Fusion of old and new: Employing touch imprint slides for next generation sequencing in solid tumors

Author:

Aydin Mericoz Cisel1ORCID,Eren Ozgur Can123ORCID,Kulac Ibrahim14ORCID,Firat Pinar1

Affiliation:

1. Department of Pathology Koç University School of Medicine Istanbul Turkey

2. Department of Immunology, Graduate School of Health Sciences Koç University Istanbul Turkey

3. Koç University IsBank Research Center for Infectious Diseases Istanbul Turkey

4. Research Center for Translational Medicine Koç University Istanbul Turkey

Abstract

AbstractBackgroundCytomorphological evaluation of tissue touch imprints during rapid on‐site evaluation or intraoperative pathology consultation has crucial value. However, literature on their utility for molecular testing is limited. In this study, we emphasize a further benefit of touch imprint slides and scrutinize our institutional experience on their use in molecular testing, specifically next generation sequencing (NGS).Materials and MethodsNGS‐based reports (2019–2023) of Koç University Hospital were retrospectively analyzed and circumstances in which sequencing was conducted on touch imprint slides were retrieved (n = 18). Type/location of the biopsy, diagnosis, results, and quality metrics were recorded.ResultsTouch imprints were addressed when they harbored more neoplastic cells compared with permanent biopsies, when suboptimal fixation mitigated deoxyribonucleic acid/ribonucleic acid (DNA/RNA) yield in resections or when the sample was obtained from bone and required decalcification. Diagnoses were diverse, namely non‐small‐cell lung cancer, gastric adenocarcinoma, glial tumor, Ewing sarcoma, and carcinoma of unknown primary. The percentage of tumor cells on slides stretched between 15% and 70%. Molecular findings ranged from KRAS mutations to TRIM1::NTRK2 and EWSR::FLI1 fusions. For five cases, sequencing did not yield any alteration, one study was not completed because it did not yield high‐quality RNA.ConclusionTouch imprint slides provide a reliable alternative, especially when neoplastic cells are scarce in permanent biopsies or decalcification deters nucleic acid quality. Based on our experience, we suggest making touch imprints on a routine basis, especially for every bone biopsy. Once digitally scanned duplicates are made, original slides can be safely used for DNA‐/RNA‐based molecular studies.

Publisher

Wiley

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