Immune profiles and DNA methylation alterations related with non-muscle-invasive bladder cancer outcomes

Chen, Ji-Qing; Salas, Lucas A.; Wiencke, John K.; Koestler, Devin C.; Andrew, Angeline S.; Seigne, John D.; Kelsey, Karl T.; Christensen, Brock C.

doi:10.1186/s13148-022-01234-6

Cited by 16 publications

(16 citation statements)

References 89 publications

(62 reference statements)

Supporting

Mentioning

Contrasting

Order By: Relevance

“…2), and therefore either its expression, DNA methylation, or copy number, or a combination of these factors may contribute to drug response. The direction of correlations in our analysis of cell line data was consistent with earlier reports of associations of increased BLCAP protein expression and lower BLCAP promoter methylation with inferior survival of bladder cancer patients [142,143]. Earlier studies showed that BLCAP expression involves different transcripts which are expressed in a promoter-specific and tissue-specific manner and that the BLCAP transcript expressed in human fetal brain is imprinted, with predominantly maternal expression [140].…”

Section: Discussionsupporting

confidence: 90%

“…The lack of association of genes in that region with survival of AML patients may be explained by multiple factors, e.g., weak to modest associations of individual genes which were associated with drug response, complex drug treatment regimens of the patients involved in the study, and genetic and clinical heterogeneity of the study patients [46]. Some effects of the genes at 20q11-q13.32 analyzed in this study may be tumor-specific, as suggested by the findings of Moreira et al [142] and Chen et al [143] of associations of BLCAP protein expression and promoter methylation levels with survival of bladder cancer patients, which were consistent with our analysis of drug response in pancancer cell lines. Similarly, Anwar et al [37] reported an association of survival of hepatocellular carcinoma patients with increased methylation of several of the same imprinted genes and imprinted gene regions (GNAS at 20q13.32, the DLK1-DIO3 cluster at 14q32.2-q32.31, and ZIM3 at 19q13.43) in primary tumor samples, which were also associated with increased drug sensitivity in our pancancer analysis of tumor cell lines (Additional file 9: Table S6).…”

Section: Discussionmentioning

confidence: 59%

See 1 more Smart Citation

Increased copy number of imprinted genes in the chromosomal region 20q11-q13.32 is associated with resistance to antitumor agents in cancer cell lines

et al. 2022

View full text Add to dashboard Cite

Background Parent of origin-specific allelic expression of imprinted genes is epigenetically controlled. In cancer, imprinted genes undergo both genomic and epigenomic alterations, including frequent copy number changes. We investigated whether copy number loss or gain of imprinted genes in cancer cell lines is associated with response to chemotherapy treatment. Results We analyzed 198 human imprinted genes including protein-coding genes and noncoding RNA genes using data from tumor cell lines from the Cancer Cell Line Encyclopedia and Genomics of Drug Sensitivity in Cancer datasets. We examined whether copy number of the imprinted genes in 35 different genome locations was associated with response to cancer drug treatment. We also analyzed associations of pretreatment expression and DNA methylation of imprinted genes with drug response. Higher copy number of BLCAP, GNAS, NNAT, GNAS-AS1, HM13, MIR296, MIR298, and PSIMCT-1 in the chromosomal region 20q11-q13.32 was associated with resistance to multiple antitumor agents. Increased expression of BLCAP and HM13 was also associated with drug resistance, whereas higher methylation of gene regions of BLCAP, NNAT, SGK2, and GNAS was associated with drug sensitivity. While expression and methylation of imprinted genes in several other chromosomal regions was also associated with drug response and many imprinted genes in different chromosomal locations showed a considerable copy number variation, only imprinted genes at 20q11-q13.32 had a consistent association of their copy number with drug response. Copy number values among the imprinted genes in the 20q11-q13.32 region were strongly correlated. They were also correlated with the copy number of cancer-related non-imprinted genes MYBL2, AURKA, and ZNF217 in that chromosomal region. Expression of genes at 20q11-q13.32 was associated with ex vivo drug response in primary tumor samples from the Beat AML 1.0 acute myeloid leukemia patient cohort. Association of the increased copy number of the 20q11-q13.32 region with drug resistance may be complex and could involve multiple genes. Conclusions Copy number of imprinted and non-imprinted genes in the chromosomal region 20q11-q13.32 was associated with cancer drug resistance. The genes in this chromosomal region may have a modulating effect on tumor response to chemotherapy.

show abstract

Section: Discussionsupporting

confidence: 90%

Section: Discussionmentioning

confidence: 59%

Increased copy number of imprinted genes in the chromosomal region 20q11-q13.32 is associated with resistance to antitumor agents in cancer cell lines

et al. 2022

View full text Add to dashboard Cite

show abstract

“…Specifically in human blood, our previous research employed differentially methylated regions identified between purified leukocyte subtypes to develop a reference‐based deconvolution algorithm, allowing estimation of the distribution of various leukocyte subtypes (Salas et al., 2022). This blood deconvolution approach has been utilized to investigate altered immune cell composition in multiple diseases, such as cancer (Chen et al., 2022, 2023), hypertension (Kresovich et al., 2023), and trisomy 21 (Zhang, Stolrow, et al., 2023).…”

Section: Introductionmentioning

confidence: 99%

Deciphering the role of immune cell composition in epigenetic age acceleration: Insights from cell‐type deconvolution applied to human blood epigenetic clocks

Zhang,

Reynolds,

Stolrow

et al. 2023

Aging Cell

Self Cite

View full text Add to dashboard Cite

Aging is a significant risk factor for various human disorders, and DNA methylation clocks have emerged as powerful tools for estimating biological age and predicting health‐related outcomes. Methylation data from blood DNA has been a focus of more recently developed DNA methylation clocks. However, the impact of immune cell composition on epigenetic age acceleration (EAA) remains unclear as only some clocks incorporate partial cell type composition information when analyzing EAA. We investigated associations of 12 immune cell types measured by cell‐type deconvolution with EAA predicted by six widely‐used DNA methylation clocks in data from >10,000 blood samples. We observed significant associations of immune cell composition with EAA for all six clocks tested. Across the clocks, nine or more of the 12 cell types tested exhibited significant associations with EAA. Higher memory lymphocyte subtype proportions were associated with increased EAA, and naïve lymphocyte subtypes were associated with decreased EAA. To demonstrate the potential confounding of EAA by immune cell composition, we applied EAA in rheumatoid arthritis. Our research maps immune cell type contributions to EAA in human blood and offers opportunities to adjust for immune cell composition in EAA studies to a significantly more granular level. Understanding associations of EAA with immune profiles has implications for the interpretation of epigenetic age and its relevance in aging and disease research. Our detailed map of immune cell type contributions serves as a resource for studies utilizing epigenetic clocks across diverse research fields, including aging‐related diseases, precision medicine, and therapeutic interventions.

show abstract

“…Considering this, we sought to ask whether blood immune profiles are altered at baseline and to what extent alterations may be attributed to dexamethasone exposure or tumor subtype prior to surgical resection. Here we estimated leukocyte subtypes using a validated methylation deconvolution method that has an improved accuracy over previous deconvolution methods [ 4 , 13 , 15 , 18 ], has been applied in other studies [ 4 , 19 ] and whose approach has compared favorably to other methods [ 20 ].. We show for the first time that pre-surgery immune subset profiles vary by glioma subtype; most notably, compared with other glioma subtypes, patients with IDHwt GBM had lower levels of all immune subsets except neutrophils, which were higher. We show that immune subsets were higher, except neutrophils which were lower, in controls than in glioma patients.…”

Section: Discussionmentioning

confidence: 99%

Pre-surgery immune profiles of adult glioma patients

Bracci¹,

Rice

Hansen

et al. 2022

J Neurooncol

Self Cite

View full text Add to dashboard Cite

Introduction Although immunosuppression is a known characteristic of glioma, no previous large studies have reported peripheral blood immune cell profiles prior to patient surgery and chemoradiation. This report describes blood immune cell characteristics and associated variables prior to surgery among typical glioma patients seen at a large University practice. Methods We analyzed pre-surgery blood samples from 139 glioma patients diagnosed with a new or recurrent grade II/III glioma (LrGG, n = 64) or new glioblastoma (GBM, n = 75) and 454 control participants without glioma. Relative cell fractions of CD4, CD8, B-cells, Natural Killer cells, monocytes, and neutrophils, were estimated via a validated deconvolution algorithm from blood DNA methylation measures from Illumina EPIC arrays. Results Dexamethasone use at time of blood draw varied by glioma type being highest among patients with IDH wild-type (wt) GBM (75%) and lowest for those with oligodendroglioma (14%). Compared to controls, glioma patients showed statistically significant lower cell fractions for all immune cell subsets except for neutrophils which were higher (all p-values < 0.001), in part because of the higher prevalence of dexamethasone use at time of blood draw for IDHwt GBM. Patients who were taking dexamethasone were more likely to have a low CD4 count (< 200, < 500), increased neutrophils, low absolute lymphocyte counts, higher total cell count and higher NLR. Conclusion We show that pre-surgery blood immune profiles vary by glioma subtype, age, and more critically, by use of dexamethasone. Our results highlight the importance of considering dexamethasone exposures in all studies of immune profiles and of obtaining immune measures prior to use of dexamethasone, if possible.

show abstract

Immune profiles and DNA methylation alterations related with non-muscle-invasive bladder cancer outcomes

Cited by 16 publications

References 89 publications

Increased copy number of imprinted genes in the chromosomal region 20q11-q13.32 is associated with resistance to antitumor agents in cancer cell lines

Increased copy number of imprinted genes in the chromosomal region 20q11-q13.32 is associated with resistance to antitumor agents in cancer cell lines

Deciphering the role of immune cell composition in epigenetic age acceleration: Insights from cell‐type deconvolution applied to human blood epigenetic clocks

Pre-surgery immune profiles of adult glioma patients

Contact Info

Product

Resources

About