Characteristics of Mismatch Repair–Deficient Colon Cancer in Relation to Mismatch Repair Protein Loss, Hypermethylation Silencing, and Constitutional and Biallelic Somatic Mismatch Repair Gene Pathogenic Variants. Issue 4 (20th June 2022)
- Record Type:
- Journal Article
- Title:
- Characteristics of Mismatch Repair–Deficient Colon Cancer in Relation to Mismatch Repair Protein Loss, Hypermethylation Silencing, and Constitutional and Biallelic Somatic Mismatch Repair Gene Pathogenic Variants. Issue 4 (20th June 2022)
- Main Title:
- Characteristics of Mismatch Repair–Deficient Colon Cancer in Relation to Mismatch Repair Protein Loss, Hypermethylation Silencing, and Constitutional and Biallelic Somatic Mismatch Repair Gene Pathogenic Variants
- Authors:
- Keshinro, Ajaratu
Ganesh, Karuna
Vanderbilt, Chad
Firat, Canan
Kim, Jin K.
Chen, Chin-Tung
Yaeger, Rona
Segal, Neil H.
Gonen, Mithat
Shia, Jinru
Stadler, Zsofia K.
Weiser, Martin R. - Abstract:
- Abstract : BACKGROUND: Mismatch repair–deficient colon cancer is heterogeneous. Differentiating inherited constitutional variants from somatic genetic alterations and gene silencing is important for surveillance and genetic counseling. OBJECTIVE: This study aimed to determine the extent to which the underlying mechanism of loss of mismatch repair influences molecular and clinicopathologic features of microsatellite instability-high colon cancer. DESIGN: This is a retrospective analysis. SETTINGS: This study was conducted at a comprehensive cancer center. PATIENTS: Patients with microsatellite instability-high colon cancer of stage I, II, or III were included. INTERVENTION: Patients underwent a curative surgical resection. MAIN OUTCOME MEASURES: The main outcome measures were hypermethylation of the MLH1 promoter, biallelic inactivation, constitutional pathogenic variants, and loss of specific mismatch repair proteins. RESULTS: Of the 157 identified tumors with complete genetic analysis, 66% had hypermethylation of the MLH1 promoter, 18% had constitutional pathogenic variants, (Lynch syndrome), 11% had biallelic somatic mismatch repair gene pathogenic variants, and 6% had unexplained high microsatellite instability. The distribution of mismatch repair loss was as follows: MLH1 and PMS2 co-loss, 79% of the tumors; MSH2 and MSH6 co-loss, 10%; MSH6 alone, 3%; PMS2 alone, 2%; other combinations, 2%; no loss, 2%. Tumor mutational burden was lowest in MLH1- and PMS2-deficientAbstract : BACKGROUND: Mismatch repair–deficient colon cancer is heterogeneous. Differentiating inherited constitutional variants from somatic genetic alterations and gene silencing is important for surveillance and genetic counseling. OBJECTIVE: This study aimed to determine the extent to which the underlying mechanism of loss of mismatch repair influences molecular and clinicopathologic features of microsatellite instability-high colon cancer. DESIGN: This is a retrospective analysis. SETTINGS: This study was conducted at a comprehensive cancer center. PATIENTS: Patients with microsatellite instability-high colon cancer of stage I, II, or III were included. INTERVENTION: Patients underwent a curative surgical resection. MAIN OUTCOME MEASURES: The main outcome measures were hypermethylation of the MLH1 promoter, biallelic inactivation, constitutional pathogenic variants, and loss of specific mismatch repair proteins. RESULTS: Of the 157 identified tumors with complete genetic analysis, 66% had hypermethylation of the MLH1 promoter, 18% had constitutional pathogenic variants, (Lynch syndrome), 11% had biallelic somatic mismatch repair gene pathogenic variants, and 6% had unexplained high microsatellite instability. The distribution of mismatch repair loss was as follows: MLH1 and PMS2 co-loss, 79% of the tumors; MSH2 and MSH6 co-loss, 10%; MSH6 alone, 3%; PMS2 alone, 2%; other combinations, 2%; no loss, 2%. Tumor mutational burden was lowest in MLH1- and PMS2-deficient tumors. MSH6-deficient tumors had the lowest levels of tumor-infiltrating lymphocytes, lowest MSI scores, and fewest frameshift deletions. Patients with MLH1 promoter hypermethylation were significantly more likely to be older and female and to have right-sided colon lesions than patients with biallelic inactivation. Mutation was the most prevalent second hit in tumors with biallelic inactivation and tumors of patients with Lynch syndrome. LIMITATIONS: This study was limited by potential selection or referral bias, missing data for some patients, and relatively small sizes of some subgroups. CONCLUSIONS: Clinical characteristics of mismatch repair–deficient colon cancer vary with the etiology of microsatellite instability, and its molecular characteristics vary with the affected mismatch repair protein. See Video Abstract at http://links.lww.com/DCR/B984 . CARACTERÍSTICAS DEL CÁNCER DE COLON CON DEFICIENCIA EN LA REPARACIÓN DE ERRORES DE EMPAREJAMIENTO EN RELACIÓN CON LA PÉRDIDA DE PROTEÍNAS MMR, SILENCIAMIENTO DE LA HIPERMETILACIÓN Y LAS VARIANTES PATÓGENAS SOMÁTICAS DE GENES MMR CONSTITUCIONAL Y BIALÉLICO: ANTECEDENTES: El cáncer de colon deficiente en la reparación de errores de emparejamiento es heterogéneo. La diferenciación de las variantes constitucionales heredadas de las alteraciones genéticas somáticas y el silenciamiento de genes es importante para la vigilancia y el asesoramiento genético. OBJETIVO: Determinar hasta qué punto el mecanismo subyacente de pérdida de reparación de desajustes influye en las características moleculares y clinicopatológicas del cáncer de colon con alta inestabilidad de microsatélites. DISEÑO: Análisis retrospectivo. ESCENARIO: Centro integral de cáncer. PACIENTES: Pacientes con cáncer de colon con inestabilidad de microsatélites alta en estadio I, II, o III. INTERVENCIÓN: Resección quirúrgica con intención curativa. PRINCIPALES RESULTADOS Y MEDIDAS: Hipermetilación del promotor MLH1, inactivación bialélica, variante patógena constitucional y pérdida de proteínas específicas reparadoras de desajustes. RESULTADOS: De los 157 tumores identificados con un análisis genético completo, el 66 % tenía hipermetilación del promotor MLH1, el 18 % tenía una variante patogénica constitucional (síndrome de Lynch), el 11 % tenía variantes patogénicas somáticas bialélicas de algún gen MMR y el 6 % tenía una alta inestabilidad de microsatélites sin explicación. La distribución de la pérdida según la proteína de reparación del desajuste fue la siguiente: pérdida conjunta de MLH1 y PMS2, 79 % de los tumores; co-pérdida de MSH2 y MSH6, 10%; MSH6 solo, 3%; PMS2 solo, 2%; otras combinaciones, 2%; sin pérdida, 2%. La carga mutacional del tumor fue más baja en los tumores deficientes en MLH1 y PMS2. Los tumores con deficiencia de MSH6 tenían los niveles más bajos de linfocitos infiltrantes de tumores, las puntuaciones más bajas del sensor de IMS y la menor cantidad de deleciones por cambio de marco. Los pacientes con hipermetilación del promotor MLH1 tenían significativamente más probabilidades de ser mayores y mujeres y de tener lesiones en el colon derecho que los pacientes con inactivación bialélica. La mutación fue el segundo golpe más frecuente en tumores con inactivación bialélica y tumores de pacientes con síndrome de Lynch. LIMITACIONES: Sesgo potencial de selección o referencia, datos faltantes para algunos pacientes y tamaños relativamente pequeños de algunos subgrupos. CONCLUSIONES: Las características clínicas del cáncer de colon deficiente en reparación de desajustes varían con la etiología de la inestabilidad de microsatélites, y sus características moleculares varían con la proteína de reparación de desajustes afectada. Vea Resumen de video en http://links.lww.com/DCR/B984 . (Traducción—Dr. Felipe Bellolio ) … (more)
- Is Part Of:
- Diseases of the colon & rectum. Volume 66:Issue 4(2023)
- Journal:
- Diseases of the colon & rectum
- Issue:
- Volume 66:Issue 4(2023)
- Issue Display:
- Volume 66, Issue 4 (2023)
- Year:
- 2023
- Volume:
- 66
- Issue:
- 4
- Issue Sort Value:
- 2023-0066-0004-0000
- Page Start:
- 549
- Page End:
- 558
- Publication Date:
- 2022-06-20
- Subjects:
- Biallelic somatic pathogenic variants -- Colon cancer -- Constitutional pathogenic variants -- Hypermethylation -- Lynch syndrome -- Microsatellite instability -- Mismatch repair deficiency
Colon (Anatomy) -- Diseases -- Periodicals
Rectum -- Diseases -- Periodicals
Colonic Diseases -- Periodicals
Colorectal Surgery -- Periodicals
616.34 - Journal URLs:
- http://journals.lww.com/dcrjournal/Pages/default.aspx ↗
http://journals.lww.com ↗ - DOI:
- 10.1097/DCR.0000000000002452 ↗
- Languages:
- English
- ISSNs:
- 0012-3706
- Deposit Type:
- Legaldeposit
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- Available online (eLD content is only available in our Reading Rooms) ↗
- Physical Locations:
- British Library DSC - 3598.200000
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- 26127.xml