July 21, 2015
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Epstein-Barr virus DNA may predict treatment efficacy for advanced nasopharyngeal cancer

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Plasma Epstein-Barr virus DNA may serve as the most significant prognostic biomarker for adjuvant therapy selection in patients with nasopharyngeal cancer, according to study results.

Perspective from Barbara Ann Burtness, MD

Further, the excision repair cross-contaminating group 1 codon 118 (ERCC1 C118T) genotype may help identify a favorable subgroup of plasma Epstein-Barr virus–negative patients who would not benefit from adjuvant therapy, according to the study researchers.

“Cisplatin combined with radiotherapy is the current standard treatment for patients with advanced nasopharyngeal cancer," Anthony T.C. Chan, MD, associate dean of medicine and professor and chairman of clinical oncology at The Chinese University of Hong Kong, and colleagues wrote. “However, the addition of cisplatin leads to added toxicities, which narrow the ultimate therapeutic gain. Therefore, the ability to identify patients who cannot benefit from cisplatin may render a more personalized therapy and maximize the therapeutic ratio.”

Single nucleotide polymorphism (SNP) of the ERCC1 gene may indicate sensitivity to platinum and radiation, according to study background.

Chan and colleagues surmised that the ERCC1 genotype for the SNPs cytosine-to-thymine substitution at codon 118T (C118T) and cytosine-to-adenine substitution at codon 8092 (C8092A) is prognostic for patients with nasopharyngeal cancer who receive radiotherapy alone or with cisplatin.

Researchers evaluated biomarker screening samples from the Hong Kong NPC Study Group 0502, which used post-radiotherapy plasma Epstein-Barr virus (pEBV) DNA levels to screen patients with advanced nasopharyngeal cancer for the use of adjuvant chemotherapy.

The analysis included ERCC1 SNPs from 576 consecutive patients screened by pEBV. Overall, the ECRR1 C118T or C8092A genotypes were not significantly associated with OS or RFS in the study population. Further, researchers observed no correlation between ERCC1 genotype and the ERCC1 protein or messenger RNA expression among patients with available paired biopsies.

However, ERCC1 C118T genotype significantly interacted with post-radiotherapy pEBV status for RFS (P = .0106) and OS (P = .0067). The ERCC1 C118T genotype was significantly associated with RFS (HR = 1.67; 95% CI, 1.07-2.61) and OS (HR = 2.31; 95% CI, 1.22-4.4) in the post-radiotherapy pEBV-negative population, but not in the pEBV-positive population.

“The current results validate the pEBV level as the most significant prognostic biomarker in nasopharyngeal cancer, and it is being used in the first biomarker-based, randomized, controlled clinical trial to select patients with high-risk nasopharyngeal cancer for adjuvant therapy,” Chan and colleagues concluded. “The ERCC1 C118T T/T genotype may help to identify a favorable subgroup (approximately 7%) of patients with pEBV-negative nasopharyngeal cancer who have an excellent prognosis (3-year RFS 96%; OS, 100%) who could be spared the toxicities of additional therapy.”

Patient characteristics may account for some of these outcomes, Wendy Hara, MD, and Quynh-Thu Le, MD, both of the department of radiation oncology at Stanford University School of Medicine, wrote in an accompanying editorial.

“A closer look [at Supporting Table 2 in their article] suggests that patients in the TT genotype group had less advanced lymph node disease and stage IV tumors, which may explain their better outcomes,” Hara and Le wrote. “Although the authors observed no interaction between treatment and ERCC1 C118T genotype, it is still not clear which patients received radiotherapy alone and which received chemoradiotherapy. … These findings have generated a hypothesis that will need validation in future studies, as the authors rightly point out.”

Despite potential limitations, study findings may lead to more effective personalized treatment, Hara and Lee concluded.

“[Hui and colleagues] should be commended for their important work confirming that post-treatment EBV DNA levels remain a strong biomarker for survival in patients with nasopharyngeal cancer in the modern era,” they wrote. “Stratifications of patients by appropriate biomarkers hopefully will lead to more individualized treatments and allow us to spare low-risk patients from excessive therapy while identifying high-risk patients who need treatment intensification.” – by Cameron Kelsall

Disclosure: Chan reports no relevant financial disclosures. One researcher reports receiving personal fees from Novartis and nonfinancial support from Pfizer and SIRTEX. Hara and Le report no relevant financial disclosures.