BIRC2–BIRC3 amplification: a potentially druggable feature of a subset of head and neck cancers in patients with Fanconi anemia

Roohollahi, Khashayar; Jong, Yvonne de; Pai, Govind; Zaini, Mohamad Amr; Lint, Klaas de; Sie, Daoud; Rooimans, Martin A.; Rockx, Davy; Hoskins, Elizabeth E.; Ameziane, Najim; Wolthuis, Rob M. F.; Joenje, Hans; Wells, Susanne I.; Dorsman, Josephine C.

doi:10.1038/s41598-021-04042-9

Cited by 10 publications

(17 citation statements)

References 51 publications

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“…In addition, we also found the germline mutations in the FANCA gene that had previously been diagnosed in all three FA patients [27] (Supplementary Table 3). These results are in line with the frequent detection of TP53 alterations in SCC from FA patients [19][20][21]. Therefore, animal models resembling germline FANCA and somatic TP53 mutations might model SCC in FA.…”

Section: Resultssupporting

confidence: 85%

“…Therefore, additional genetic events are needed. We have found TP53 mutations in all five HNSCC from three FA patients (Supplementary Table 3, Supplementary Table 4), which is in agreement with the high frequency of mutations or deletions in TP53 described in HPVnegative, FA [18][19][20][21] and non-FA patients [34][35][36]. In addition, TP53 mutations are early events during HPV-negative HNSCC carcinogenesis in non-FA patients [37,38].…”

Section: Discussionsupporting

confidence: 87%

“…Most HNSCCs from FA patients display alterations typically found in HPVnegative HNSCC tumors from the general population, such as mutations in the TP53 gene [18][19][20][21]. Here, we also detected mutations in TP53 in all five SCCs analyzed from the oral cavity of three FA patients.…”

Section: Introductionsupporting

confidence: 60%

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Development of a mouse model for spontaneous oral squamous cell carcinoma in Fanconi anemia

Errazquin

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Suñol

et al. 2022

Preprint

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Fanconi anemia (FA) patients frequently develop oral squamous cell carcinoma (OSCC). This cancer in FA is diagnosed within the first 3-4 decades of life, and patients respond poorly to current treatments, mainly radiotherapy and chemotherapy. In addition, FA patients develop oral lesions very often that might precede malignant transformation. Research and translation of new chemopreventive and therapeutic strategies has been unsuccessful in part because disease models are scarce or do not fully reproduce the disease. Here we report that Fanca gene knockout mice (Fanca-/-) frequently display pre-malignant lesions in the oral cavity. Moreover, when these animals were crossed with animals having conditional deletion of p53 gene in oral mucosa (K14cre;Trp53F2-10/F2-10) spontaneously develop OSCC with high penetrance and a median latency of less than ten months. Tumors are well differentiated and express markers of squamous differentiation, such as K5 and K10 keratins. In conclusion, Fanca and p53 genes cooperate to suppress oral cancer in mice, and Fanca-/-;K14cre;Trp53F2-10/F2-10 constitute the first animal model of spontaneous OSCC in FA.

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Section: Resultssupporting

confidence: 85%

Section: Discussionsupporting

confidence: 87%

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Development of a mouse model for spontaneous oral squamous cell carcinoma in Fanconi anemia

Errazquin

Page

Suñol

et al. 2022

Preprint

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“…FA-CCLR cell lines displayed both HNSCC- as well as FA-associated genomic alterations (9,12,13,31–33). Figure 2 summarizes cell line-specific single nucleotide (SNV) and copy number (CNV) variant data for cell lines where we had full data access and compares these lines with HPV-negative HNSCC samples included in TCGA data (n = 426; (19)).…”

Section: Resultsmentioning

confidence: 99%

“…Copy-number amplifications and deletions for OHSU-SCC-974, CCH-SCC-FA1 and CCH-SCC-FA2 were called using CNVkit (16) to compare tumor cell line and patient matched WGS data. SNV/indels and copy-number amplifications and deletions were called for FA patient-derived cell lines VU-SCC-1604, VU-SCC-1365 and VU-SCC1131 using, respectively, Mutect2 (17) and CNVkit to compare tumor cell line and patient matched fibroblast whole-exome sequencing (WES) data (13), with a focus on variant calling in significantly mutated genes considered to be HNSCC drivers when altered (9,18,19). Somatic mutation data for sporadic HNSCC cell lines JHU-SCC-FaDu, CAL-SCC-27, CAL-SCC-33, SFCI-SCC-09 and UM-SCC-01 were extracted from the Broad Institute Cancer Cell Line Encyclopedia (CCLE)(10), employing Mutect2 and Absolute (20) for SNV/indel and copy-number analyses.…”

Section: Methodsmentioning

confidence: 99%

Fanconi anemia-isogenic head and neck cancer cell line pairs - a basic and translational science resource

Nguyen

Tang

Webster

et al. 2022

Preprint

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Fanconi anemia (FA) is a heritable malformation, bone marrow failure and cancer predisposition syndrome that confers an exceptionally high risk of developing carcinomas arising in squamous mucosal epithelia lining the mouth, proximal esophagus, vulva and anus. The origin of these cancers is not understood, and no effective way has been identified to prevent or delay their appearance. FA-associated carcinomas are also therapeutically challenging, as they may be multi-focal and stage-advanced at diagnosis making surgical control challenging. Moreover, individuals with FA have systemic DNA damage hypersensitivity and thus an elevated risk of toxicity when treated with standard-of-care therapies such as DNA cross-linking drugs and ionizing radiation. We developed the Fanconi Anemia Cancer Cell Line Resource (FA-CCLR) in order to foster new research on the origins, treatment, and prevention of FA-associated cancers. The FA-CCLR consists of FANC-isogenic head and neck squamous cell carcinoma (HNSCC) cell line pairs from cancers arising in individuals with FA, or newly engineered from sporadic HNSCC cell lines. Molecular, cellular, and biochemical analyses were used to demonstrate the causal dependence of key FA-associated phenotypes on FANC genotype, expression and pathway activity. These FANC-isogenic cell line pairs are available to academic and non-profit investigators, with ordering information available at the Fanconi Anemia Research Materials Resource and Repository at Oregon Health & Sciences University, Portland OR.

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The expanding role of IAP antagonists for the treatment of head and neck cancer

et al. 2023

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Inhibitors of apoptosis proteins (IAPs) inhibit the intrinsic and extrinsic cell death pathways, promoting cell survival. Antagonists of these pathways are under study as anti‐cancer therapeutics. A high proportion of head and neck squamous cell carcinomas (HNSCCs) have genomic alterations in IAP pathways, resulting in the dysregulation of cell death pathways and rendering them susceptible to IAP antagonist therapy. Preclinical studies suggest IAP antagonists, also known as second mitochondria‐derived activator of caspases mimetics, may be effective treatments for HNSCC, especially when combined with radiation. Mechanistic studies have shown both molecular mechanisms (i.e., enhanced cell death) and immune mechanisms (e.g., immunogenic cell death and T‐cell activation), underlying the efficacy of these drugs in preclinical models. Phase I/II clinical trials have shown promising results, portending a future where this class of targeted therapies becomes incorporated into the treatment paradigm for head and neck cancers. IAP antagonists have shown great promise for head and neck cancer, especially in combination with radiation therapy. Here, we review recent preclinical and clinical studies on the use of these novel targeted agents for head and neck cancer.

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BIRC2–BIRC3 amplification: a potentially druggable feature of a subset of head and neck cancers in patients with Fanconi anemia

Cited by 10 publications

References 51 publications

Development of a mouse model for spontaneous oral squamous cell carcinoma in Fanconi anemia

Development of a mouse model for spontaneous oral squamous cell carcinoma in Fanconi anemia

Fanconi anemia-isogenic head and neck cancer cell line pairs - a basic and translational science resource

The expanding role of IAP antagonists for the treatment of head and neck cancer

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