Your search keyword '"Lynch syndrome"' showing total 10,408 results

201. Mismatch Repair Screening of Gastrointestinal Cancers: The Impact on Lynch Syndrome Detection and Immunotherapy.

Author

R., Openshaw M., J., Williams, T., Foo, C., Moss, A., Wotherspoon, N., Starling., and Z., Kemp

Abstract

Introduction: Mismatch repair immunohistochemistry (MMR IHC) or microsatellite instability (MSI) testing is now routinely performed in patients with colorectal cancer (CRC) to select those requiring Lynch syndrome testing. MMR IHC is also carried out on CRC and upper gastrointestinal (GI) cancers to select patients for immunotherapy. We review the Royal Marsden Hospital's pathway of molecular to germline testing for Lynch syndrome in the context of NICE guidance and the National Test Directory. Methods: We conducted (i) a retrospective audit of adherence to NICE guidance DG27 for patients diagnosed with CRC March 2017–August 2018 and (ii) a retrospective service evaluation of MMR IHC/Lynch syndrome testing in patients diagnosed with upper GI cancers January 2019–2020. Results: Of 394 patients with CRC, 346 (87.8%) had MMR IHC testing. Thirty-eight of 346 (10.9%) were MMR deficient (MMR-D) and 5 (1.4%) were found to have pathogenic germline variants causing Lynch syndrome. Of 405 patients with upper GI cancers, 221 (54.6%) had MMR IHC testing. Ten of 221 (4.5%) were MMR-D and 1 (0.5%) had a pathogenic germline variant causing Lynch syndrome. Discussion: This study highlights the small but significant number of patients, with CRC or upper GI cancers, which were caused by Lynch syndrome. It also highlights weaknesses in our testing pathway that limit access to germline testing. As MMR testing increases, it is important that clinicians are aware that patients with MMR-D tumours require reflex somatic testing or referral for germline testing. We have incorporated the guidelines into a pathway for use in clinics and multidisciplinary teams. [ABSTRACT FROM AUTHOR]

Published

2023

202. Testung auf Mismatch-Reparatur-Defizienz und Mikrosatelliteninstabilität: Eine fokussierte Aktualisierung.

Author

Rüschoff, Josef, Schildhaus, Hans-Ulrich, Rüschoff, Jan Hendrik, Jöhrens, Korinna, Bocker-Edmonston, Tina, Dietmaier, Wolfgang, Bläker, Hendrik, Baretton, Gustavo, Horst, David, Dietel, Manfred, Hartmann, Arndt, Klauschen, Frederick, Merkelbach-Bruse, Sabine, Stenzinger, Albrecht, Schöniger, Sandra, Tiemann, Markus, Weichert, Wilko, and Büttner, Reinhard

Abstract

Copyright of Die Pathologie is the property of Springer Nature and its content may not be copied or emailed to multiple sites or posted to a listserv without the copyright holder's express written permission. However, users may print, download, or email articles for individual use. This abstract may be abridged. No warranty is given about the accuracy of the copy. Users should refer to the original published version of the material for the full abstract. (Copyright applies to all Abstracts.)

Published

2023

203. Hereditäre kolorektale Karzinogenese.

Author

Bläker, Hendrik

Abstract

Copyright of Die Pathologie is the property of Springer Nature and its content may not be copied or emailed to multiple sites or posted to a listserv without the copyright holder's express written permission. However, users may print, download, or email articles for individual use. This abstract may be abridged. No warranty is given about the accuracy of the copy. Users should refer to the original published version of the material for the full abstract. (Copyright applies to all Abstracts.)

Published

2023

204. Serum matrix metalloproteinase-7: a potential biomarker in patients with Lynch Syndrome.

Author

Yablecovitch, Doron, Mahajna, Hussein, Horesh, Nir, Katz, Efraim, Picard, Orit, Yavzori, Miri, Fudim, Ella, Saker, Talia, Ben-Horin, Shomron, and Laish, Ido

Abstract

Background and aims: The expression of tissue and serum matrix metalloproteinase-7 (MMP-7) was shown to be elevated both in colon cancer and dysplastic lesions. We aimed to evaluate, for the first time, its role as a diagnostic marker in Lynch syndrome (LS) carriers, a hereditary syndrome with predisposition to colon cancer. Methods: This was a case control study. Baseline serum MMP-7 levels were determined by ELISA in 40 colon cancer patients, 62 LS-carriers and 60 healthy controls. Retrieved data from medical files included demographics, background diseases, clinical data regarding tumor characteristics and genetic data. We assessed the association of serum MMP-7 levels with different variables in the study cohort using linear regression model adjusted for potential confounders. Results: In crude analysis, serum MMP-7 levels were significantly higher in colon cancer group compared to LS-carriers and controls [median (IQR) 4.1 ng/ml (2.7–6.0), 2.3 ng/ml (1.7–3.1), 2.5 ng/ml (1.5–3.7), respectively; p value - p < 0.001) while there was no difference between the two last groups (p value = 0.583). However, after adjusting for age and gender, LS-carriers' patients had 18% higher concentrations of serum MMP-7 compared to healthy controls (p value = 0.037), while colon cancer patients had 50% higher serum MMP-7 level in comparison to healthy controls (p value < 0.001). Additionally, age was positively associated with higher serum MMP-7 levels across all study groups (r = 0.67, p value < 0.001). In contrast, no correlation was observed between serum MMP-7 and either tumor staging and gene mutation. Conclusions: Age-adjusted serum MMP-7 levels in asymptomatic LS carriers are higher than its levels in healthy population. While in colon cancer, MMP-7 higher level probably reflects the tumor burden and may have a prognostic effect, its significance and clinical applicability as a biomarker for tumorigenesis in LS is less clear and should be elucidated. [ABSTRACT FROM AUTHOR]

Published

2023

205. BRAFV600E/RAS Mutations and Lynch Syndrome in Patients With MSI-H/dMMR Metastatic Colorectal Cancer Treated With Immune Checkpoint Inhibitors.

Author

Colle, Raphael, Lonardi, Sara, Cachanado, Marine, Overman, Michael J, Elez, Elena, Fakih, Marwan, Corti, Francesca, Jayachandran, Priya, Svrcek, Magali, Dardenne, Antoine, Cervantes, Baptiste, Duval, Alex, Cohen, Romain, Pietrantonio, Filippo, and André, Thierry

Subjects

RESEARCH, GENETIC mutation, IMMUNE checkpoint inhibitors, CONFIDENCE intervals, HEREDITARY nonpolyposis colorectal cancer, COLORECTAL cancer, GENE expression, DESCRIPTIVE statistics, AMINO acids, PROGRESSION-free survival, LONGITUDINAL method, OVERALL survival

Abstract

Background : We pooled data from 2 cohorts of immune checkpoint inhibitors-treated microsatellite instability-high/mismatch repair-deficient (MSI/dMMR) metastatic colorectal cancer patients to evaluate the prognostic value of RAS/BRAFV600E mutations and Lynch syndrome (LS). Patients and Methods: Patients were defined as LS-linked if germline mutation was detected and as sporadic if loss of MLH1/PMS2 expression with BRAFV600E mutation and/or MLH1 promoter hypermethylation, or biallelic somatic MMR genes mutations were found. Progression-free survival (PFS) and overall survival (OS) were adjusted on prognostic modifiers selected on unadjusted analysis (P <.2) if limited number of events. Results: Of 466 included patients, 305 (65.4%) and 161 (34.5%) received, respectively, anti-PD1 alone and anti-PD1+anti-CTLA4 in the total population, 111 (24.0%) were treated in first-line; 129 (28.8%) were BRAFV600E-mutated and 153 (32.8%) RAS-mutated. Median follow-up was 20.9 months. In adjusted analysis of the whole population (PFS/OS events = 186/133), no associations with PFS and OS were observed for BRAFV600E-mutated (PFS HR= 1.20, P =.372; OS HR = 1.06, P =.811) and RAS-mutated patients (PFS HR = 0.93, P =.712, OS HR = 0.75, P =.202). In adjusted analysis in the Lynch/sporadic status-assigned population (n = 242; PFS/OS events = 80/54), LS-liked patients had an improved PFS compared to sporadic cases (HR = 0.49, P =.036). The adjusted HR for OS was 0.56 with no significance (P =.143). No adjustment on BRAFV600E mutation was done due to collinearity. Conclusion: In this cohort, RAS/BRAFV600E mutations were not associated with survival while LS conferred an improved PFS. Using data from 2 cohorts of patients with MSI/dMMR metastatic colorectal cancer treated with immune checkpoint inhibitors, this study evaluated the prognostic value of RAS/BRAFV600E mutations and Lynch syndrome. [ABSTRACT FROM AUTHOR]

Published

2023

206. Insertion of an SVA element in MSH2 as a novel cause of Lynch syndrome.

Author

Yang, Ciyu, Li, Yirong, Trottier, Magan, Farrell, Michael, Rai, Vikas, E Salo-Mullen, Erin, Gallagher, David, Stadler, Zsofia, van der Klift, Heleen, and Zhang, Liying

Subjects

Lynch syndrome, MSH2, SVA, germline, Alu Elements, Colorectal Neoplasms, Hereditary Nonpolyposis, Humans, Male, Middle Aged, Minisatellite Repeats, MutS Homolog 2 Protein

Abstract

Germline mutations in the DNA mismatch repair (MMR) genes cause Lynch syndrome (LS). In this study, we identified and characterized a novel SINE-VNTR-Alu (SVA) insertion in exon 12 of MSH2 in an individual with early-onset colorectal cancer and a very strong LS family history. RT-PCR analysis indicated a larger aberrant MSH2 transcript in one of the family members. MSK-IMPACT next-generation sequencing and long-range PCR analyses revealed an insertion in MSH2 exon 12 at the c.1972 position in an antisense orientation. The insertion was further characterized as an SVA element approximately 3 kb in length, belonging to the SVA_F1 family of retrotransposons. This variant also segregated with LS related cancers in four affected family members in this family. Based on this evidence, this MSH2 SVA insertion is considered pathogenic.

Published

2021

207. Mismatch repair protein deficiency in endometriosis: Precursor of endometriosis-associated ovarian cancer in women with lynch syndrome

Author

Munekage Yamaguchi, Yoshiki Mikami, Maki Kusunoki, Saori Yoshimura, Takeshi Motohara, and Eiji Kondoh

Subjects

Lynch syndrome, Endometriosis-associated ovarian cancer, Mismatch repair protein deficiency, Ovarian endometriosis, Gynecology and obstetrics, RG1-991

Abstract

Objective: We aimed to elucidate the pathogenesis of ovarian cancer through the loss of mismatch repair (MMR) proteins in women with Lynch syndrome (LS) in this report. Case report: Two women with LS underwent surgery for synchronous endometrial cancer and ovarian cancer. In both cases, immunohistochemical examination showed concomitant MMR protein deficiency in endometrial cancer, ovarian cancer, and contiguous ovarian endometriosis. In Case 1, the macroscopically normal ovary included multiple endometrioses with MSH2 and MSH6 expression, and FIGO grade 1 endometrioid carcinoma and contiguous endometriosis without MSH2 and MSH6 expression. In Case 2, all endometriotic cells contiguous with carcinoma in the lumen of the ovarian cyst showed loss of the expression of MSH2 and MSH6. Conclusion: Ovarian endometriosis with MMR protein deficiency may progress to endometriosis-associated ovarian cancer in women with LS. Diagnosing endometriosis in women with LS during surveillance is important.

Published

2023

208. Exceptional Response to Pembrolizumab for Treatment of Metastatic Chemorefractory Endometrial Carcinoma in a Patient with Lynch Syndrome: A Case Report

Author

Samantha Batman, J. Alejandro Rauh-Hain, Michaela Onstad Grinsfelder, Ross Harrison, Monica Avila, Han Cun, Jeffrey Andrew How, Nidhi Tandon, Xiaohong Wang, Emily Hinchcliff, Amir Anthony Jazaeri, and Kathleen M. Schmeler

Subjects

pembrolizumab, advanced endometrial cancer, lynch syndrome, Neoplasms. Tumors. Oncology. Including cancer and carcinogens, RC254-282

Abstract

Advanced endometrial cancer is associated with poor outcomes and few treatment options exist. Recently, the US Federal Drug Administration approved pembrolizumab for the treatment of endometrial cancers that are deficient in mismatch repair and have high microsatellite instability (MSI). Lynch syndrome is an autosomal dominant disease that causes MSI-high endometrial cancer. We report a case of a 46-year-old woman with Lynch syndrome and advanced endometrial cancer who experienced progressive disease after treatment with chemotherapy with carboplatin and paclitaxel. She was then treated with single-agent pembrolizumab and had an exceptional response. She was noted to have a significant decrease in the size of a large uterine mass extending into the vagina and vulva, as well as decrease in the size of lymphadenopathy. Data are limited at this time for patients with Lynch syndrome treated with single-agent pembrolizumab. Our case report seeks to add to the body of literature that suggests that this patient population may particularly benefit from this novel therapy.

Published

2023

209. A tumor focused approach to resolving the etiology of DNA mismatch repair deficient tumors classified as suspected Lynch syndrome

Author

Romy Walker, Khalid Mahmood, Jihoon E. Joo, Mark Clendenning, Peter Georgeson, Julia Como, Sharelle Joseland, Susan G. Preston, Yoland Antill, Rachel Austin, Alex Boussioutas, Michelle Bowman, Jo Burke, Ainsley Campbell, Simin Daneshvar, Emma Edwards, Margaret Gleeson, Annabel Goodwin, Marion T. Harris, Alex Henderson, Megan Higgins, John L. Hopper, Ryan A. Hutchinson, Emilia Ip, Joanne Isbister, Kais Kasem, Helen Marfan, Di Milnes, Annabelle Ng, Cassandra Nichols, Shona O’Connell, Nicholas Pachter, Bernard J. Pope, Nicola Poplawski, Abiramy Ragunathan, Courtney Smyth, Allan Spigelman, Kirsty Storey, Rachel Susman, Jessica A. Taylor, Linda Warwick, Mathilda Wilding, Rachel Williams, Aung K. Win, Michael D. Walsh, Finlay A. Macrae, Mark A. Jenkins, Christophe Rosty, Ingrid M. Winship, Daniel D. Buchanan, and for the Family Cancer Clinics of Australia

Subjects

Suspected Lynch syndrome, DNA mismatch repair deficiency, Colorectal cancer, Endometrial cancer, Sebaceous skin tumor, Lynch syndrome, Medicine

Abstract

Abstract Routine screening of tumors for DNA mismatch repair (MMR) deficiency (dMMR) in colorectal (CRC), endometrial (EC) and sebaceous skin (SST) tumors leads to a significant proportion of unresolved cases classified as suspected Lynch syndrome (SLS). SLS cases (n = 135) were recruited from Family Cancer Clinics across Australia and New Zealand. Targeted panel sequencing was performed on tumor (n = 137; 80×CRCs, 33×ECs and 24xSSTs) and matched blood-derived DNA to assess for microsatellite instability status, tumor mutation burden, COSMIC tumor mutational signatures and to identify germline and somatic MMR gene variants. MMR immunohistochemistry (IHC) and MLH1 promoter methylation were repeated. In total, 86.9% of the 137 SLS tumors could be resolved into established subtypes. For 22.6% of these resolved SLS cases, primary MLH1 epimutations (2.2%) as well as previously undetected germline MMR pathogenic variants (1.5%), tumor MLH1 methylation (13.1%) or false positive dMMR IHC (5.8%) results were identified. Double somatic MMR gene mutations were the major cause of dMMR identified across each tumor type (73.9% of resolved cases, 64.2% overall, 70% of CRC, 45.5% of ECs and 70.8% of SSTs). The unresolved SLS tumors (13.1%) comprised tumors with only a single somatic (7.3%) or no somatic (5.8%) MMR gene mutations. A tumor-focused testing approach reclassified 86.9% of SLS into Lynch syndrome, sporadic dMMR or MMR-proficient cases. These findings support the incorporation of tumor sequencing and alternate MLH1 methylation assays into clinical diagnostics to reduce the number of SLS patients and provide more appropriate surveillance and screening recommendations.

Published

2023

210. A Novel MSH6 Gene Variant in a Lynch Syndrome Patient with Lipomas

Author

Ana Paula Giannoni, Ina Sevic, Fernanda Parenti, and Laura Alaniz

Subjects

MSH6, Lynch syndrome, lipomas, genetic screening, cancer risk, Medicine (General), R5-920

Abstract

Colorectal cancer is one of the most frequently occurring cancers today, with a large percentage of cases having a hereditary basis. Lynch syndrome is the most common cause of hereditary colorectal cancer. The genetic defect characteristics of this syndrome involve mutations in mismatch repair (MMR) genes, which result in microsatellite instability. Early detection of the mutation can help evaluate the cancer risk and, consequently, a proper course of clinical management for the person harboring the mutation. Herein, we describe the first report of a c.1458dup (p.Glu487*) new mutation in a 53-year-old colorectal cancer patient with diagnosed Lynch syndrome. Additionally, the existence of lipomas in this patient and his family could be related to this syndrome. Further investigation may provide a possible visual clue that can indicate a need for genetic screening.

Published

2023

211. Lynch-like Syndrome and its Molecular Approaches: A Brief Report and Literature Review

Author

Zeinab Abdollahi, Mohammad Amin Tabatabaiefar, Mohammad Hassan Emami, and Mehrdad Zeinalian

Subjects

lynch syndrome, colorectal cancer, neoplastic syndromes, hereditary, mismatch repair gene, Neoplasms. Tumors. Oncology. Including cancer and carcinogens, RC254-282

Abstract

Lynch syndrome (LS) predisposes individuals to early-onset colorectal and other Lynch-associated cancer. This disorder is an autosomal dominant genetic disturbance caused by germline mutations in one of the mismatch repair genes. Different clinical and molecular criteria are used to diagnose LS. Microsatellite instability testing and immunohistochemistry are two widely used methods for the molecular screening of LS-associated cancers. According to the immunohistochemistry and Microsatellite instability testing, we introduce three Persian families with Lynch-like syndrome (LLS) who met clinical Amsterdam-II criteria and their probands were mismatch repair deficient. In the case of immunohistochemistry-MLH1 absent, BRAF-V600E mutation was evaluated to rule out the sporadic colorectal cancer cases. No pathogenic germline variants were found by next generation sequencing method. Multiplex ligation-dependant probe amplification technique was done to find large in/dels within MLH1/MSH2 genes of the probands. A two-exon deletion within MLH1 gene was eventually identified in one of the patients. Finally, we have represented a molecular pipeline to diagnose LLS based on literature review and the introduced cases.

Published

2023

212. Double somatic mismatch repair gene pathogenic variants as common as Lynch syndrome among endometrial cancer patients

Author

Hampel, Heather, Pearlman, Rachel, de la Chapelle, Albert, Pritchard, Colin C, Zhao, Weiqiang, Jones, Dan, Yilmaz, Ahmet, Chen, Wei, Frankel, Wendy L, Suarez, Adrian A, Cosgrove, Casey, Backes, Floor, Copeland, Larry, Fowler, Jeffrey, O'Malley, David, Salani, Ritu, McElroy, Joseph P, Stanich, Peter P, Goodfellow, Paul, and Cohn, David E

Subjects

Rare Diseases, Clinical Research, Genetics, Digestive Diseases, Colo-Rectal Cancer, Cancer, Aetiology, 2.1 Biological and endogenous factors, Adult, Aged, Aged, 80 and over, Colorectal Neoplasms, Hereditary Nonpolyposis, DNA Methylation, DNA Mismatch Repair, Endometrial Neoplasms, Female, Germ-Line Mutation, Humans, Middle Aged, MutL Protein Homolog 1, Neoplasm Staging, Young Adult, Endometrial, Neoplasm, Mismatch repair, Lynch syndrome, Somatic, Double somatic, Oncology and Carcinogenesis, Paediatrics and Reproductive Medicine, Oncology & Carcinogenesis

Abstract

ObjectiveLynch syndrome is the most common cause of inherited endometrial cancer, attributable to germline pathogenic variants (PV) in mismatch repair (MMR) genes. Tumor microsatellite instability (MSI-high) and MMR IHC abnormalities are characteristics of Lynch syndrome. Double somatic MMR gene PV also cause MSI-high endometrial cancers. The aim of this study was to determine the relative frequency of Lynch syndrome and double somatic MMR PV.Methods341 endometrial cancer patients enrolled in the Ohio Colorectal Cancer Prevention Initiative at The Ohio State University Comprehensive Cancer Center from 1/1/13-12/31/16. All tumors underwent immunohistochemical (IHC) staining for the four MMR proteins, MSI testing, and MLH1 methylation testing if the tumor was MMR-deficient (dMMR). Germline genetic testing for Lynch syndrome was undertaken for all cases with dMMR tumors lacking MLH1 methylation. Tumor sequencing followed if a germline MMR gene PV was not identified.ResultsTwenty-seven percent (91/341) of tumors were either MSI-high or had abnormal IHC indicating dMMR. As expected, most dMMR tumors had MLH1 methylation; (69, 75.8% of the dMMR cases; 20.2% of total). Among the 22 (6.5%) cases with dMMR not explained by methylation, 10 (2.9% of total) were found to have Lynch syndrome (6 MSH6, 3 MSH2, 1 PMS2). Double somatic MMR PV accounted for the remaining 12 dMMR cases (3.5% of total).ConclusionsSince double somatic MMR gene PV are as common as Lynch syndrome among endometrial cancer patients, paired tumor and germline testing for patients with non-methylated dMMR tumor may be the most efficient approach for LS screening.

Published

2021

213. Lynch syndrome associated endometrial cancer : screening and novel biology

Author

Ryan, Neil, Evans, Dafydd, and Crosbie, Emma

Subjects

Microsatellite instability, Genomics, Mismatch Repair, Endometrial cancer, Lynch syndrome

Abstract

Background: Lynch syndrome (LS) is the most common inherited cause of Endometrial Cancer (EC), however testing for LS in EC is not routine. Identifying LS determines eligibility for immunotherapy trials, enables surveillance to reduce colorectal cancer deaths, and promotes cascade testing of relatives. Methods: I performed a systematic review with meta-analysis of the prevalence of LS associated EC. Next, LS testing was offered to all women presenting with EC to our institution between 2015-2017. Tumours were tested for microsatellite instability (MSI) and mismatch repair (MMR) deficiency immunohistochemistry (IHC), with MLH1 hypermethylation testing and/or germline next generation sequencing (NGS) as indicated. I assessed the acceptability of LS testing at various stages of the cancer pathway. Costs were identified using micro-costing, whereby clinical/laboratory staff time and consumables/capital equipment costs were calculated. The immunological and molecular landscape of proven LS-EC was compared to sporadic EC by IHC and NGS. Results: The systematic review included 12,633 EC cases and found 3% were LS-associated. This was supported by our prospective cohort study of 500 patients, of whom only less than 1% declined testing, when offered on the day of surgery. Consenting women for LS testing in follow-up was associated with less cancer worry. Sensitivity and specificity for microsatellite instability testing with targeted MLH1 promotor hypermethylation analysis was 62.5% and 97.3% respectively. For immunohistochemistry with targeted MLH1 promotor hypermethylation analysis the sensitivity and specificity were 100% and 98.6% respectively. Sixteen women had LS-EC, of whom only three were known to have LS. Eleven variants of unknown significance were found. Of those tumours with unexplained microsatellite instability or immunohistochemistry mismatch protein loss, 16% and 92% were found to have a somatic path_MMR mutation. The cheapest testing strategy cost just £42.01/EC. LS15 EC (n=63) had significantly higher densities of infiltrating immune cells than sporadic MMR-deficient (n=95)/proficient EC (n=402), and its distinct molecular profile reflected its unique heritage. Conclusion: Unselected testing of EC for LS is cheap, acceptable to women and by directing tailored treatment and risk-reducing interventions, will save lives. The immunological and somatic mutational landscape of LS associated EC is distinct from other etiologies of EC MMR deficiency; this should inform clinical treatment trials exploring the efficacy of checkpoint inhibition in MMR deficient cancers. These results pioneered international LS-EC guidance and opened discussion with UK policy makers.

Published

2020

214. Insertion of an Alu‐like element in MLH1 intron 7 as a novel cause of Lynch syndrome

Author

Li, Yirong, Salo‐Mullen, Erin, Varghese, Anna, Trottier, Magan, Stadler, Zsofia K, and Zhang, Liying

Subjects

Biological Sciences, Medicinal and Biomolecular Chemistry, Chemical Sciences, Genetics, Digestive Diseases, Colo-Rectal Cancer, Rare Diseases, Cancer, 2.1 Biological and endogenous factors, Aetiology, Adult, Alu Elements, Colorectal Neoplasms, Hereditary Nonpolyposis, Humans, Introns, Male, MutL Protein Homolog 1, Mutagenesis, Insertional, RNA Splicing, AluSx, Lynch syndrome, MLH1, splicing, MLH1, Clinical Sciences, Medicinal and biomolecular chemistry

Abstract

BackgroundLynch Syndrome (LS) is caused by germline mutations in the DNA mismatch repair (MMR) genes with mutations in MLH1 accounting for ~40% of LS-related alterations.MethodsMSK-IMPACT analysis was performed on peripheral blood from a patient with early- onset colorectal cancer. Subsequently PCR and sequencing was performed to characterize the insertion. Immunohistochemistry for MMR genes and MLH1 promoter methylation were analyzed on patient's tumor.ResultsMSK-IMPACT germline testing revealed an insertion into c.588+8_588+9 of MLH1 intron 7. The insertion was further characterized as an AluSx-like element with ~115 bp in length. Functional studies demonstrated that the AluSx-like element led to complete disruption of mRNA splicing and probably resulted in transcriptional termination at the poly (A) region of the AluSx-like insertion.ConclusionsThe insertion of a truncated AluSx like element into MLH1 intron 7 results in aberrant splicing and transcription, thereby causing Lynch syndrome. This study confirms that retrotransposon insertions may be an important mechanism for cancer predisposition.

Published

2020

215. Recurrent colon cancer in a patient with Muir–Torre syndrome: a case report.

Author

Rivkin, Angeline C, Bystrom, Philip, Lin, Amy Y, and Chaudhry, Vivek

Subjects

*HEREDITARY nonpolyposis colorectal cancer, *COLON cancer, *CANCER patients, *DNA mismatch repair, *COLORECTAL cancer, *SYNDROMES

Abstract

Muir–Torre syndrome (MTS) is a rare subtype of hereditary nonpolyposis colorectal cancer syndrome caused by a defect in DNA mismatch repair leading to microsatellite instability. It is characterized by the presence of at least one sebaceous gland tumor and one internal malignancy, most commonly colorectal and endometrial tumors. These patients have a high propensity for tumorigenesis, and while strict screening protocols are in place, there are only two cases that describe the management approach to recurrent colon cancer. Here, we present a case of recurrent colorectal cancer in a patient with MTS, and describe how it was managed at our facility by a multidisciplinary team. [ABSTRACT FROM AUTHOR]

Published

2024

216. Lung adenocarcinoma in a patient with Lynch syndrome: a case report and literature review

Author

Alan Hodges, Kai Sun, Tiffany G. Sheu, and Eric H. Bernicker

Subjects

Lynch syndrome, NSCLC, MLH1, immune checkpoint therapy, ctDNA, Neoplasms. Tumors. Oncology. Including cancer and carcinogens, RC254-282

Abstract

This article presents a case of a 62-year-old Vietnamese woman with a history of Lynch syndrome (LS), who developed lung adenocarcinoma with EGFR L858R mutation. LS is an autosomal dominant cancer predisposition syndrome caused by a pathogenic germline variant in DNA mismatch repair genes, often leading to microsatellite instability. While LS is primarily associated with gastrointestinal, endometrial, ovarian, and urologic tract cancers, lung cancer accounts for less than 1% of LS-related cancers, with only six cases of LS-related lung cancer previously reported in the literature. The patient underwent multiple lines of treatment for her lung adenocarcinoma, including tyrosine kinase inhibitors, stereotactic body radiation therapy, pemetrexed and pembrolizumab, amivantamab, and fam-trastuzumab deruxtecan, but all resulted in only a partial response followed by a progressive disease. This case highlights the complex interplay of genetic cancer predisposition syndromes and the development of spontaneous driver mutations in the disease course and the subsequent management of tumors arising in these patients.

Published

2023

217. From variant of unknown significance to likely pathogenic: Characterization and pathogenicity determination of a large genomic deletion in the MLH1 gene

Author

Ahmed Bouras, Clementine Legrand, Jihen Kourda, Eric Ruano, Chloé Grand‐Masson, Cedrick Lefol, and Qing Wang

Subjects

dMMR, large genomic rearrangement, Lynch syndrome, MLH1, NGS, RNA analysis, Genetics, QH426-470

Abstract

Abstract Background The MLH1 gene is one of the DNA mismatch repair genes (MMR), implicated in Lynch syndrome (LS), an autosomal dominant hereditary tumor susceptibility disease. The advent of next‐generation sequencing (NGS) technologies has accelerated the diagnosis of inherited diseases and increased the percentage of diagnosis of inherited cancers. However, some complex genomic alterations require the combination of several analytical strategies to allow correct biological interpretations. Here, we describe a novel MLH1 deletion and its pathogenicity determination in a patient suspected of LS. Methods The index case was a French 73‐year‐old man diagnosed with colorectal cancer displaying microsatellite instability and the loss of MLH1 and PMS2 expression. NGS analysis was used as the primary method for MMR genes screening. Long‐range PCR and reverse transcriptase polymerase chain reaction (RT‐PCR) were used for breakpoints and pathogenicity determinations. Results A large genomic deletion was detected which removed the last six nucleotides of MLH1 exon 11 together with a large part of intron 11. It was initially considered as a variant of unknown significance (VUS). Genomic breakpoints were subsequently characterized defining the deletion as c.1033_1039‐248del. Further RNA analysis demonstrated that this variant activated a cryptic donor splice site at the 5′ of the breakpoint, leading to a premature truncated protein: p.Thr345Alafs*13. Conclusion Our finding suggested that although NGS technologies have increased variant detection yield, combined approaches were still needed for complex variant characterization and pathogenicity assessment.

Published

2023

218. Constitutional mismatch repair deficiency syndrome with atypical features caused by a homozygous MLH1 missense variant (c.1918C>A, p.(Pro640Thr)): a case report.

Author

Akrout, Firas, Achour, Ahlem, Tops, Carli M. J., Gallon, Richard, Meddeb, Rym, Achoura, Sameh, Rekaya, Mariem Ben, Hamdeni, Emna, Rammeh, Soumaya, Chkili, Ridha, Mansouri, Nada, Belguith, Neila, and Mrad, Ridha

Subjects

HEREDITARY nonpolyposis colorectal cancer, MISSENSE mutation, GENETIC disorders, CARCINOMA, HEMATOLOGIC malignancies, SYNDROMES

Abstract

Constitutional mismatch repair deficiency (CMMRD) syndrome is a rare autosomal recessive genetic disorder caused by biallelic germline mutations in one of the mismatch repair genes. Carriers are at exceptionally high risk for developing, typically in early life, hematological and brain malignancies, as well as cancers observed in Lynch syndrome. We report a homozygous MLH1 missense variant (c.1918C>A p.(Pro640Thr)) in a Tunisian patient with CMMRD syndrome and a family history of early-age colorectal cancer. The proband presented initially with colonic oligopolyposis and adenosquamous carcinoma of the caecum. He later developed several malignancies, including undifferentiated carcinoma of the parotid, grade 4 IDH-mutant astrocytoma, and ampulla of Vater adenocarcinoma. The patient was older than typical for this disease and had a remarkably prolonged survival despite developing four distinct aggressive malignancies. The current report highlights the challenges in assessing the pathogenicity of the identified variant and the remarkable phenotypic diversity in CMMRD. [ABSTRACT FROM AUTHOR]

Published

2023

219. Immune microenvironment profiling of normal appearing colorectal mucosa biopsied over repeat patient visits reproducibly separates lynch syndrome patients based on their history of colon cancer.

Author

Brand, Rhonda M., Dudley, Beth, Karloski, Eve, Zyhowski, Ashley, Raphael, Rebecca, Pitlor, Danielle, Metter, E. Jeffrey, Pai, Reet, Lee, Kenneth, Brand, Randall E., and Uttam, Shikhar

Subjects

HEREDITARY nonpolyposis colorectal cancer, COLON cancer, MUCOUS membranes, COLORECTAL cancer, INFLAMMATION

Abstract

Introduction: Lynch syndrome (LS) is the most common hereditary cause of colorectal cancer (CRC), increasing lifetime risk of CRC by up to 70%. Despite this higher lifetime risk, disease penetrance in LS patients is highly variable and most LS patients undergoing CRC surveillance will not develop CRC. Therefore, biomarkers that can correctly and consistently predict CRC risk in LS patients are needed to both optimize LS patient surveillance and help identify better prevention strategies that reduce risk of CRC development in the subset of highrisk LS patients. Methods: Normal-appearing colorectal tissue biopsies were obtained during repeat surveillance colonoscopies of LS patients with and without a history of CRC, healthy controls (HC), and patients with a history of sporadic CRC. Biopsies were cultured in an ex-vivo explant system and their supernatants were assayed via multiplexed ELISA to profile the local immune signaling microenvironment. High quality cytokines were identified using the rxCOV fidelity metric. These cytokines were used to perform elastic-net penalized logistic regression-based biomarker selection by computing a new measure - overall selection probability - that quantifies the ability of each marker to discriminate between patient cohorts being compared. Results: Our study demonstrated that cytokine based local immune microenvironment profiling was reproducible over repeat visits and sensitive to patient LS-status and CRC history. Furthermore, we identified sets of cytokines whose differential expression was predictive of LS-status in patients when compared to sporadic CRC patients and in identifying those LS patients with or without a history of CRC. Enrichment analysis based on these biomarkers revealed an LS and CRC status dependent constitutive inflammatory state of the normal appearing colonic mucosa. Discussion: This prospective pilot study demonstrated that immune profiling of normal appearing colonic mucosa discriminates LS patients with a prior history of CRC from those without it, as well as patients with a history of sporadic CRC from HC. Importantly, it suggests the existence of immune signatures specific to LSstatus and CRC history. We anticipate that our findings have the potential to assess CRC risk in individuals with LS and help in preemptively mitigating it by optimizing surveillance and identifying candidate prevention targets. Further studies are required to validate our findings in an independent cohort of LS patients over multiple visits. [ABSTRACT FROM AUTHOR]

Published

2023

220. Variant Characterization of a Representative Large Pedigree Suggests "Variant Risk Clusters" Convey Varying Predisposition of Risk to Lynch Syndrome.

Author

Barbirou, Mouadh, Miller, Amanda A., Mezlini, Amel, Bouhaouala-Zahar, Balkiss, and Tonellato, Peter J.

Subjects

*DIAGNOSIS of hereditary nonpolyposis colorectal cancer, *SEQUENCE analysis, *HEREDITARY nonpolyposis colorectal cancer, *GENETIC variation, *COLORECTAL cancer, *GENOMICS, *RESEARCH funding, *GENETIC techniques, *GENEALOGY, *DISEASE risk factors

Abstract

Simple Summary: Approximately 20% of colorectal cancer (CRC) cases are diagnosed in individuals under 40, with a severe prognosis due to germline variant accumulation. Many of these variants have been classified as hereditary cancer causative, while others remain poorly researched. The identification of germline variants across different populations is critical for accurate prognosis, treatment, and follow-up. We aimed to identify and predict the functional implications of germline variants using whole-genome sequencing of a Tunisian pedigree with Lynch syndrome CRC risk. Two SNPs/indels were identified in genes with CRC association (MLH1 and PRH1-TAS2R14) and four in genes with non-CRC cancer association (PPP1R13B, LAMA5, FTO, and NLRP14). Three structural variants overlapped genes associated with non-CRC digestive cancer (RELN, IRS2, and FOXP1) and one overlapped RRAS2 with non-CRC cancer associations. This study provides further evidence of genetic predisposition according to the risk clustering of variants based on their functional implications and risk mechanisms within the same pedigree. Recently, worldwide incidences of young adult aggressive colorectal cancer (CRC) have rapidly increased. Of these incidences diagnosed as familial Lynch syndrome (LS) CRC, outcomes are extremely poor. In this study, we seek novel familial germline variants from a large pedigree Tunisian family with 12 LS-affected individuals to identify putative germline variants associated with varying risk of LS. Whole-genome sequencing analysis was performed to identify known and novel germline variants shared between affected and non-affected pedigree members. SNPs, indels, and structural variants (SVs) were computationally identified, and their oncological influence was predicted using the Genetic Association of Complex Diseases and Disorders, OncoKB, and My Cancer Genome databases. Of 94 germline familial variants identified with predicted functional impact, 37 SNPs/indels were detected in 28 genes, 2 of which (MLH1 and PRH1-TAS2R14) have known association with CRC and 4 others (PPP1R13B, LAMA5, FTO, and NLRP14) have known association with non-CRC cancers. In addition, 48 of 57 identified SVs overlap with 43 genes. Three of these genes (RELN, IRS2, and FOXP1) have a known association with non-CRC digestive cancers and one (RRAS2) has a known association with non-CRC cancer. Our study identified 83 novel, predicted functionally impactful germline variants grouped in three "variant risk clusters" shared in three familiarly associated LS groups (high, intermediate and low risk). This variant characterization study demonstrates that large pedigree investigations provide important evidence supporting the hypothesis that different "variant risk clusters" can convey different mechanisms of risk and oncogenesis of LS-CRC even within the same pedigree. [ABSTRACT FROM AUTHOR]

Published

2023

221. The MSH2 c.793-1G>A variant disrupts normal splicing and is associated with Lynch syndrome.

Author

Yiming Li, Lulu Yu, Jiajia Cui, Jiye Yin, and Wei Wu

Subjects

HEREDITARY nonpolyposis colorectal cancer, GENETIC variation, COLORECTAL cancer, MANUFACTURING defects, ALTERNATIVE RNA splicing, PROTEIN expression

Abstract

Instruction: Lynch syndrome (LS) is the most common inherited cancer predisposition disorder of colorectal cancer (CRC) which is associated with pathogenic variants in 4 mismatch repair (MMR) genes. Here, we reported a multi-generation Chinese family clinically diagnosed with LS. Methods: To identify the underlying pathogenic gene variants, 30 whole blood samples and 4 colorectal cancer tissue samples and their clinical data were obtained from this four-generation family. Microsatellite instability-high (MSI) testing, immunohistochemistry (IHC), and Whole-Exome Sequencing (WES) were performed to identify the MMR/MSI and the underlying gene variants. The minigene splicing assay and in vitro splicing assay were used to explore the function of this variant. Results: MSI-H and dMMR was revealed by the MSI testing and IHC, Whole-Exome Sequencing (WES) in 3 patients successfully identified a splicing variant (c.793-1G>A) in intron 4 of MSH2. Sanger sequencing validated the WES results, and all the "healthy" individuals carrying the variant have been identified in the family by PCR. Bioinformatics analysis and in vitro minigene assay showed that the pathogenic variant affected the splicing process of MSH2 gene to generate 2 kinds defective transcription products, and consequently reduced the expression of MSH2 protein. The mutation carriers were later recommended for colonoscopy and other important cancer diagnostic inspections every 1-2 years because they both have a higher risk of LS. Discussion: We found a pathogenic splicing variant (rs863225397, c.793-1G>A) of MSH2 gene, and furtherly confirmed that this mutation plays an important role in LS patients of this pedigree based on the vitro study. Our study indicates that one splicing mutation in the MSH2 gene (c.793-1G>A) causes LS and highlights the importance of LS gene testing. [ABSTRACT FROM AUTHOR]

Published

2023

222. Evaluating mismatch repair deficiency in colorectal cancer biopsy specimens.

Author

Grillo, F., Paudice, M., Gambella, A., Bozzano, S., Sciallero, S., Puccini, A., Lastraioli, S., Dono, M., Parente, P., Vanoli, A., Angerilli, V., Fassan, M., and Mastracci, L.

Subjects

*COLORECTAL cancer, *IMMUNE checkpoint inhibitors, *BIOPSY, *INTERNAL auditing

Abstract

Mismatch repair (MMR) testing on all new cases of colorectal cancer (CRC) has customarily been preferably performed on surgical specimens, as more tissue is available; however, new clinical trials for the use of immune checkpoint inhibitors in the neoadjuvant setting require MMR testing on biopsy samples. This study aims at identifying advantages, disadvantages and any potential pitfalls in MMR evaluation on biopsy tissue and how to cope with them. The study is prospective-retrospective, recruiting 141 biopsies (86 proficient (p)MMR and 55 deficient (d)MMR) and 97 paired surgical specimens (48 pMMR; 49 dMMR). In biopsy specimens, a high number of indeterminate stains was observed, in particular for MLH1 (31 cases, 56.4%). The main reasons were a punctate nuclear expression of MLH1, relatively weak MLH1 nuclear expression compared to internal controls, or both (making MLH1 loss difficult to interpret), which was solved by reducing primary incubation times for MLH1. A mean of ≥ 5 biopsies had adequate immunostains, compared to ≤ 3 biopsies in inadequate cases. Conversely, surgical specimens rarely suffered from indeterminate reactions, while weaker staining intensity (p < 0.007) for MLH1 and PMS2 and increased patchiness grade (p < 0.0001) were seen. Central artefacts were almost exclusive to surgical specimens. MMR status classification was possible in 92/97 matched biopsy/resection specimen cases, and all of these were concordant (47 pMMR and 45 dMMR). Evaluation of MMR status on CRC biopsy samples is feasible, if pitfalls in interpretation are known, making laboratory-specific appropriate staining protocols fundamental for high-quality diagnoses. [ABSTRACT FROM AUTHOR]

Published

2023

223. Improving genetic testing following abnormal mismatch repair immunohistochemistry results in endometrial cancer.

Author

Karpel, Hannah C., Smith, Maria, Brodsky, Allison, and Pothuri, Bhavana

Subjects

*ENDOMETRIAL cancer, *GENETIC testing, *HEREDITARY nonpolyposis colorectal cancer, *DNA mismatch repair, *GENETIC counseling, *IMMUNOHISTOCHEMISTRY, *ETHYLCELLULOSE

Abstract

Although universal mismatch repair (MMR) immunohistochemistry (IHC) in endometrial cancer began at our institution in July 2015, not all eligible patients were referred for genetic testing (GT). In April 2017, genetic counselors obtained IHC data and contacted physicians to approve genetic counseling referrals (GCRs) for Lynch Syndrome (LS) in eligible patients. We assessed if this protocol increased frequency of GCRs and GT in patients with abnormal MMR IHC. We retrospectively (7/2015–5/2022) identified patients with abnormal MMR IHC at a large urban hospital. GCRs and GT were compared between cases from 7/2015–4/2017 (pre-protocol) and 5/2017–5/2022 (post-protocol) with chi-square and Fisher's exact tests. Of 794 patients with IHC testing, 177 (22.3%) had abnormal MMR results with 46 (26.0%) meeting criteria for LS screening with GT. Of 46 patients, 16 (34.8%) were identified prior to and 30 (65.2%) after the protocol initiation. GCRs significantly increased from 11/16 (68.8%) to 29/30 (96.7%) in the pre-protocol versus post-protocol groups, p = 0.02. There was no statistically significant difference in GT between groups (10/16, 62.5% vs 26/30, 86.7%, p = 0.07). Of 36 patients who underwent GT, 16 (44.4%) had LS: MSH6, 9; MSH2, 4 ; PMS2, 2; MLH1, 1. Increased frequency of GCRs was observed following the change in protocol, which is important as LS screening has clinical implications for patients and their families. Despite this additional effort, approximately 15% who met criteria did not undergo GT; further efforts such as universal germline testing in patients with endometrial cancer should be considered. • In endometrial cancer (EC) cases with abnormal immunohistochemistry, a protocol aimed to increase germline testing (GT). • In eligible patients, genetic counseling referrals (GCRs) but not GT significantly increased after the protocol. • About 15% of eligible patients still did not undergo GT following the protocol implementation. • Further measures, such as universal GT in patients with EC, should be considered to appropriately screen for Lynch Syndrome. [ABSTRACT FROM AUTHOR]

Published

2023

224. Lynch Syndrome Biopathology and Treatment: The Potential Role of microRNAs in Clinical Practice.

Author

Ascrizzi, Serena, Arillotta, Grazia Maria, Grillone, Katia, Caridà, Giulio, Signorelli, Stefania, Ali, Asad, Romeo, Caterina, Tassone, Pierfrancesco, and Tagliaferri, Pierosandro

Subjects

*DISEASE progression, *GENETIC mutation, *DNA, *HEREDITARY nonpolyposis colorectal cancer, *MICRORNA, *GENETIC disorders, *GENE expression, *AGE factors in disease, *GENE expression profiling, *TUMOR markers, *EPIGENOMICS, *HEREDITARY cancer syndromes

Abstract

Simple Summary: Lynch syndrome is an autosomal dominant hereditary disease that confers a high risk of developing various types of tumors, especially colorectal and endometrial cancer. In recent years, the molecular mechanisms underlying Lynch syndrome have generated considerable interest. Several studies have highlighted the epiphenomenon of microsatellite instability, caused by a deficit in the ability of cells to repair DNA damage, as a disease-specific feature. The discovery of microRNAs has served to clarify how these small oligonucleotide molecules may contribute to the progression of Lynch syndrome by modulating the expression of several players involved in DNA repair pathways. The purpose of this review is to analyze the management of patients with Lynch syndrome by emphasizing the importance of microRNAs as markers or therapeutics for the development of novel clinical approaches. Lynch syndrome (LS), also known as Hereditary Non-Polyposis Colorectal Cancer (HNPCC), is an autosomal dominant cancer syndrome which causes about 2–3% of cases of colorectal carcinoma. The development of LS is due to the genetic and epigenetic inactivation of genes involved in the DNA mismatch repair (MMR) system, causing an epiphenomenon known as microsatellite instability (MSI). Despite the fact that the genetics of the vast majority of MSI-positive (MSI+) cancers can be explained, the etiology of this specific subset is still poorly understood. As a possible new mechanism, it has been recently demonstrated that the overexpression of certain microRNAs (miRNAs, miRs), such as miR-155, miR-21, miR-137, can induce MSI or modulate the expression of the genes involved in LS pathogenesis. MiRNAs are small RNA molecules that regulate gene expression at the post-transcriptional level by playing a critical role in the modulation of key oncogenic pathways. Increasing evidence of the link between MSI and miRNAs in LS prompted a deeper investigation into the miRNome involved in these diseases. In this regard, in this study, we discuss the emerging role of miRNAs as crucial players in the onset and progression of LS as well as their potential use as disease biomarkers and therapeutic targets in the current view of precision medicine. [ABSTRACT FROM AUTHOR]

Published

2023

225. The Role of Colonoscopy in the Management of Individuals with Lynch Syndrome: A Narrative Review.

Author

D'Angelo, Valentina, Rega, Daniela, Marone, Pietro, Di Girolamo, Elena, Civiletti, Corrado, Tatangelo, Fabiana, Duraturo, Francesca, De Rosa, Marina, de Bellis, Mario, and Delrio, Paolo

Subjects

*PUBLIC health surveillance, *COLONOSCOPY, *COLON polyps, *HEREDITARY nonpolyposis colorectal cancer, *EARLY detection of cancer, *COLORECTAL cancer, *RISK assessment, *MEDICAL protocols, *ALGORITHMS, *DISEASE risk factors, *DISEASE complications

Abstract

Simple Summary: The research is being suggested from the observation that the incidence of colorectal cancer in individuals with Lynch Syndrome did not entirely decrease as expected, despite the high quality colonscopies performed in the surveillance programs, according to current Guidelines. The authors would like to highlight that the factors responsible for these results are indipendent of both endoscopy surveillance and adherence to prevention programs of individuals affected by Lynch Syndrome. Probably, the peculiarity of carcinogenesis itself in Lynch Syndrome is responsible for the above mentioned unexpected decrease in incidence of colorectal cancer in individuals with Lynch Syndome. Therefore, rather than continuing to shorten the timing of endoscopic surveillance, other early diagnostic techniques and subsequent prevention strategies should be forecasted in order to allow a more effective and customized endoscopic surveillance of individuals with Lynch Syndome. The history of Lynch syndrome changed definitively in 2000, when a study published in Gastroenterology demonstrated a significant reduction in mortality among individuals with Lynch syndrome who undergo regular endoscopic surveillance. As a consequence of this clinical evidence, all scientific societies developed guidelines, which highlighted the role of colonoscopy in the management of Lynch syndrome, especially for individuals at high risk of colorectal cancer. Over the years, these guidelines were modified and updated. Specialized networks were developed in order to standardize endoscopic surveillance programs and evaluate all the clinical data retrieved by the results of colonoscopies performed for both the screening and the surveillance of individuals with Lynch syndrome. Recent data show that the impact of colonoscopy (with polypectomy) on the prevention of colorectal cancer in individuals with Lynch syndrome is less significant than previously thought. This narrative review summarizes the current discussion, the hypotheses elaborated and the algorithms depicted for the management of individuals with Lynch Syndrome on the basis of the recent data published in the literature. [ABSTRACT FROM AUTHOR]

Published

2023

226. Malignant Adenomyoepithelioma of the Breast: An Unexpected Malignancy in a Lynch Syndrome Patient.

Author

Joyon, Natacha, Guillaume, Zoe, Ouafi, Lamia, Cotteret, Sophie, Rouleau, Etienne, Caron, Olivier, Goldbarg, Veronica, and Lacroix-Triki, Magali

Subjects

*BREAST, *HEREDITARY nonpolyposis colorectal cancer, *ADENOID cystic carcinoma, *NUCLEOTIDE sequencing

Abstract

We believe that our discovery was an incidental finding especially as the tumoural cells didn't show any loss of expression of MMR proteins, and this despite the fact that our tumour presents certain characteristics of MMR-deficient breast cancers (high grade, high mitotic index, triple negative phenotype). This case highlights two points: first, a germline mutation is not necessarily involved in a given carcinogenesis and second, as cancer predisposition syndromes are not uncommon, and as genetic testing use increases, the incidental discovery of these syndromes will be more and more frequent, requiring appropriate management and interpretation. Keywords: adenomyoepihtelioma; lynch syndrome EN adenomyoepihtelioma lynch syndrome 572 575 4 07/04/23 20230801 NES 230801 We report a case of a malignant adenomyoepithelioma in a 46-year-old woman with a significant family history of cancer. [Extracted from the article]

Published

2023

227. Prognostic value of Lynch syndrome, BRAFV600E, and RAS mutational status in dMMR/MSI‐H metastatic colorectal cancer in a pooled analysis of Dutch and French cohorts.

Author

Zwart, Koen, van der Baan, Frederieke H., Cohen, Romain, Aparicio, Thomas, de la Fouchardiére, Christelle, Lecomte, Thierry, Punt, Cornelis J. A., Sefrioui, David, Verheijden, Rik J., Vink, Geraldine R., Wensink, G. Emerens, Zaanan, Aziz, Koopman, Miriam, Tougeron, David, and Roodhart, Jeanine M. L.

Subjects

*COLORECTAL cancer, *HEREDITARY nonpolyposis colorectal cancer, *PROGNOSIS, *METASTASIS, *CANCER chemotherapy, *REGRESSION analysis

Abstract

Background: Current knowledge on prognostic biomarkers (especially BRAFV600E/RAS mutations) in metastatic colorectal cancer (mCRC) is mainly based on mCRC patients with proficient mismatch repair (pMMR) tumors. It is uncertain whether these biomarkers have the same prognostic value in mCRC patients with deficient mismatch repair (dMMR) tumors. Methods: This observational cohort study combined a population‐based Dutch cohort (2014–2019) and a large French multicenter cohort (2007–2017). All mCRC patients with a histologically proven dMMR tumor were included. Results: In our real‐world data cohort of 707 dMMR mCRC patients, 438 patients were treated with first‐line palliative systemic chemotherapy. Mean age of first‐line treated patients was 61.9 years, 49% were male, and 40% had Lynch syndrome. BRAFV600E mutation was present in 47% of tumors and 30% harbored a RAS mutation. Multivariable regression analysis on OS showed significant hazard rates (HR) for known prognostic factors as age and performance status, however showed no significance for Lynch syndrome (HR: 1.07, 95% CI: 0.66–1.72), BRAFV600E mutational status (HR: 1.02, 95% CI: 0.67–1.54), and RAS mutational status (HR: 1.01, 95% CI: 0.64–1.59), with similar results for PFS. Conclusion: BRAFV600E and RAS mutational status are not associated with prognosis in dMMR mCRC patients, in contrast to pMMR mCRC patients. Lynch syndrome is also not an independent prognostic factor for survival. These findings underline that prognostic factors of patients with dMMR mCRC are different of those with pMMR, which could be taken into consideration when prognosis is used for clinical decision‐making in dMMR mCRC patients and underline the complex heterogeneity of mCRC. [ABSTRACT FROM AUTHOR]

Published

2023

228. Comparison of clinicopathologic features, survival, and demographics in sebaceous carcinoma patients with and without Muir-Torre syndrome.

Author

Maloney, Nolan J., Zacher, Natasha C., Hirotsu, Kelsey E., Rajan, Neil, Aasi, Sumaira Z., and Kibbi, Nour

Abstract

Visceral malignancies in patients with Lynch syndrome behave less aggressively than in those without Lynch syndrome. The behavior of sebaceous carcinoma (SC) in Muir-Torre syndrome (MTS), a variant of Lynch syndrome, is incompletely investigated. To investigate features and survival of SC patients with and without MTS. Retrospective cohort study in the Surveillance, Epidemiology, and End Results 17 database from 2000 to 2019 of patients with SC. Patients were classified as MTS or non-MTS cases based on a threshold score of 2 on the Mayo MTS risk score. We identified 105 (2.8%) MTS cases and 3677 (97.2%) non-MTS cases. On univariate analysis, MTS patients were younger, had a higher proportion of tumors outside the head/neck, and had fewer high-grade tumors. On Kaplan-Meier analysis, MTS patients trended toward having better SC-specific survival. On multivariate Cox proportional hazards analysis adjusting for other covariates, MTS status was an independent predictor of worse overall survival. However, there was no association between MTS status and SC-specific survival. Given relatively high disease-specific survival in SC, our study may have been underpowered to detect a difference on Kaplan-Meier analysis. Our study suggests SC does not behave more aggressively in patients with MTS. [ABSTRACT FROM AUTHOR]

Published

2023

229. In person and virtual process mapping experiences to capture and explore variability in clinical practice: application to genetic referral pathways across seven Australian hospital networks.

Author

Morrow, April, Steinberg, Julia, Chan, Priscilla, Tiernan, Gabriella, Kennedy, Elizabeth, Egoroff, Natasha, Hilton, Desiree, Sankey, Lucien, Venchiarutti, Rebecca, Hayward, Anne, Pearn, Amy, McKay, Skye, Debono, Deborah, Hogden, Emily, and Taylor, Natalie

Abstract

Genetic referral for Lynch syndrome (LS) exemplifies complex clinical pathways. Identifying target behaviours (TBs) for change and associated barriers requires structured group consultation activities with busy clinicians – consolidating implementation activities whilst retaining rigour is crucial. This study aimed to: i) use process mapping to gain in-depth understandings of site-specific LS testing and referral practices in Australian hospitals and support identification of TBs for change, ii) explore if barriers to identified TBs could be identified through process mapping focus-group data, and iii) demonstrate pandemic-induced transition from in-person to virtual group interactive process mapping methods. LS clinical stakeholders attended interactive in-person or virtual focus groups to develop site-specific "process maps" visually representing referral pathways. Content analysis of transcriptions informed site-specific process maps, then clinical audit data was compared to highlight TBs for change. TBs were reviewed in follow-up focus groups. Secondary thematic analysis explored barriers to identified TBs, coded against the Theoretical Domains Framework (TDF). The transition from in-person to pandemic-induced virtual group interactive process mapping methods was documented. Process mapping highlighted six key areas of clinical practice variation across sites and site-specific TBs for change were identified. Key barriers to identified TBs emerged, categorised to seven TDF domains. Process mapping revealed variations in clinical practices surrounding LS referral between sites. Incorporating qualitative perspectives enhances process mapping by facilitating identification of TBs for change and barriers, providing a pathway to developing targeted interventions. Virtual process mapping activities produced detailed data and enabled comprehensive map development. [ABSTRACT FROM AUTHOR]

Published

2023

230. Familial intestinal polyposis and device assisted enteroscopy: where do we stand?

Author

Losurdo, Giuseppe, Di Leo, Milena, Rizzi, Salvatore, Lacavalla, Ilaria, Celiberto, Francesca, Iannone, Andrea, Rendina, Maria, Ierardi, Enzo, Iabichino, Giuseppe, De Luca, Luca, and Di Leo, Alfredo

Subjects

HEREDITARY nonpolyposis colorectal cancer, ENTEROSCOPY, HEREDITARY cancer syndromes, ADENOMATOUS polyposis coli, POLYPECTOMY, SMALL intestine, MAGNETIC resonance imaging, COLORECTAL cancer, INTESTINES

Abstract

Hereditary polyposis syndromes are a group of inherited disorders associated with a high risk of developing colorectal cancer. The best known ones are familial adenomatous polyposis (FAP), Peutz-Jeghers (PJS), juvenile polyposis and Cowden syndromes, as well as conditions predisposing to cancer, such as Lynch syndrome. Some of them are characterized by an increased risk of small bowel polyps occurrence. Literature search in PubMed was performed in November 2022 and a narrative review was carried out. Since performing small bowel polypectomy is important in such patients, device assisted enteroscopy (DAE) is the key for this procedure. A screening strategy for small bowel polyps is recommended only for PJS. Guidelines endorse either magnetic resonance imaging (MRI) or videocapsule endoscopy (VCE) every 1–3 years, according to the phenotype of the disease. Enteroscopy should be considered for therapeutic purpose in patients with a positive VCE or MRI. DAE has a central role in the resection of polyps larger than mm or causing symptoms of subocclusion or intussusception. Both single (SBE) and double balloon enteroscopy (DBE) are indicated and able to resect polyps up to 6–10 cm. American guidelines have restricted the indications to small bowel enteroscopy only to FAP patients with grade IV Spiegelman. Only some groups of patients (PJS, FAP with demonstrated small bowel polyp burden) may benefit from DAE. [ABSTRACT FROM AUTHOR]

Published

2023

231. Characteristics of glioblastomas and immune microenvironment in a Chinese family with Lynch syndrome and concurrent porokeratosis.

Author

Zhi-Gang Yao, Fang Hua, Zuo-Hua Yin, Ying-Jie Xue, Yang-Hao Hou, Yi-Cong Nie, Zhi-Ming Zheng, Miao-Qing Zhao, Xiao-Hong Guo, Chao Ma, Xiao-Kang Li, Zhou Wang, Guang-Cun Liu, and Gui-Hui Zhang

Subjects

HEREDITARY nonpolyposis colorectal cancer, MULTINUCLEATED giant cells, GLIOBLASTOMA multiforme, IMMUNOSTAINING, IMMUNE checkpoint inhibitors, GENETIC counseling

Abstract

Background: Lynch syndrome (LS)-associated glioblastoma (GBM) is rare in clinical practice, and simultaneous occurrence with cutaneous porokeratosis is even rarer. In this study, we analyzed the clinicopathological and genetic characteristics of LS-associated GBMs and concurrent porokeratosis, as well as evaluated the tumor immune microenvironment (TIME) of LS-associated GBMs. Methods: Immunohistochemical staining was used to confirm the histopathological diagnosis, assess MMR and PD-1/PD-L1 status, and identify immune cell subsets. FISH was used to detect amplification of EGFR and PDGFRA, and deletion of 1p/19q and CDKN2A. Targeted NGS assay analyzed somatic variants, MSI, and TMB status, while whole-exome sequencing and Sanger sequencing were carried out to analyze the germline mutations. Results: In the LS family, three members (I:1, II:1 and II:4) were affected by GBM. GBMs with loss of MSH2 and MSH6 expression displayed giant and multinucleated bizarre cells, along with mutations in ARID1A, TP53, ATM, and NF1 genes. All GBMs had TMB-H but notMSI-H. CD8+ T cells and CD163+macrophageswere abundant in each GBM tissue. The primary and recurrent GBMs of II:1 showed mesenchymal characteristics with high PD-L1 expression. The family members harbored a novel heterozygous germline mutation in MSH2 and FDPS genes, confirming the diagnosis of LS and disseminated superficial actinic porokeratosis. Conclusion: LS-associated GBM exhibits heterogeneity in clinicopathologic and molecular genetic features, as well as a suppressive TIME. The presence of MMR deficiency and TMB-H may serve as predictive factors for the response to immune checkpoint inhibitor therapy in GBMs. The identification of LSassociated GBM can provide significant benefits to both patients and their family members, including accurate diagnosis, genetic counseling, and appropriate screening or surveillance protocols. Our study serves as a reminder to clinicians and pathologists to consider the possibility of concurrent genetic syndromes in individuals or families. [ABSTRACT FROM AUTHOR]

Published

2023

232. Using a multistep approach with multidisciplinary team to increase the diagnosis rate of Lynch syndrome-associated colorectal cancer after universal screening: a single-center study in Japan.

Author

Tatsuta, Kyota, Sakata, Mayu, Iwaizumi, Moriya, Kojima, Risa, Yamanaka, Katsumasa, Baba, Satoshi, Suzuki, Katsunori, Morita, Yoshifumi, Kikuchi, Hirotoshi, Hiramatsu, Yoshihiro, Kurachi, Kiyotaka, and Takeuchi, Hiroya

Subjects

*HEREDITARY nonpolyposis colorectal cancer, *COLORECTAL cancer, *MEDICAL screening, *GENETIC counseling, *MEDICAL specialties & specialists, *GENETIC testing

Abstract

Backgrounds: : This study aimed to evaluate the changes in the rates of genetic counseling and genetic testing as well as the diagnosis rate of Lynch syndrome (LS)-associated colorectal cancer before and after multistep approach with multidisciplinary team in Japanese. Methods: In September 2016, we started universal screening for LS by mismatch repair protein immunohistochemistry and prospectively collected the records. Following patient interviews, we started multistep approach with multidisciplinary team (MA) in January 2020. MA consists of six surgeons, one genetic counselor, one medical geneticist, and six pathologists. MA is set up to compensate for patients' lack of knowledge about genetic diseases and make case selection for elderly colorectal cancer patients with deficient mismatch repair (dMMR). MA is designed as a system that could be performed by a small number of medical genetic specialists. A total of 522 patients were included during the study duration, 323 and 199 patients in the pre-MA (P-MA) and MA groups, respectively. Results: The frequency of dMMR in all patients was 10.0%. The patient interview results indicated a significant lack of patient education regarding genetic diseases. The rates of genetic counseling and genetic testing was significantly higher in MA group than in P-MA group (genetic counseling: MA 34.6% vs. P-MA 7.7%, p = 0.04; genetic testing: MA 30.8% vs. P-MA 3.8%, p = 0.02). Moreover, the diagnosis rate of LS-associated colorectal cancer was significantly higher in MA group (2.5%) than in P-MA group (0.3%) (P = 0.03). In addition, MA could be performed without problems despite the small number of medical and human genetics specialists. Conclusions: MA has achieved appropriate pickup of suspected hereditary colorectal cancer patients and complemented the lack of knowledge about genetic diseases. The introduction of MA increased LS-associated colorectal cancer after universal screening. MA is an appropriate LS screening protocol for Japanese patients who lag behind in medical and human genetics education. [ABSTRACT FROM AUTHOR]

Published

2023

233. The Prevalence and Molecular Landscape of Lynch Syndrome in the Affected and General Population.

Author

Roht, Laura, Laidre, Piret, Tooming, Mikk, Tõnisson, Neeme, Nõukas, Margit, Nurm, Miriam, Roomere, Hanno, Rekker, Kadri, Toome, Kadri, Fjodorova, Olga, Murumets, Ülle, Šamarina, Ustina, Pajusalu, Sander, Aaspõllu, Anu, Salumäe, Liis, Muhu, Kristina, Soplepmann, Jaan, Õunap, Katrin, and Kahre, Tiina

Subjects

*CONFIDENCE intervals, *SEQUENCE analysis, *IMMUNOHISTOCHEMISTRY, *HEREDITARY nonpolyposis colorectal cancer, *GENETIC testing, *MOLECULAR biology, *GENETIC markers, *DISEASE susceptibility, *RESEARCH funding, *DESCRIPTIVE statistics, *DATA analysis software, *ODDS ratio, *LONGITUDINAL method

Abstract

Simple Summary: Lynch syndrome accounts for 2–3% of all CRC cases. This retroactive and prospective study aimed to estimate the prevalence of Lynch syndrome and describe disease-causing variants in mismatch repair genes in a diagnostic setting and in the Estonian general population. For that, ten years (2012–2022) of data was gathered. In addition, a pilot study for estimating the improvement of Lynch syndrome diagnostics by raising the age limit of mismatch repair gene immunohistochemistry was conducted. We estimated the birth prevalence of LS in Estonia at 1:8638 (95% CI: 1:9859–7588) or 11.58 (95% CI: 10.14–13.18) for 100,000 LBs between 1930 and 2003. The prevalence of Lynch syndrome has increased approximately six-fold in ten years. Due to the improvement of awareness in families and patients sharing information with their family members, the latter receives the diagnosis eight years earlier when most individuals are still healthy, illustrating the benefit of genetic testing and therefore an opportunity for prevention. Furthermore, the pilot study proved to be beneficial. Background: Lynch syndrome (LS) is the most frequent genetically pre-disposed colorectal cancer (CRC) syndrome, accounting for 2–3% of all CRC cases. In Estonia, ~1000 new cases are diagnosed each year. This retroactive and prospective study aimed to estimate the prevalence of LS and describe disease-causing variants in mismatch repair (MMR) genes in a diagnostic setting and in the Estonian general population. Methods: LS data for the diagnostic cohort were gathered from 2012 to 2022 and data for the general population were acquired from the Estonian Biobank (EstBB). Furthermore, we conducted a pilot study to estimate the improvement of LS diagnostic yield by raising the age limit to >50 years for immunohistochemistry analysis of MMR genes. Results: We estimated LS live birth prevalence between 1930 and 2003 in Estonia at 1:8638 (95% CI: 1: 9859–7588). During the study period, we gathered 181 LS individuals. We saw almost a six-fold increase in case prevalence, probably deriving from better health awareness, improved diagnostic possibilities and the implementation of MMR IHC testing in a broader age group. Conclusion: The most common genes affected in the diagnostic and EstBB cohorts were MLH1 and PMS2 genes, respectively. The LS diagnosis mean age was 44.8 years for index cases and 36.8 years (p = 0.003) for family members. In the MMR IHC pilot study, 29% had LS. [ABSTRACT FROM AUTHOR]

Published

2023

234. Gender-specific counselling of patients with upper tract urothelial carcinoma and Lynch syndrome.

Author

Cerrato, Clara, Pandolfo, Savio Domenico, Autorino, Riccardo, Panunzio, Andrea, Tafuri, Alessandro, Porcaro, Antonio Benito, Veccia, Alessandro, De Marco, Vincenzo, Cerruto, Maria Angela, Antonelli, Alessandro, Derweesh, Ithaar H., and Maresma, Maria Carmen Mir

Subjects

*HEREDITARY nonpolyposis colorectal cancer, *TRANSITIONAL cell carcinoma, *TESTICULAR cancer, *COUNSELING, *PANCREATIC cancer, *PROSTATE cancer

Abstract

Purpose: Lynch syndrome (LS) is an autosomal dominant genetic syndrome resulting in a wide spectrum of malignancies caused by germline mutations in mismatch repair genes (MMR). Gene mutations have different effects and penetrance between the two genders. The aim of this review is to offer a gender-specific evidence-based clinical guide on diagnosis, screening, surveillance, and counselling of UTUC patients with LS. Methods: Using MEDLINE, a non-systematic review was performed including articles between 2004 and 2022. English language original articles, reviews, and editorials were selected based on their clinical relevance. Results: Upper tract urothelial carcinoma (UTUC) is the third most common malignancy in Lynch syndrome. Up to 21% of new UTUC cases may have unrecognized LS as the underlying cause. LS-UTUC does not have a clear gender prevalence, even if it seems to slightly prefer the male gender. The MSH6 variant is significantly associated with female gender (p < 0.001) and with gynecological malignancies. Female MSH2 and MLH1 carriers have higher rates for endometrial and ovarian cancer with respect to the general population, while male MSH2 and MLH1 carriers have, respectively, higher rate of prostate cancer and upper GI tract, or biliary or pancreatic cancers. Conflicting evidence remains on the association of testicular cancer with LS. Conclusion: LS is a polyhedric disease, having a great impact on patients and their families that requires a multidisciplinary approach. UTUC patients should be systematically screened for LS, and urologists have to be aware that the same MMR mutation may lead to different malignancies according to the patient's gender. [ABSTRACT FROM AUTHOR]

Published

2023

235. Looking beyond the surface: Muir Torre syndrome.

Author

Bagga, Ekta, Innes, David, and Leung, Edmund

Subjects

*IRON deficiency anemia, *EPIDERMAL cyst, *GENETIC testing, *MEDICAL screening, *EARLY detection of cancer

Abstract

Muir-Torre Syndrome (MTS) is associated with multiple visceral malignancies. Initial presentation may be a benign skin tumor mimicking a sebaceous cyst. This case report highlights the importance of early diagnosis, genetic testing, and multidisciplinary screening. A 67-year-old man was diagnosed with MTS following excision of a skin lesion (sebaceoma). He was declined both screening colonoscopy and genetic testing. Subsequently, advanced colon cancer was found following presentation with iron deficiency anemia, which ultimately led to palliation despite successful surgery. MTS can present insidiously with skin lesions clinically diagnosed as sebaceous cysts. Once MTS is suspected on histology, genetic testing and screening for MTS-related cancers is warranted. Better understanding of the genetic variants for MTS can aid in earlier diagnosis thus not dismissing the need for screening for MTS-related cancers. [ABSTRACT FROM AUTHOR]

Published

2023

236. Lynch syndrome-associated chordoma with high tumor mutational burden and significant response to immune checkpoint inhibitors.

Author

Shinojima, Naoki, Ozono, Kazutaka, Yamamoto, Haruaki, Abe, Sakiko, Sasaki, Rumi, Tomita, Yusuke, Kai, Azusa, Mori, Ryosuke, Yamamoto, Takahiro, Uekawa, Ken, Matsui, Hirotaka, Nosaka, Kisato, Matsuzaki, Hiroaki, Komohara, Yoshihiro, Mikami, Yoshiki, and Mukasa, Akitake

Abstract

Chordoma is a rare malignant bone tumor arising from notochordal tissue. Conventional treatments, such as radical resection and high-dose irradiation, frequently fail to control the tumor, resulting in recurrence and re-growth. In this study, genetic analysis of the tumor in a 72-year-old male patient with refractory conventional chordoma of the skull base revealed a high tumor mutational burden (TMB) and mutations in the MSH6 and MLH1 genes, which are found in Lynch syndrome. The patient and his family had a dense cancer history, and subsequent germline genetic testing revealed Lynch syndrome. This is the first report of a chordoma that has been genetically proven to be Lynch syndrome. Chordomas usually have low TMB; however, this is an unusual case, because the TMB was high, and immune checkpoint inhibitors effectively controlled the tumor. This case provides a basis for determining the indications for immunotherapy of chordoma based on the genetic analysis. Therefore, further extensive genetic analysis in the future will help to stratify the treatment of chordoma. [ABSTRACT FROM AUTHOR]

Published

2023

237. Upper Tract Urothelial Carcinoma: A Rare Malignancy with Distinct Immuno-Genomic Features in the Era of Precision-Based Therapies.

Author

Evmorfopoulos, Konstantinos, Mitrakas, Lampros, Karathanasis, Athanasios, Zachos, Ioannis, Tzortzis, Vassilios, and Vlachostergios, Panagiotis J.

Subjects

TRANSITIONAL cell carcinoma, FIBROBLAST growth factor receptors, CIRCULATING tumor DNA, IMMUNE checkpoint inhibitors, KIDNEY pelvis, HEREDITARY nonpolyposis colorectal cancer

Abstract

Upper tract urothelial carcinoma (UTUC) is a rare malignancy, occurring in 5–10% of patients diagnosed with UC, and involves the renal pelvis, calyces, or ureters. UTUC can be sporadic or hereditary as a clinical manifestation of Lynch syndrome. Therapeutic management of these patients is challenging. Following risk stratification of localized disease, patients with low-grade UTUC may undergo kidney-sparing surgery or radical nephroureterectomy (RNU) and/or chemoablation with mitomycin-c instillation to reduce recurrence. In high-grade disease, RNU followed by adjuvant chemotherapy remains the standard of care. For decades, platinum-based chemotherapy has been the cornerstone of treatment for locally advanced and metastatic disease. The aim of the present review is to summarize recent advances in UTUC's therapeutic management through the lens of its genomic and immune landscape. Accumulating knowledge on the genetic and immune aspects of UTUC tumors has increased our understanding of their underlying biology, supporting a luminal papillary, T-cell depleted contexture and enrichment in fibroblast growth factor receptor (FGFR) expression. These advances have fueled successful clinical testing of several precision-based therapeutic approaches, including immune checkpoint inhibitors (ICIs), the antibody–drug conjugates (ADCs) enfortumab vedotin and sacituzumab govitecan, and agents targeting the FGFR axis such as erdafitinib and other kinase inhibitors, allowing their entry into the therapeutic armamentarium and improving the prognosis of these patients. Not all patients respond to these precision-based targeted therapies; thus, validating and expanding the toolkit of potential biomarkers of response or resistance, including molecular subtypes, FGFR pathway gene alterations, DNA repair gene defects, tumor mutational burden (TMB), circulating tumor DNA (ctDNA), nectin-4, TROP2, and programmed death ligand-1 (PD-L1), are key to maximizing the benefit to these particular subgroups of patients. [ABSTRACT FROM AUTHOR]

Published

2023

238. How to set up an in-house nurse-led colorectal Lynch syndrome clinic.

Author

Carvalho, Filipe, Koziel, Anna, and Monje-Garcia, Laura

Abstract

The NHS long term plan sets a target that by 2028, 75% of cancers will be diagnosed at an early stage. One of the ways this ambition will be reached is through targeted screening and personalised surveillance of those most at risk of developing cancer, such as those with Lynch syndrome. This article outlines the essential steps to consider when setting up and managing an in-house nurse-led colorectal Lynch syndrome clinic. It highlights the educational requirements, patient criteria, the importance of thorough planning and the need to liaise-on with key stakeholders. [ABSTRACT FROM AUTHOR]

Published

2023

239. Clinical predominance of whole‐exome sequencing to evaluate microsatellite instability status.

Author

Takamatsu, Reika, Nakamura, Kohei, Suzuki, Okihide, Okada, Chihiro, Mori, Ryo, Kawano, Ryutaro, Hayashi, Hideyuki, Ishikawa, Marin, Aimono, Eriko, Nohara, Sachio, Tanishima, Shigeki, Ueki, Arisa, Ishida, Hideyuki, and Nishihara, Hiroshi

Abstract

The microsatellite instability (MSI)/mismatch repair (MMR) status is one of the critical genomic biomarkers for predicting patient response to immune checkpoint inhibitors (ICIs). In this study, we aimed to investigate the concordance among the MSIsensor score obtained from whole‐exome sequencing (WES), which could be a futuristic clinical cancer sequencing method, using only tumor tissues, MSI‐PCR results, and immunohistochemistry (IHC) results to analyze various solid cancer types. We first endeavored to set the cut‐off value of MSIsensor to determine functional deficient mismatch repair (f‐dMMR) status. The MSI status of 1054 patients analyzed using WES was evaluated using MSIsensor. In addition, 87 of these patients were further analyzed using MSI‐PCR and MMR IHC to calculate the sensitivity and specificity of the MSIsensor cut‐off score. Our results showed that score 12.5 was an adequate cut‐off score equivalent to PCR‐confirmed MSS/MSI‐low and MSI‐high statuses, with sensitivity, specificity, and area under the curve values of 95.2%, 100%, and 0.998, respectively. Moreover, we identified false‐positive cases of tumors with high mutational burden with an MSIsensor score <12.5, and optional IHC examination could rescue these cases. In conclusion, the MSIsensor score obtained using WES with tumor tissue showed a high clinical validity, with a cut‐off value of 12.5 for f‐dMMR detection, in combination with optional IHC analysis for MMR. Our novel algorithm will provide insights into the development of ICIs for cancer treatment, particularly when WES becomes a more common cancer genomic test in the near future. [ABSTRACT FROM AUTHOR]

Published

2023

240. A PMS2 non-canonical splicing site variant leads to aberrant splicing in a patient suspected for lynch syndrome.

Author

Bouras, Ahmed, Naibo, Pierre, Legrand, Clémentine, Marc'hadour, François Le, Ruano, Eric, Grand-Masson, Chloé, Lefol, Cedrick, and Wang, Qing

Subjects

HEREDITARY nonpolyposis colorectal cancer, DNA mismatch repair, RNA analysis, GENE expression, NON-coding RNA, ENDOMETRIAL cancer

Abstract

The PMS2 gene is one of the DNA mismatch repair genes (MMR) implicated in Lynch syndrome (LS). A subset of PMS2 pathogenic variants (PVs) are splice variants mostly affecting canonical GT/AG splicing sequences. However, the majority of the intronic variants outside canonical splice sites remained as variants of unknown significance, even though some of them would alter the splicing process. In this report, we describe the analysis of such an intronic variant (c.251-5T > C) detected in an 82-year-old patient diagnosed with endometrial cancer displaying microsatellite instability and the loss of PMS2 expression displayed. RNA analysis demonstrated that this variant lead to the complete exon 4 skipping, resulting in the synthesis of a truncated protein. This finding shows the relevance of functional RNA analysis in the non-canonical intronic variant assessment and the importance of systematic evaluation of MSI/loss of expression of MMR genes for LS screening in patients with endometrial cancers. [ABSTRACT FROM AUTHOR]

Published

2023

241. A retrospective cohort study of genetic referral and diagnosis of Lynch syndrome in patients with cutaneous sebaceous lesions.

Author

Kattapuram, Meera, Shabet, Christina, Austin, Sarah, Jacobs, Michelle F., Koeppe, Erika, Smith, Emily H., Lowe, Lori, Else, Tobias, and Cha, Kelly B.

Subjects

GENETIC disorder diagnosis, HEREDITARY nonpolyposis colorectal cancer, CANCER genetics, GENETIC testing, COHORT analysis, MEDICAL referrals

Abstract

Immunohistochemistry (IHC) of cutaneous sebaceous lesions (SL) can be used to screen patients for Lynch syndrome (LS). There is little data on rates of genetic referral and outcomes of genetic testing for patients with SL. This single-center retrospective study characterizes 400 + patients with SL, including IHC results, genetics referrals, and outcomes of genetic testing. Retrospective chart reviews were performed for patients with a pathology-confirmed diagnosis of SL at the University of Michigan between January 2009 and December 2019. 447 patients with 473 SL were identified. Excluding 20 patients with known LS, IHC was conducted in 173 (41%) patients. 92/173 (53%) patients had abnormal results. 69 of these 92 (75%) patients were referred to genetics. 32 additional patients were referred with normal IHC (n = 22) or without IHC (n = 10). Of 101 patients referred, 65 (64%) were seen and 47 (47%) completed genetic testing. 7/47 (15%) had pathogenic variants associated with LS, six with concordant abnormal IHC and one without IHC. Cancer genetics referral of patients with SL, particularly for lesions with abnormal IHC, yields a significant rate of LS diagnosis. Providers should consider genetics referral for patients with SL. [ABSTRACT FROM AUTHOR]

Published

2023

242. Early-Onset Colorectal Cancer: Current Insights.

Author

Ullah, Fauzia, Pillai, Ashwathy Balachandran, Omar, Najiullah, Dima, Danai, and Harichand, Seema

Subjects

*COLORECTAL cancer, *RISK assessment, *AGE factors in disease, *DISEASE risk factors

Abstract

Simple Summary: Early-onset colorectal cancer is increasing in incidence in the United States, and it is expected to more than double in the next 10 years. There are many risk factors that lead to the development of early-onset colorectal cancer, including hereditary cancer syndromes, such as Lynch syndrome, obesity, diet, sedentary lifestyle, inflammatory bowel disease and altered microbiome. There is a significant lack of awareness of early-onset colorectal cancer, and the rise in the number of cases indicates that more coordinated efforts are needed to understand and treat early-onset colorectal cancer better, through promoting the benefits of screening, including genetic profiling, and increasing adherence to current screening guidelines. The aim of this review is to discuss the available literature regarding early-onset colorectal cancer to better define the risk factors, histopathology, genetic makeup and management. Over the past decade, the incidence of colorectal cancer has increased in individuals under the age of 50 years. Meanwhile, the incidence has gradually decreased in the older population. As described herein, we reviewed the available literature to summarize the current landscape of early-onset colorectal cancer, including risk factors, clinicopathological presentation, genetic makeup of patients, and management. Currently, early-onset colorectal cancer is treated similarly as late-onset colorectal cancer, yet the available literature shows that early-onset colorectal cancer is more aggressive and different, and this remains a significant unmet need. A detailed understanding of early-onset colorectal cancer is needed to identify risk factors for the increased incidence and tailor treatments accordingly. [ABSTRACT FROM AUTHOR]

Published

2023

243. Paget's Disease of the Bone and Lynch Syndrome: An Exceptional Finding.

Author

Gheorghe, Ana-Maria, Stanescu, Laura-Semonia, Petrova, Eugenia, Carsote, Mara, Nistor, Claudiu, and Ghemigian, Adina

Subjects

*OSTEITIS deformans, *CHONDROSARCOMA, *HEREDITARY nonpolyposis colorectal cancer, *GENETIC variation, *GENETIC testing, *GENE expression, *LITERATURE reviews

Abstract

Our objective is to present an exceptional case of a patient diagnosed with Paget's disease of the bone (PDB) while being confirmed with Lynch syndrome (LS). A 44-year-old woman was admitted for progressive pain in the left forearm 2 years ago, and was partially relieved since admission by non-steroidal anti-inflammatory drugs. Suggestive imaging findings and increased blood bone turnover markers helped the diagnosis of PDB. She was offered zoledronate 5 mg. She had two more episodes of relapse, and a decision of new medication was taken within the following years (a second dose of zoledronate, as well as denosumab 60 mg). Her family history showed PDB (mother) and colorectal cancer (father). Whole exome sequencing was performed according to the manufacturer's standard procedure (Ion AmpliSeq™ Exome RDY S5 Kit). A heterozygous pathogenic variant in the SQSTM1 gene (c.1175C>T, p.Pro392Leu) was confirmed, consistent with the diagnosis of PDB. Additionally, a heterozygous pathogenic variant of MSH2 gene (c.2634+1G>T) was associated with LS. The patient's first-degree relatives (her brother, one of her two sisters, and her only daughter) underwent specific genetic screening and found negative results, except for her daughter, who tested positive for both pathogenic variants while being clinically asymptomatic. The phenotype influence of either mutation is still an open issue. To our current knowledge, no similar case has been published before. Both genetic defects that led to the two conditions appeared highly transmissible in the patient's family. The patient might have an increased risk of osteosarcoma and chondrosarcoma, both due to PDB and LS, and a review of the literature was introduced in this particular matter. The phenotypic expression of the daughter remains uncertain and is yet to be a lifelong follow-up as the second patient harbouring this unique combination of gene anomalies. [ABSTRACT FROM AUTHOR]

Published

2023

244. Multi‐omic analysis in normal colon organoids highlights MSH4 as a novel marker of defective mismatch repair in Lynch syndrome and microsatellite instability.

Author

Devall, Matthew, Ali, Mourad W., Eaton, Stephen, Weisenberger, Daniel J., Reilley, Matthew J., Powell, Steven M., Li, Li, and Casey, Graham

Subjects

*HEREDITARY nonpolyposis colorectal cancer, *COLON (Anatomy), *MICROSATELLITE repeats, *ORGANOIDS, *GENE expression, *DNA methylation

Abstract

Introduction: Lynch syndrome (LS) is a hereditary condition that increases the risk of colorectal (CRC) and extracolonic cancers that exhibit microsatellite instability (MSI‐H). MSI‐H is driven by defective mismatch repair (dMMR), and approximately 15% of nonhereditary CRCs also exhibit MSI‐H. Here, we aimed to better define mechanisms underlying tumor initiation in LS and MSI‐H cancers through multi‐omic analyses of LS normal colon organoids and MSI‐H tumors. Methods: Right (n = 35) and left (n = 23) colon organoids generated from normal colon biopsies at routine colonoscopy of LS and healthy individuals were subjected to Illumina EPIC array. Differentially methylated region (DMR) analysis was performed by DMRcate. RNA‐sequencing (n = 16) and bisulfite‐sequencing (n = 15) were performed on a subset of right colon organoids. CRISPR‐cas9‐mediated editing of MMR genes in colon organoids of healthy individuals was followed by quantitative PCR of MSH4. The relationship between MSH4 expression and tumor mutational burden was further explored in three independent tumor data sets. Results: We identified a hypermethylated region of MSH4 in both the right and left colon organoids of LS versus healthy controls, which we validated using bisulfite‐sequencing. DMR analysis in three gastrointestinal and one endometrial data set revealed that this region was also hypermethylated in MSI‐H versus microsatellite stable (MSS) tumors. MSH4 expression was increased in colon organoids of LS versus healthy subjects and in publicly available MSI‐H versus MSS tumors across four RNA‐seq and four microarray data sets. CRISPR‐cas9 editing of MLH1 and MSH2, but not MSH6, in normal colon organoids significantly increased MSH4 expression. MSH4 expression was significantly associated with tumor mutational burden in three publicly available data sets. Conclusions: Our findings implicate DNA methylation and gene expression differences of MSH4 as a marker of dMMR and as a potential novel biomarker of LS. Our study of LS colon organoids supports the hypothesis that dMMR exists in the colons of LS subjects prior to CRC. [ABSTRACT FROM AUTHOR]

Published

2023

245. Beyond germline genetic testing - heterozygous pathogenic variants in PMS2 in two children with Osteosarcoma and Ependymoma.

Author

Kuhlen, Michaela, Golas, Mariola Monika, Schaller, Tina, Stadler, Nicole, Maier, Felicitas, Witt, Olaf, and Frühwald, Michael C.

Subjects

*HEREDITARY nonpolyposis colorectal cancer, *GENETIC variation, *GENETIC testing, *EPENDYMOMA, *GERM cells, *OSTEOSARCOMA

Abstract

Background: Lynch syndrome (LS) is not considered part of childhood cancer predisposition syndromes. Case presentation: Analysis of a pediatric osteosarcoma (OS) displayed hypermutation (16.8), alternative lengthening of telomeres (ALT), loss of PMS2 expression in tumor tissue (retained in non-neoplastic cells), PMS2 loss of heterozygosity (LOH), and high-degree of microsatellite instability (MSI) tested by PCR. A heterozygous duplication c.1076dup p.(Leu359Phefs*6) in exon 10 of NM_000535.6:PMS2 was detected by SNV analysis in peripheral blood, confirming diagnosis of LS in the patient. The tumor molecular features suggest LS-associated development of OS. In a second case, whole-genome sequencing identified a heterozygous SNV c.1 A > T p.? in exon 1 of PMS2 in tumor and germline material of a girl with ependymoma. Tumor analysis displayed evidence for ALT and low mutational burden (0.6), PMS2 expression was retained, MSI was low. Multiplex ligation-dependent probe amplification identified no additional PMS2 variant and germline MSI testing did not reveal increased gMSI ratios in the patient´s lymphocytes. Thus, CMMRD was most closely excluded and our data do not suggest that ependymoma was related to LS in the child. Conclusions: Our data suggest that the LS cancer spectrum may include childhood cancer. The importance of LS in pediatric cancers necessitates prospective data collection. Comprehensive molecular workup of tumor samples is necessary to explore the causal role of germline genetic variants. [ABSTRACT FROM AUTHOR]

Published

2023

246. A mainstreaming oncogenomics model: improving the identification of Lynch syndrome.

Author

O'Shea, Rosie, Crook, Ashley, Jacobs, Chris, Kentwell, Maira, Gleeson, Margaret, Tucker, Katherine M., Hampel, Heather, Kulchak Rahm, Alanna, Taylor, Natalie, Lewis, Sarah, and Rankin, Nicole M.

Subjects

HEREDITARY nonpolyposis colorectal cancer, HEREDITARY cancer syndromes, MEDICAL personnel, GENETIC testing, ELECTRONIC health records, INTEGRATIVE medicine

Abstract

Introduction: "Mainstreaming" is a proposed strategy to integrate genomic testing into oncology. The aim of this paper is to develop a mainstreaming oncogenomics model by identifying health system interventions and implementation strategies for mainstreaming Lynch syndrome genomic testing. Methods: A rigorous theoretical approach inclusive of conducting a systematic review and qualitative and quantitative studies was undertaken using the Consolidated Framework for Implementation Research. Theory-informed implementation data were mapped to the Genomic Medicine Integrative Research framework to generate potential strategies. Results: The systematic review identified a lack of theory-guided health system interventions and evaluation for Lynch syndrome and other mainstreaming programs. The qualitative study phase included 22 participants from 12 health organizations. The quantitative Lynch syndrome survey included 198 responses: 26% and 66% from genetic and oncology health professionals, respectively. Studies identified the relative advantage and clinical utility of mainstreaming to improve genetic test access and to streamline care, and adaptation of current processes was recognized for results delivery and follow-up. Barriers identified included funding, infrastructure and resources, and the need for process and role delineation. The interventions to overcome barriers were as follows: embedded mainstream genetic counselors, electronic medical record genetic test ordering, results tracking, and mainstreaming education resources. Implementation evidence was connected through the Genomic Medicine Integrative Research framework resulting in a mainstreaming oncogenomics model. Discussion: The proposed mainstreaming oncogenomics model acts as a complex intervention. It features an adaptable suite of implementation strategies to inform Lynch syndrome and other hereditary cancer service delivery. Implementation and evaluation of the model are required in future research. [ABSTRACT FROM AUTHOR]

Published

2023

247. Current chemoprevention approaches in Lynch syndrome and Familial adenomatous polyposis: a global clinical practice survey.

Author

Mraz, Kathryn A., Hodan, Rachel, Rodgers-Fouche, Linda, Arora, Sanjeevani, Balaguer, Francesc, Guillem, Jose G., Jeter, Joanne M., Kanth, Priyanka, Dan Li, Liska, David, Melson, Joshua, Perez, Kimberly, Ricker, Charite, Shirts, Brian H., Vilar, Eduardo, Katona, Bryson W., and Dominguez-Valentin, Mev

Subjects

ADENOMATOUS polyposis coli, HEREDITARY nonpolyposis colorectal cancer, CHEMOPREVENTION, CANCER chemoprevention, FAMILY history (Medicine), GASTROINTESTINAL cancer

Abstract

Background: International chemoprevention preferences and approaches in Lynch syndrome (LS) and APC-associated polyposis, including Familial adenomatous polyposis (FAP) and attenuated FAP (AFAP) have not been previously explored. Aim: To describe current chemoprevention strategies for patients with LS or FAP/AFAP (referred to collectively as FAP) practiced by members of four international hereditary cancer societies through administration of a survey. Results: Ninety-six participants across four hereditary gastrointestinal cancer societies responded to the survey. Most respondents (91%, 87/96) completed information regarding their demographics and practice characteristics relating to hereditary gastrointestinal cancer and chemoprevention clinical practices. Sixtynine percent (60/87) of respondents offer chemoprevention for FAP and/or LS as a part of their practice. Of the 75% (72/96) of survey respondents who were eligible to answer practice-based clinical vignettes based off of their responses to ten barrier questions regarding chemoprevention, 88% (63/72) of those participants completed at least one case vignette question to further characterize chemoprevention practices in FAP and/or LS. In FAP, 51% (32/63) would offer chemoprevention for rectal polyposis, with sulindac - 300 mg (18%, 10/56) and aspirin (16%, 9/56) being the most frequently selected options. In LS, 93% (55/59) of professionals discuss chemoprevention and 59% (35/59) frequently recommend chemoprevention. Close to half of the respondents (47%, 26/55) would recommend beginning aspirin at time of commencement of the patient's first screening colonoscopy (usually at age 25yrs). Ninety-four percent (47/50) of respondents would consider a patient's diagnosis of LS as an influential factor for aspirin use. There was no consensus on the dose of aspirin (=100 mg, >100 mg - 325 mg or 600 mg) to offer patients with LS and there was no agreement on how other factors, such as BMI, hypertension, family history of colorectal cancer, and family history of heart disease, would affect the recommendation for aspirin use. Possible harm among older patients (>70 years) was identified as the most common reason to discourage aspirin use. Conclusion: Although chemoprevention is widely discussed and offered to patients with FAP and LS by an international group of hereditary gastrointestinal cancer experts, there is significant heterogeneity in how it is applied in clinical practice. [ABSTRACT FROM AUTHOR]

Published

2023

248. Genome sequencing identifies complex structural MLH1 variant in unsolved Lynch syndrome.

Author

Witt, Dennis, Faust, Ulrike, Strobl‐Wildemann, Gertrud, Sturm, Marc, Buchert, Rebecca, Zuleger, Theresia, Admard, Jakob, Casadei, Nicolas, Ossowski, Stephan, Haack, Tobias B., Rieß, Olaf, and Schroeder, Christopher

Subjects

*HEREDITARY nonpolyposis colorectal cancer, *NUCLEOTIDE sequencing, *GENETIC variation, *DNA sequencing, *DNA mismatch repair, *EARLY detection of cancer

Abstract

Background: Lynch syndrome is one of the most common cancer predisposition syndromes. It is caused by inherited changes in the mismatch repair pathway. With current diagnostic approaches, a causative genetic variant can be found in less than 50% of cases. A correct diagnosis is important for ensuring that an appropriate surveillance program is used and that additional high‐risk family members are identified. Methods: We used clinical genome sequencing on DNA from blood and subsequent transcriptome sequencing for confirmation. Data were analyzed using the megSAP pipeline and classified according to basic criteria in diagnostic laboratories. Segregation analyses in family members were conducted via breakpoint PCR. Results: We present a family with the clinical diagnosis of Lynch syndrome in which standard diagnostic tests, such as panel or exome sequencing, were unable to detect the underlying genetic variant. Genome sequencing in the index patient confirmed the previous diagnostic results and identified an additional complex rearrangement with intronic breakpoints involving MLH1 and its neighboring gene LRRFIP2. The previously undetected structural variant was classified as medically relevant. Segregation analysis in the family identified additional at‐risk individuals which were offered intensified cancer screening. Discussion and Conclusions: This case illustrates the advantages of clinical genome sequencing in detecting structural variants compared with current diagnostic approaches. Although structural variants are rare in Lynch syndrome families, they seem to be underreported, in part because of technical challenges. Clinical genome sequencing offers a comprehensive genetic characterization detecting a wide range of genetic variants. [ABSTRACT FROM AUTHOR]

Published

2023

249. Hereditary Cancer Genes and Related Risks.

Author

TOMLINSON-HANSEN, SANDRA and BEASTON, MARCINA

Subjects

*HEREDITARY cancer syndromes, *HEREDITARY nonpolyposis colorectal cancer, *CANCER genes, *CANCER genetics, *MEDICAL societies, *TUMOR suppressor genes, *CHECKPOINT kinase 2

Abstract

The article focuses on updates in cancer genetic testing, management, and counseling. The topics covered include hereditary cancer genes such as Lynch syndrome, hereditary breast and ovarian cancer syndrome (HBOCS), and other high and moderate risk genes like PALB2, ATM, CHEK2, BRIP1, RAD51C, RAD51D, and BARD1.

Published

2023

250. Pathogenic Insights into DNA Mismatch Repair (MMR) Genes–Proteins and Microsatellite Instability: Focus on Adrenocortical Carcinoma and Beyond.

Author

Carsote, Mara, Turturea, Ionut Florin, Turturea, Maria Roxana, Valea, Ana, Nistor, Claudiu, and Gheorghisan-Galateanu, Ancuta-Augustina

Subjects

*HEREDITARY nonpolyposis colorectal cancer, *DNA mismatch repair, *MICROSATELLITE repeats, *IMMUNE checkpoint inhibitors, *GENETIC testing, *BIOMARKERS, *MOLECULAR pathology

Abstract

DNA damage repair pathways, including mismatch repair (MMR) genes, are prone to carcinoma development in certain patients. The assessment of the MMR system is widely recognized as part of strategies concerning solid tumors (defective MMR cancers), especially MMR proteins (through immunohistochemistry), and molecular assays for microsatellite instability (MSI). We aim to highlight the status of MMR genes–proteins (including MSI) in the relationship with ACC (adrenocortical carcinoma) according to current knowledge. This is a narrative review. We included PubMed-accessed, full-length English papers published between January 2012 and March 2023. We searched studies on ACC patients for whom MMR status was assessed, respectively subjects harboring MMR germline mutations, namely Lynch syndrome (LS), who were diagnosed with ACC. MMR system assessments in ACCs involve a low level of statistical evidence. Generally, there are two main types of endocrine insights: 1. the role of MMR status as a prognostic marker in different endocrine malignancies (including ACC)—which is the topic of the present work, and 2. establishing the indication of immune checkpoint inhibitors (ICPIs) in selective, mostly highly aggressive, non-responsive to standard care forms upon MMR evaluation (which belongs to the larger chapter of immunotherapy in ACCs). Our one-decade, sample-case study (which, to our knowledge, it is the most comprehensive of its kind) identified 11 original articles (from 1 patient to 634 subjects per study diagnosed with either ACC or LS). We identified four studies published in 2013 and 2020 and two in 2021, three cohorts and two retrospective studies (the publication from 2013 includes a retrospective and a cohort distinct section). Among these four studies, patients already confirmed to have LS (N = 643, respective 135) were found to be associated with ACC (N = 3, respective 2), resulting in a prevalence of 0.0046%, with a respective of 1.4% being confirmed (despite not having a large amount of similar data outside these two studies). Studies on ACC patients (N = 364, respective 36 pediatric individuals, and 94 subjects with ACC) showed that 13.7% had different MMR gene anomalies, with a respective of 8.57% (non-germline mutations), while 3.2% had MMR germline mutations (N = 3/94 cases). Two case series included one family, with a respective four persons with LS, and each article introduced one case with LS-ACC. Another five case reports (between 2018 and 2021) revealed an additional five subjects (one case per paper) diagnosed with LS and ACC (female to male ratio of 4 to 1; aged between 44 and 68). Interesting genetic testing involved children with TP53-positive ACC and further MMR anomalies or an MSH2 gene-positive subject with LS with a concurrent germline RET mutation. The first report of LS-ACC referred for PD-1 blockade was published in 2018. Nevertheless, the use of ICPI in ACCs (as similarly seen in metastatic pheochromocytoma) is still limited. Pan-cancer and multi-omics analysis in adults with ACC, in order to classify the candidates for immunotherapy, had heterogeneous results, and integrating an MMR system in this larger and challenging picture is still an open issue. Whether individuals diagnosed with LS should undergo surveillance for ACC has not yet been proven. An assessment of tumor-related MMR/MSI status in ACC might be helpful. Further algorithms for diagnostics and therapy, also taking into consideration innovative biomarkers as MMR-MSI, are necessary. [ABSTRACT FROM AUTHOR]

Published

2023