Identification of Differentially Methylated Genes in Normal Prostate Tissues from African American and Caucasian Men

Kwabi-Addo, Bernard; Wang, Songping; Chung, Woonbok; Jelı́nek, Jaroslav; Patierno, Steven R.; Wang, Bi-Dar; Andrawis, Ramez; Lee, Norman H.; Apprey, Victor; Issa, Jean–Pierre J.; Ittmann, Michael

doi:10.1158/1078-0432.ccr-09-3342

Cited by 119 publications

(117 citation statements)

References 23 publications

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“…Additional logistic regression analysis of our data suggests that the difference in specificity can be correlated, in part, with subject age and ethnicity. This is intriguing, as it has been previously reported that DNA methylation patterns for some genes depend on both subject age and ethnicity (33 ).…”

Section: Discussionmentioning

confidence: 86%

Validation of a Real-Time PCR–Based Qualitative Assay for the Detection of Methylated SEPT9 DNA in Human Plasma

et al. 2014

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Section: Discussionmentioning

confidence: 86%

Validation of a Real-Time PCR–Based Qualitative Assay for the Detection of Methylated SEPT9 DNA in Human Plasma

et al. 2014

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“…The studies that involved unbiased screening by gene expression analysis have shown SPARC expression to be correlated with high-grade, androgen-resistant, and metastatic disease. In addition, SPARC was shown previously to attract prostate cancer cells into bone by promoting a migratory and invasive phenotype (39 -42 (48) have shown that SPARC is silenced by promoter methylation in African-American patients who often develop aggressive prostate cancer with 2-fold higher mortality rate than Caucasian American patients (48). The apparent disagreement between these studies may be due to multiple factors, including expression profiling of the primary tumor, batch variability, and lack of clinical data for the site of metastasis.…”

Section: Discussionmentioning

confidence: 99%

Secreted Protein Acidic and Rich in Cysteine (SPARC) Mediates Metastatic Dormancy of Prostate Cancer in Bone

Sharma

Xing

Yin

et al. 2016

Journal of Biological Chemistry

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Prostate cancer is known to frequently recur in bone; however, how dormant cells switch its phenotype leading to recurrent tumor remains poorly understood. We have isolated two syngeneic cell lines (indolent and aggressive) through in vivo selection by implanting PC3mm stem-like cells into tibial bones. We found that indolent cells retained the dormant phenotype, whereas aggressive cells grew rapidly in bone in vivo, and the growth rates of both cells in culture were similar, suggesting a role of the tumor microenvironment in the regulation of dormancy and recurrence. Indolent cells were found to secrete a high level of secreted protein acidic and rich in cysteine (SPARC), which significantly stimulated the expression of BMP7 in bone marrow stromal cells. The secreted BMP7 then kept cancer cells in a dormant state by inducing senescence, reducing "stemness," and activating dormancy-associated p38 MAPK signaling and p21 expression in cancer cells. Importantly, we found that SPARC was epigenetically silenced in aggressive cells by promoter methylation, but 5-azacytidine treatment reactivated the expression. Furthermore, high SPARC promoter methylation negatively correlated with disease-free survival of prostate cancer patients. We also found that the COX2 inhibitor NS398 down-regulated DNMTs and increased expression of SPARC, which led to tumor growth suppression in bone in vivo. These findings suggest that SPARC plays a key role in maintaining the dormancy of prostate cancer cells in the bone microenvironment.

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“…9 These results are supported by differences in the specific methylation of genes such as GSTP1, AR, RAR beta2, SPARC, TIMP3 and NKX2-5 in which higher methylation was found in African-Americans than in Caucasian-Americans. 10 The methylation differences found in adulthood could potentially be contributed by neonatal imprinting, as demonstrated in our early studies where we showed that both the growth of sex steroid-sensitive organs and their steroidmetabolizing enzymes in the target organs were affected by prior exposure of animals to testosterone or 17-b-estradiol during the neonatal period. [11][12][13] In addition to the report cited above characterizing racial/ethnic differences in prostate cancer among AfricanAmericans, Caucasian-Americans, Chinese and Japanese, numerous other attempts have been made to characterize the differences among Americans, Europeans, Africans and other Asian races.…”

mentioning

confidence: 74%

Interracial differences in prostate cancer progression among patients from the United States, China and Japan

Zhau¹,

Li²,

Chung³

2013

Asian J Androl

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Identification of Differentially Methylated Genes in Normal Prostate Tissues from African American and Caucasian Men

Cited by 119 publications

References 23 publications

Validation of a Real-Time PCR–Based Qualitative Assay for the Detection of Methylated SEPT9 DNA in Human Plasma

Validation of a Real-Time PCR–Based Qualitative Assay for the Detection of Methylated SEPT9 DNA in Human Plasma

Secreted Protein Acidic and Rich in Cysteine (SPARC) Mediates Metastatic Dormancy of Prostate Cancer in Bone

Interracial differences in prostate cancer progression among patients from the United States, China and Japan

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