1. Filter Paper–based Nucleic Acid Storage in High-throughput Solid Tumor Genotyping
- Author
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Lynette M. Sholl, Janina A. Longtine, Yonghui Jia, Nematullah Sharaf, Matthew D. Stachler, Jacqueline E. Wade, and Elizabeth P. Garcia
- Subjects
Paper ,Lung Neoplasms ,Tissue Fixation ,Histology ,Genotype ,Genotyping Techniques ,Adenocarcinoma ,Diamines ,Biology ,Pathology and Forensic Medicine ,chemistry.chemical_compound ,Formaldehyde ,Humans ,Tissue Collection ,Benzothiazoles ,Organic Chemicals ,Fragmentation (cell biology) ,Solid tumor ,Genotyping ,Fluorescent Dyes ,Reagent Strips ,Tissue Embedding ,Filter paper ,DNA, Neoplasm ,Molecular biology ,Kidney Neoplasms ,High-Throughput Screening Assays ,Pancreatic Neoplasms ,Medical Laboratory Technology ,chemistry ,Colonic Neoplasms ,Carcinoma, Squamous Cell ,Quinolines ,Fresh frozen ,Nucleic acid ,DNA - Abstract
Molecular testing of tumors from formalin-fixed paraffin-embedded (FFPE) tissue blocks is central to clinical practice; however, it requires histology support and increases test turnaround time. Prospective fresh frozen tissue collection requires special handling, additional storage space, and may not be feasible for small specimens. Filter paper-based collection of tumor DNA reduces the need for histology support, requires little storage space, and preserves high-quality nucleic acid. We investigated the performance of tumor smears on filter paper in solid tumor genotyping, as compared with paired FFPE samples. Whatman FTA Micro Card (FTA preps) smears were prepared from 21 fresh tumor samples. A corresponding cytology smear was used to assess tumor cellularity and necrosis. DNA was isolated from FTA preps and FFPE core samples using automated methods and quantified using SYBR green dsDNA detection. Samples were genotyped for 471 mutations on a mass spectrophotometry-based platform (Sequenom). DNA concentrations from FTA preps and FFPE correlated for untreated carcinomas but not for mesenchymal tumors (Spearman σ=0.39 and σ=-0.1, respectively). Average DNA concentrations were lower from FTA preps as compared with FFPE, but DNA quality was higher with less fragmentation. Seventy-six percent of FTA preps and 86% of FFPE samples generated adequate DNA for genotyping. FTA preps tended to perform poorly for collection of DNA from pretreated carcinomas and mesenchymal neoplasms. Of the 16 paired DNA samples that were genotyped, 15 (94%) gave entirely concordant results. Filter paper-based sample preservation is a feasible alternative to FFPE for use in automated, high-throughput genotyping of carcinomas.
- Published
- 2015