研究发现了一种分子谱,可以区分家族性腺瘤性息肉病(FAP)和不完全型家族性腺瘤性息肉病(AFAP)患者正常结肠组织。通过对FAP和AFAP患者的基因表达分析,确定了48个具有统计显著性的mRNA探针,这些探针在FAP和AFAP中表现出不同的表达模式,可能用于诊断。此外,还识别出一组基因可以区分具有相同APC突变但息肉数量不同的AFAP个体,揭示了表型差异的可能原因。
Background
Familial adenomatous polyposis (FAP) is a colon cancer syndrome with a prevalence of 1:10,000. Patients have 100's to 1000's of precancerous colonic polyps and nearly 100% risk of developing colon cancer at an average age of 39 years in the absence of colon surveillance and surgery. Mutations in the APC gene lead to FAP as well as an attenuated form (AFAP) which presents with variable phenotypic expression, reduced polyp numbers and reduced cancer risk as compared to FAP. Current methods for the clinical diagnosis of genetic diseases most commonly involve analysis of germline DNA. Germline DNA-based diagnosis can be incomplete, for example no mutation is found in approximately 20% of FAP and 50% of AFAP patients. The objective of this study is to determine a molecular profile of the colonic epithelia from patients with APC mutations leading to FAP or AFAP then to use this information to establish a gene expression signature for diagnosis and for better understanding of the disease in the primary affected tissue.Methods
Fresh normal-appearing colonic epithelia were obtained as biopsies during endoscopy and immediately placed in RNA-later, a tissue preservative for RNA integrity. RNA was extracted using Qiagen RNeasy purification system. Aglient 44K RNA microarrays were run using mRNA from FAP patients (n=6), AFAP patients (n=14) and control patients (n=12). Normalized log ratios for each sample vs. reference RNA were the input for analysis using the Rank Product to generate a p-value for significance of differential expression and to cluster using Ward's Method in the Spotire DecisionSite software.Results
Analysis using the Rank Product method found 48 mRNA probes with statistical significance (p<0.001) that consistently distinguish between control, FAP and AFAP normal appearing colonic tissue. These probes are up in FAP vs. control but low in AFAP vs. control or vice versa and will be tested for their accuracy to classify FAP and AFAP patients. Differential expression was also evaluated to better understand the phenotypic variability within AFAP using 5 individuals with> 100 adenomas versus 6 individuals with < 20 adenomas with the identical APC mutation. Differential expression identified 245 probes with a p-value of <0.05. The most striking were DEFA5 and DEFA6, encoding microbicidal defensins involved in host defense, which consistently showed increased expression in the >100 adenoma group. It is not clear if this reflects a host or an environmental difference and will require further study.Conclusions
In conclusion, a distinct gene expression signature can be identified in FAP vs. AFAP patients that, in turn, can be applied to diagnostics. A separate set of genes can also distinguish colonic phenotypic classes of individuals with the identical APC mutation and may suggest secondary factors that modify the phenotypic penetrance in AFAP.
Acknowledgement
This research was funded by NIH grants ROl-CA040641 (RWB) and P01-CA07392 and Huntsman Cancer Foundation.Author information
Affiliations2000 Circle of Hope, Huntsman Cancer Institute, University of Utah, Salt Lake City, Utah, 84112-5550, USA
Deborah W Neklason, Brett A Milash, Therese M Tuohy, Jennifer Lilley & Randall W Burt
AuthorsDeborah W Neklason
Brett A Milash
Therese M Tuohy
Jennifer Lilley
Randall W Burt
Corresponding author
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Deborah W Neklason.Rights and permissions
Open Access This article is published under license to BioMed Central Ltd. This is an Open Access article is distributed under the terms of the Creative Commons Attribution 2.0 International License (https://creativecommons.org/licenses/by/2.0), which permits unrestricted use, distribution, and reproduction in any medium, provided the original work is properly cited.About this article
Cite this article
Neklason, D.W., Milash, B.A., Tuohy, T.M. et al. Differential gene expression in primary colonic tissue from control, FAP and AFAP patients reveals unique signatures with diagnostic potential.
Hered Cancer Clin Pract 8,P13 (2010). https://doi.org/10.1186/1897-4287-8-S1-P13
KeywordsAdenoma
Familial Adenomatous Polyposis
Gene Expression Signature
Colonic Epithelium
Familial Adenomatous Polyposis Patient
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