to not affect function of AR, p53, and pRB. RNA-seq data revealed numerous TP53 and RB1 mRNA splice variants and the lack of AR mRNA expression. This is consistent with retention of p53 function in response to DNA damage and pRB function in response to contact inhibition. Soft agar anchorage-independent analysis indicated that the cells are transformed, confirmed by principal component analysis where ACRJ-PC28 cells cluster alongside other prostate cancer tumor tissues, yet was distinct. The novel methodology described should advance prostate cell line development, addressing the disparity in prostate cancer among Black men. SIGNIFICANCE: Cell line development continues to attract less than 10% success rate. More than 98% of prostate cancer cell lines are from White men. This may contribute to the poorer response by Black men with prostate cancer to therapy compared with White men with prostate cancer, increasing overall survivorship among White men. The methodology described here to develop ACRJ-PC28, should advance the presence of Black prostate cancer cell lines thereby addressing prostate cancer disparity.
format Online
Article
Text
id pubmed-9836004
institution National Center for Biotechnology Information
language English
publishDate 2022
publisher American Association for Cancer Research
record_format MEDLINE/PubMed
spelling pubmed-98360042023-01-12 Expanding the Prostate Cancer Cell Line Repertoire with ACRJ-PC28, an AR-negative Neuroendocrine Cell Line Derived From an African-Caribbean Patient Valentine, Henkel Aiken, William Morrison, Belinda Zhao, Ziran Fowle, Holly Wasserman, Jason S. Thompson, Elon Chin, Warren Young, Mark Clarke, Shannique Gibbs, Denise Harrison, Sharon McLaughlin, Wayne Kwok, Tim Jin, Fang Campbell, Kerry S. Horvath, Anelia Thompson, Rory Lee, Norman H. Zhou, Yan Graña, Xavier Ragin, Camille Badal, Simone Cancer Res Commun Research Article Prostate cancer cell lines from diverse backgrounds are important to addressing disparities in prostate cancer incidence and mortality rates among Black men. ACRJ-PC28 was developed from a transrectal needle biopsy and established via inactivation of the CDKN2A locus and simultaneous expression of human telomerase. Characterization assays included growth curve analysis, immunoblots, IHC, three-dimensional cultures, immunofluorescence imaging, confocal microscopy, flow cytometry, whole-genome sequencing (WGS), and RNA sequencing (RNA-seq). ACRJ-PC28 has been passaged more than 40 times in vitro over 10 months with a doubling time of 45 hours. Short tandem repeat profiling confirmed the novelty and human origin of the cell line. RNA-seq confirmed the expression of prostate specific genes alpha-methylacyl-CoA racemase (AMACR) and NKX3.1 and neuroendocrine specific markers synaptophysin and enolase 2 (ENO2) and IHC confirmed the presence of AMACR. Immunoblots indicated the cell line is of basal-luminal type; expresses p53 and pRB and is androgen receptor (AR) negative. WGS confirmed the absence of exonic mutations and the presence of intronic variants that appear to not affect function of AR, p53, and pRB. RNA-seq data revealed numerous TP53 and RB1 mRNA splice variants and the lack of AR mRNA expression. This is consistent with retention of p53 function in response to DNA damage and pRB function in response to contact inhibition. Soft agar anchorage-independent analysis indicated that the cells are transformed, confirmed by principal component analysis where ACRJ-PC28 cells cluster alongside other prostate cancer tumor tissues, yet was distinct. The novel methodology described should advance prostate cell line development, addressing the disparity in prostate cancer among Black men. SIGNIFICANCE: Cell line development continues to attract less than 10% success rate. More than 98% of prostate cancer cell lines are from White men. This may contribute to the poorer response by Black men with prostate cancer to therapy compared with White men with prostate cancer, increasing overall survivorship among White men. The methodology described here to develop ACRJ-PC28, should advance the presence of Black prostate cancer cell lines thereby addressing prostate cancer disparity. American Association for Cancer Research 2022-11-07 /pmc/articles/PMC9836004/ /pubmed/36643868 http://dx.doi.org/10.1158/2767-9764.CRC-22-0245 Text en © 2022 The Authors; Published by the American Association for Cancer Research https://creativecommons.org/licenses/by/4.0/This open access article is distributed under the Creative Commons Attribution 4.0 International (CC BY 4.0) license.
spellingShingle Research Article
Valentine, Henkel
Aiken, William
Morrison, Belinda
Zhao, Ziran
Fowle, Holly
Wasserman, Jason S.
Thompson, Elon
Chin, Warren
Young, Mark
Clarke, Shannique
Gibbs, Denise
Harrison, Sharon
McLaughlin, Wayne
Kwok, Tim
Jin, Fang
Campbell, Kerry S.
Horvath, Anelia
Thompson, Rory
Lee, Norman H.
Zhou, Yan
Graña, Xavier
Ragin, Camille
Badal, Simone
Expanding the Prostate Cancer Cell Line Repertoire with ACRJ-PC28, an AR-negative Neuroendocrine Cell Line Derived From an African-Caribbean Patient
title Expanding the Prostate Cancer Cell Line Repertoire with ACRJ-PC28, an AR-negative Neuroendocrine Cell Line Derived From an African-Caribbean Patient
title_full Expanding the Prostate Cancer Cell Line Repertoire with ACRJ-PC28, an AR-negative Neuroendocrine Cell Line Derived From an African-Caribbean Patient
title_fullStr Expanding the Prostate Cancer Cell Line Repertoire with ACRJ-PC28, an AR-negative Neuroendocrine Cell Line Derived From an African-Caribbean Patient
title_full_unstemmed Expanding the Prostate Cancer Cell Line Repertoire with ACRJ-PC28, an AR-negative Neuroendocrine Cell Line Derived From an African-Caribbean Patient
title_short Expanding the Prostate Cancer Cell Line Repertoire with ACRJ-PC28, an AR-negative Neuroendocrine Cell Line Derived From an African-Caribbean Patient
title_sort expanding the prostate cancer cell line repertoire with acrj-pc28, an ar-negative neuroendocrine cell line derived from an african-caribbean patient
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9836004/
https://www.ncbi.nlm.nih.gov/pubmed/36643868
http://dx.doi.org/10.1158/2767-9764.CRC-22-0245
work_keys_str_mv AT valentinehenkel expandingtheprostatecancercelllinerepertoirewithacrjpc28anarnegativeneuroendocrinecelllinederivedfromanafricancaribbeanpatient
AT aikenwilliam expandingtheprostatecancercelllinerepertoirewithacrjpc28anarnegativeneuroendocrinecelllinederivedfromanafricancaribbeanpatient
AT morrisonbelinda expandingtheprostatecancercelllinerepertoirewithacrjpc28anarnegativeneuroendocrinecelllinederivedfromanafricancaribbeanpatient
AT zhaoziran expandingtheprostatecancercelllinerepertoirewithacrjpc28anarnegativeneuroendocrinecelllinederivedfromanafricancaribbeanpatient
AT fowleholly expandingtheprostatecancercelllinerepertoirewithacrjpc28anarnegativeneuroendocrinecelllinederivedfromanafricancaribbeanpatient
AT wassermanjasons expandingtheprostatecancercelllinerepertoirewithacrjpc28anarnegativeneuroendocrinecelllinederivedfromanafricancaribbeanpatient
AT thompsonelon expandingtheprostatecancercelllinerepertoirewithacrjpc28anarnegativeneuroendocrinecelllinederivedfromanafricancaribbeanpatient
AT chinwarren expandingtheprostatecancercelllinerepertoirewithacrjpc28anarnegativeneuroendocrinecelllinederivedfromanafricancaribbeanpatient
AT youngmark expandingtheprostatecancercelllinerepertoirewithacrjpc28anarnegativeneuroendocrinecelllinederivedfromanafricancaribbeanpatient
AT clarkeshannique expandingtheprostatecancercelllinerepertoirewithacrjpc28anarnegativeneuroendocrinecelllinederivedfromanafricancaribbeanpatient
AT gibbsdenise expandingtheprostatecancercelllinerepertoirewithacrjpc28anarnegativeneuroendocrinecelllinederivedfromanafricancaribbeanpatient
AT harrisonsharon expandingtheprostatecancercelllinerepertoirewithacrjpc28anarnegativeneuroendocrinecelllinederivedfromanafricancaribbeanpatient
AT mclaughlinwayne expandingtheprostatecancercelllinerepertoirewithacrjpc28anarnegativeneuroendocrinecelllinederivedfromanafricancaribbeanpatient
AT kwoktim expandingtheprostatecancercelllinerepertoirewithacrjpc28anarnegativeneuroendocrinecelllinederivedfromanafricancaribbeanpatient
AT jinfang expandingtheprostatecancercelllinerepertoirewithacrjpc28anarnegativeneuroendocrinecelllinederivedfromanafricancaribbeanpatient
AT campbellkerrys expandingtheprostatecancercelllinerepertoirewithacrjpc28anarnegativeneuroendocrinecelllinederivedfromanafricancaribbeanpatient
AT horvathanelia expandingtheprostatecancercelllinerepertoirewithacrjpc28anarnegativeneuroendocrinecelllinederivedfromanafricancaribbeanpatient
AT thompsonrory expandingtheprostatecancercelllinerepertoirewithacrjpc28anarnegativeneuroendocrinecelllinederivedfromanafricancaribbeanpatient
AT leenormanh expandingtheprostatecancercelllinerepertoirewithacrjpc28anarnegativeneuroendocrinecelllinederivedfromanafricancaribbeanpatient
AT zhouyan expandingtheprostatecancercelllinerepertoirewithacrjpc28anarnegativeneuroendocrinecelllinederivedfromanafricancaribbeanpatient
AT granaxavier expandingtheprostatecancercelllinerepertoirewithacrjpc28anarnegativeneuroendocrinecelllinederivedfromanafricancaribbeanpatient
AT ragincamille expandingtheprostatecancercelllinerepertoirewithacrjpc28anarnegativeneuroendocrinecelllinederivedfromanafricancaribbeanpatient
AT badalsimone expandingtheprostatecancercelllinerepertoirewithacrjpc28anarnegativeneuroendocrinecelllinederivedfromanafricancaribbeanpatient

Ejemplares similares