Assessing the spectrum of germline variation in Fanconi anemia genes among patients with head and neck carcinoma before age 50

Settara C. Chandrasekharappa; Steven B. Chinn; Frank X. Donovan; Naweed I. Chowdhury; Aparna Kamat; Adebowale A. Adeyemo; James W. Thomas; Meghana Vemulapalli; Caroline S. Hussey; Holly H. Reid; James C. Mullikin; Qingyi Wei; Erich M. Sturgis

doi:10.1002/cncr.30802

Assessing the spectrum of germline variation in Fanconi anemia genes among patients with head and neck carcinoma before age 50

Settara C. Chandrasekharappa, Steven B. Chinn, Frank X. Donovan, Naweed I. Chowdhury, Aparna Kamat, Adebowale A. Adeyemo, James W. Thomas, Meghana Vemulapalli, Caroline S. Hussey, Holly H. Reid, James C. Mullikin, Qingyi Wei, Erich M. Sturgis

Head & Neck Surgery

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39 Scopus citations

Abstract

BACKGROUND: Patients with Fanconi anemia (FA) have an increased risk for head and neck squamous cell carcinoma (HNSCC). The authors sought to determine the prevalence of undiagnosed FA and FA carriers among patients with HNSCC as well as an age cutoff for FA genetic screening. METHODS: Germline DNA samples from 417 patients with HNSCC aged <50 years were screened for sequence variants by targeted next-generation sequencing of the entire length of 16 FA genes. RESULTS: The sequence revealed 194 FA gene variants in 185 patients (44%). The variant spectrum was comprised of 183 nonsynonymous point mutations, 9 indels, 1 large deletion, and 1 synonymous variant that was predicted to effect splicing. One hundred eight patients (26%) had at least 1 rare variant that was predicted to be damaging, and 57 (14%) had at least 1 rare variant that was predicted to be damaging and had been previously reported. Fifteen patients carried 2 rare variants or an X-linked variant in an FA gene. Overall, an age cutoff for FA screening was not identified among young patients with HNSCC, because there were no significant differences in mutation rates when patients were stratified by age, tumor site, ethnicity, smoking status, or human papillomavirus status. However, an increased burden, or mutation load, of FA gene variants was observed in carriers of the genes FA complementation group D2 (FANCD2), FANCE, and FANCL in the HNSCC patient cohort relative to the 1000 Genomes population. CONCLUSIONS: FA germline functional variants offer a novel area of study in HNSCC tumorigenesis. FANCE and FANCL, which are components of the core complex, are known to be responsible for the recruitment and ubiquitination, respectively, of FANCD2, a critical step in the FA DNA repair pathway. In the current cohort, the increased mutation load of FANCD2, FANCE, and FANCL variants among younger patients with HNSCC indicates the importance of the FA pathway in HNSCC. Cancer 2017;123:3943-54.

Original language	English (US)
Pages (from-to)	3943-3954
Number of pages	12
Journal	Cancer
Volume	123
Issue number	20
DOIs	https://doi.org/10.1002/cncr.30802
State	Published - Oct 15 2017

Keywords

Fanconi anemia
germline variations
head and neck cancers
recessive inherited disorders
squamous cell carcinoma

ASJC Scopus subject areas

Oncology
Cancer Research

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10.1002/cncr.30802

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Chandrasekharappa, S. C., Chinn, S. B., Donovan, F. X., Chowdhury, N. I., Kamat, A., Adeyemo, A. A., Thomas, J. W., Vemulapalli, M., Hussey, C. S., Reid, H. H., Mullikin, J. C., Wei, Q., & Sturgis, E. M. (2017). Assessing the spectrum of germline variation in Fanconi anemia genes among patients with head and neck carcinoma before age 50. Cancer, 123(20), 3943-3954. https://doi.org/10.1002/cncr.30802

Chandrasekharappa, SC, Chinn, SB, Donovan, FX, Chowdhury, NI, Kamat, A, Adeyemo, AA, Thomas, JW, Vemulapalli, M, Hussey, CS, Reid, HH, Mullikin, JC, Wei, Q & Sturgis, EM 2017, 'Assessing the spectrum of germline variation in Fanconi anemia genes among patients with head and neck carcinoma before age 50', Cancer, vol. 123, no. 20, pp. 3943-3954. https://doi.org/10.1002/cncr.30802

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title = "Assessing the spectrum of germline variation in Fanconi anemia genes among patients with head and neck carcinoma before age 50",

abstract = "BACKGROUND: Patients with Fanconi anemia (FA) have an increased risk for head and neck squamous cell carcinoma (HNSCC). The authors sought to determine the prevalence of undiagnosed FA and FA carriers among patients with HNSCC as well as an age cutoff for FA genetic screening. METHODS: Germline DNA samples from 417 patients with HNSCC aged <50 years were screened for sequence variants by targeted next-generation sequencing of the entire length of 16 FA genes. RESULTS: The sequence revealed 194 FA gene variants in 185 patients (44%). The variant spectrum was comprised of 183 nonsynonymous point mutations, 9 indels, 1 large deletion, and 1 synonymous variant that was predicted to effect splicing. One hundred eight patients (26%) had at least 1 rare variant that was predicted to be damaging, and 57 (14%) had at least 1 rare variant that was predicted to be damaging and had been previously reported. Fifteen patients carried 2 rare variants or an X-linked variant in an FA gene. Overall, an age cutoff for FA screening was not identified among young patients with HNSCC, because there were no significant differences in mutation rates when patients were stratified by age, tumor site, ethnicity, smoking status, or human papillomavirus status. However, an increased burden, or mutation load, of FA gene variants was observed in carriers of the genes FA complementation group D2 (FANCD2), FANCE, and FANCL in the HNSCC patient cohort relative to the 1000 Genomes population. CONCLUSIONS: FA germline functional variants offer a novel area of study in HNSCC tumorigenesis. FANCE and FANCL, which are components of the core complex, are known to be responsible for the recruitment and ubiquitination, respectively, of FANCD2, a critical step in the FA DNA repair pathway. In the current cohort, the increased mutation load of FANCD2, FANCE, and FANCL variants among younger patients with HNSCC indicates the importance of the FA pathway in HNSCC. Cancer 2017;123:3943-54.",

keywords = "Fanconi anemia, germline variations, head and neck cancers, recessive inherited disorders, squamous cell carcinoma",

author = "Chandrasekharappa, {Settara C.} and Chinn, {Steven B.} and Donovan, {Frank X.} and Chowdhury, {Naweed I.} and Aparna Kamat and Adeyemo, {Adebowale A.} and Thomas, {James W.} and Meghana Vemulapalli and Hussey, {Caroline S.} and Reid, {Holly H.} and Mullikin, {James C.} and Qingyi Wei and Sturgis, {Erich M.}",

note = "Publisher Copyright: {\textcopyright} 2017 American Cancer Society",

year = "2017",

month = oct,

day = "15",

doi = "10.1002/cncr.30802",

language = "English (US)",

volume = "123",

pages = "3943--3954",

journal = "Cancer",

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T1 - Assessing the spectrum of germline variation in Fanconi anemia genes among patients with head and neck carcinoma before age 50

AU - Chandrasekharappa, Settara C.

AU - Chinn, Steven B.

AU - Donovan, Frank X.

AU - Chowdhury, Naweed I.

AU - Kamat, Aparna

AU - Adeyemo, Adebowale A.

AU - Thomas, James W.

AU - Vemulapalli, Meghana

AU - Hussey, Caroline S.

AU - Reid, Holly H.

AU - Mullikin, James C.

AU - Wei, Qingyi

AU - Sturgis, Erich M.

PY - 2017/10/15

Y1 - 2017/10/15

N2 - BACKGROUND: Patients with Fanconi anemia (FA) have an increased risk for head and neck squamous cell carcinoma (HNSCC). The authors sought to determine the prevalence of undiagnosed FA and FA carriers among patients with HNSCC as well as an age cutoff for FA genetic screening. METHODS: Germline DNA samples from 417 patients with HNSCC aged <50 years were screened for sequence variants by targeted next-generation sequencing of the entire length of 16 FA genes. RESULTS: The sequence revealed 194 FA gene variants in 185 patients (44%). The variant spectrum was comprised of 183 nonsynonymous point mutations, 9 indels, 1 large deletion, and 1 synonymous variant that was predicted to effect splicing. One hundred eight patients (26%) had at least 1 rare variant that was predicted to be damaging, and 57 (14%) had at least 1 rare variant that was predicted to be damaging and had been previously reported. Fifteen patients carried 2 rare variants or an X-linked variant in an FA gene. Overall, an age cutoff for FA screening was not identified among young patients with HNSCC, because there were no significant differences in mutation rates when patients were stratified by age, tumor site, ethnicity, smoking status, or human papillomavirus status. However, an increased burden, or mutation load, of FA gene variants was observed in carriers of the genes FA complementation group D2 (FANCD2), FANCE, and FANCL in the HNSCC patient cohort relative to the 1000 Genomes population. CONCLUSIONS: FA germline functional variants offer a novel area of study in HNSCC tumorigenesis. FANCE and FANCL, which are components of the core complex, are known to be responsible for the recruitment and ubiquitination, respectively, of FANCD2, a critical step in the FA DNA repair pathway. In the current cohort, the increased mutation load of FANCD2, FANCE, and FANCL variants among younger patients with HNSCC indicates the importance of the FA pathway in HNSCC. Cancer 2017;123:3943-54.

AB - BACKGROUND: Patients with Fanconi anemia (FA) have an increased risk for head and neck squamous cell carcinoma (HNSCC). The authors sought to determine the prevalence of undiagnosed FA and FA carriers among patients with HNSCC as well as an age cutoff for FA genetic screening. METHODS: Germline DNA samples from 417 patients with HNSCC aged <50 years were screened for sequence variants by targeted next-generation sequencing of the entire length of 16 FA genes. RESULTS: The sequence revealed 194 FA gene variants in 185 patients (44%). The variant spectrum was comprised of 183 nonsynonymous point mutations, 9 indels, 1 large deletion, and 1 synonymous variant that was predicted to effect splicing. One hundred eight patients (26%) had at least 1 rare variant that was predicted to be damaging, and 57 (14%) had at least 1 rare variant that was predicted to be damaging and had been previously reported. Fifteen patients carried 2 rare variants or an X-linked variant in an FA gene. Overall, an age cutoff for FA screening was not identified among young patients with HNSCC, because there were no significant differences in mutation rates when patients were stratified by age, tumor site, ethnicity, smoking status, or human papillomavirus status. However, an increased burden, or mutation load, of FA gene variants was observed in carriers of the genes FA complementation group D2 (FANCD2), FANCE, and FANCL in the HNSCC patient cohort relative to the 1000 Genomes population. CONCLUSIONS: FA germline functional variants offer a novel area of study in HNSCC tumorigenesis. FANCE and FANCL, which are components of the core complex, are known to be responsible for the recruitment and ubiquitination, respectively, of FANCD2, a critical step in the FA DNA repair pathway. In the current cohort, the increased mutation load of FANCD2, FANCE, and FANCL variants among younger patients with HNSCC indicates the importance of the FA pathway in HNSCC. Cancer 2017;123:3943-54.

KW - Fanconi anemia

KW - germline variations

KW - head and neck cancers

KW - recessive inherited disorders

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Assessing the spectrum of germline variation in Fanconi anemia genes among patients with head and neck carcinoma before age 50

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