Interplay between Tumor Mutational Burden and Mutational Profile and Its Effect on Overall Survival: A Pilot Study of Metastatic Patients Treated with Immune Checkpoint Inhibitors

Xavier, Camila Bragança; Lopes, Carlos Diego Holanda; Awni, Beatriz Mendes; Campos, Eduardo Felicio; Alves, Joao Pedro B.; Camargo, Anamaria A.; Guardia, Gabriela D. A.; Galante, Pedro A. F.; Jardim, Denis Leonardo Fontes

doi:10.3390/cancers14215433

Cited by 4 publications

(2 citation statements)

References 26 publications

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“…The FAM46C gene was originally identified as mutated in 13% of the cases analysed by Chapman and colleagues in their 2011 parallel sequencing of 38 MM patient genomes/exomes [5]. Later, similar mutation frequencies were confirmed by others using techniques ranging from fluorescence in situ hybridization (FISH) approaches to genetargeted next generation sequencing (NGS) [45][46][47][48][49][50][51][52][53]. Mutation mapping revealed alterations throughout the entire ORF of FAM46C, with an exception in a small portion of the Nterminal region, with most mutations being either indels or missense single nucleotide variations predicted to have a deleterious effect on protein structure/functionality [54], suggesting that FAM46C behaves as a tumour suppressor gene.…”

Section: The Fam46c Gene and Its Mutations In Cancermentioning

confidence: 98%

Dissecting the Puzzling Roles of FAM46C: A Multifaceted Pan-Cancer Tumour Suppressor with Increasing Clinical Relevance

Lai,

De Grossi,

Catusi

et al. 2024

Cancers

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FAM46C is a well-established tumour suppressor with a role that is not completely defined or universally accepted. Although FAM46C expression is down-modulated in several tumours, significant mutations in the FAM46C gene are only found in multiple myeloma (MM). Consequently, its tumour suppressor activity has primarily been studied in the MM context. However, emerging evidence suggests that FAM46C is involved also in other cancer types, namely colorectal, prostate and gastric cancer and squamous cell and hepatocellular carcinoma, where FAM46C expression was found to be significantly reduced in tumoural versus non-tumoural tissues and where FAM46C was shown to possess anti-proliferative properties. Accordingly, FAM46C was recently proposed to function as a pan-cancer prognostic marker, bringing FAM46C under the spotlight and attracting growing interest from the scientific community in the pathways modulated by FAM46C and in its mechanistic activity. Here, we will provide the first comprehensive review regarding FAM46C by covering (1) the intracellular pathways regulated by FAM46C, namely the MAPK/ERK, PI3K/AKT, β-catenin and TGF-β/SMAD pathways; (2) the models regarding its mode of action, specifically the poly(A) polymerase, intracellular trafficking modulator and inhibitor of centriole duplication models, focusing on connections and interdependencies; (3) the regulation of FAM46C expression in different environments by interferons, IL-4, TLR engagement or transcriptional modulators; and, lastly, (4) how FAM46C expression levels associate with increased/decreased tumour cell sensitivity to anticancer agents, such as bortezomib, dexamethasone, lenalidomide, pomalidomide, doxorubicin, melphalan, SK1-I, docetaxel and norcantharidin.

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Section: The Fam46c Gene and Its Mutations In Cancermentioning

confidence: 98%

Dissecting the Puzzling Roles of FAM46C: A Multifaceted Pan-Cancer Tumour Suppressor with Increasing Clinical Relevance

Lai,

De Grossi,

Catusi

et al. 2024

Cancers

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“…Although the ≥10 mutations/Mb cut-off (TMB-high) has been used for the FDA approval of pembrolizumab for patients’ treatment, still a sizeable proportion of patients with TMB-high tumors do not respond to this type of ICI, making it necessary to identify additional molecular alterations that influence the TMB, which could assist in a better patient selection for immunotherapy. In this respect, the study by Xavier et al [ 11 ] investigated the mutational profiles of patients from the study by Samstein et al [ 12 ], which examined the association between TMB-high and survival outcomes in patients receiving ICI across a wide variety of cancer types. The authors could identify mutations in 27 genes which, in univariate analyses, correlated significantly with OS upon treatment with immune checkpoint inhibitors when tumors with TMB ≥ 10 mut/Mb were assessed.…”

mentioning

confidence: 99%

Biomarkers in the Era of Precision Oncology

Baxevanis

2023

Cancers

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A 20-gene mutation signature predicts the efficacy of immune checkpoint inhibitor therapy in advanced non-small cell lung cancer patients

Guo

Shi

et al. 2023

BMC Pulm Med

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Background There is an unmet need to identify novel predictive biomarkers that enable more accurate identification of individuals who can benefit from immune checkpoint inhibitor (ICI) therapy. The US FDA recently approved tumor mutational burden (TMB) score of ≥ 10 mut/Mb as a threshold for pembrolizumab treatment of solid tumors. Our study aimed to test the hypothesis that specific gene mutation signature may predict the efficacy of ICI therapy more precisely than high TMB (≥ 10). Methods We selected 20 candidate genes that may predict for the efficacy of ICI therapy by the analysis of data from a published cohort of 350 advanced non-small cell lung cancer (NSCLC) patients. Then, we compared the influences of various gene mutation signatures on the efficacy of ICI treatment. They were also compared with PD-L1 and TMB. The Kaplan-Meier method was utilized to evaluate the prognosis univariates, while selected univariates were adopted to develop a systematic nomogram. Results A high mutation signature, where three or more of the 20 selected genes were mutated, was associated with the significant benefits of ICI therapy. Specifically, patients with high mutation signature were confirmed to have better prognosis for ICI treatment, compared with those with wild type (the median PFS: 7.17 vs. 2.90 months, p = 0.0004, HR = 0.47 (95% [CI]:0.32–0.68); the median OS: unreached vs. 9 months, p = 1.8E-8, HR = 0.17 (95% [CI]:0.11–0.25)). Moreover, those patients with the high mutation signature achieved significant ICI treatment benefits, while there was no difference of OS and PFS between patients without the signature but TMB-H (≥ 10) and those without the signature and low TMB(< 10). Finally, we constructed a novel nomogram to evaluate the efficacy of ICI therapy. Conclusion A high mutational signature with 3 or more of the 20-gene panel could provide more accurate predictions for the outcomes of ICI therapy than TMB ≥ 10 in NSCLC patients.

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Interplay between Tumor Mutational Burden and Mutational Profile and Its Effect on Overall Survival: A Pilot Study of Metastatic Patients Treated with Immune Checkpoint Inhibitors

Cited by 4 publications

References 26 publications

Dissecting the Puzzling Roles of FAM46C: A Multifaceted Pan-Cancer Tumour Suppressor with Increasing Clinical Relevance

Dissecting the Puzzling Roles of FAM46C: A Multifaceted Pan-Cancer Tumour Suppressor with Increasing Clinical Relevance

Biomarkers in the Era of Precision Oncology

A 20-gene mutation signature predicts the efficacy of immune checkpoint inhibitor therapy in advanced non-small cell lung cancer patients

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