Document detail
ID
doi:10.1186/s12864-024-10354-7...
Author
Quintanilha, Julia C.F. Sibley, Alexander B. Liu, Yingmiao Niedzwiecki, Donna Halabi, Susan Rogers, Layne O’Neil, Bert Kindler, Hedy Kelly, William Venook, Alan McLeod, Howard L. Ratain, Mark J. Nixon, Andrew B. Innocenti, Federico Owzar, KourosLangue
enEditor
BioMed Central
Category
Life Sciences
Year
2024
listing date
5/15/2024
Keywords
cancer common germline variation genome-wide analysis study circulating protein biomarkers protein quantitative trait loci inflammatory markers angiogenesis markers tgf-2 long non-coding rna prostate levels markers calgb analysis cis study circulating protein cancerAbstract
Background Herein, we report results from a genome-wide study conducted to identify protein quantitative trait loci (pQTL) for circulating angiogenic and inflammatory protein markers in patients with metastatic colorectal cancer (mCRC).
The study was conducted using genotype, protein marker, and baseline clinical and demographic data from CALGB/SWOG 80405 (Alliance), a randomized phase III study designed to assess outcomes of adding VEGF or EGFR inhibitors to systemic chemotherapy in mCRC patients.
Germline DNA derived from blood was genotyped on whole-genome array platforms.
The abundance of protein markers was quantified using a multiplex enzyme-linked immunosorbent assay from plasma derived from peripheral venous blood collected at baseline.
A robust rank-based method was used to assess the statistical significance of each variant and protein pair against a strict genome-wide level.
A given pQTL was tested for validation in two external datasets of prostate (CALGB 90401) and pancreatic cancer (CALGB 80303) patients.
Bioinformatics analyses were conducted to further establish biological bases for these findings.
Results The final analysis was carried out based on data from 540,021 common typed genetic variants and 23 protein markers from 869 genetically estimated European patients with mCRC.
Correcting for multiple testing, the analysis discovered a novel cis -pQTL in LINC02869 , a long non-coding RNA gene, for circulating TGF- β 2 levels (rs11118119; AAF = 0.11; P -value < 1.4e-14).
This finding was validated in a cohort of 538 prostate cancer patients from CALGB 90401 (AAF = 0.10, P -value < 3.3e-25).
The analysis also validated a cis -pQTL we had previously reported for VEGF-A in advanced pancreatic cancer, and additionally identified trans -pQTLs for VEGF-R3, and cis -pQTLs for CD73.
Conclusions This study has provided evidence of a novel cis germline genetic variant that regulates circulating TGF- β 2 levels in plasma of patients with advanced mCRC and prostate cancer.
Moreover, the validation of previously identified pQTLs for VEGF-A, CD73, and VEGF-R3, potentiates the validity of these associations.
Quintanilha, Julia C.F.,Sibley, Alexander B.,Liu, Yingmiao,Niedzwiecki, Donna,Halabi, Susan,Rogers, Layne,O’Neil, Bert,Kindler, Hedy,Kelly, William,Venook, Alan,McLeod, Howard L.,Ratain, Mark J.,Nixon, Andrew B.,Innocenti, Federico,Owzar, Kouros, 2024, Common variation in a long non-coding RNA gene modulates variation of circulating TGF-β2 levels in metastatic colorectal cancer patients (Alliance), BioMed Central
Projection-Specific Heterogeneity of the Axon Initial Segment of Pyramidal Neurons in the Prelimbic Cortex
heterogeneity projection-specific
