Abstract
Human papillomavirus positive (HPV+) oropharyngeal squamous cell carcinoma (OPC) is a distinct clinical entity within the head and neck cancers, with a unique epidemiology and, in general, a favorable prognosis. Because of this favorable prognosis, researchers have considered de-intensifying the current standard treatment of HPV+ OPC in order to reduce acute and late treatment related toxicity without compromising outcome. Current ongoing trials can be divided in three main categories: de-intensification of the chemotherapy by replacing concomitant platinum-based chemotherapy with the EGFR-inhibitor cetuximab, or de-intensification of the radiation dose of either the primary radiotherapy of selected, good-responding patients after induction chemotherapy or of the adjuvant radiotherapy based on pathology features after primary surgery. Despite the good prognosis of the majority of HPV+ OPC patients, a proportion of them still have poor prognosis. This unmet need has led clinical research on new treatment strategies focused on influencing the unique micro-environment of HPV+ OPC with for example immunotherapy. This article summarizes the current understanding regarding the optimal treatment of non-metastatic HPV+ OPC. Ongoing and published clinical trials regarding de-intensification strategies, immunotherapy and proton therapy are described focusing on the rationale and underlying evidence of these emerging treatment strategies. Nevertheless, until the results of the ongoing trials are known, the treatment of HPV+ OPC in clinical practice should remain identical to the treatment of HPV negative OPC.
Highlights
Oropharyngeal squamous cell carcinomas (OPC) are tumors located in the soft palate, the pharyngeal wall, the tonsils or the base of tongue, the latter two being the preferred location of Human Papillomavirus related (HPV+) oropharyngeal squamous cell carcinoma (OPC)
The optimal treatment approach for HPV+ OPC will be determined based on the results of several running trials
Sufficient follow up of all these studies is crucial in order to be confident that outcome is not compromised, since HPV+ disease shows a trend for later relapses than HPV– disease
Summary
Oropharyngeal squamous cell carcinomas (OPC) are tumors located in the soft palate, the pharyngeal wall, the tonsils or the base of tongue, the latter two being the preferred location of Human Papillomavirus related (HPV+) OPC. The De-ESCALaTE trial (NCT01874171) and TROG 12.01 trial (NCT01855451) compare the toxicity of both treatments, whereas the largest trial, the RTOG 1016 (NCT01302834), including around 1,000 patients, is currently the only randomized controlled trial with oncologic outcome as primary endpoint (Table 2) This treatment approach is promising, the efficacy of cetuximab in HPV+ OPC is controversial. Rosenthal et al conducted a retrospective subset analysis of the IMCL-9815 trial of Bonner et al focusing on the potential impact of p16 status (a surrogate marker of HPV positivity) on the outcome of 182 OPC patients [6, 21] They showed benefit for cetuximab on locoregional control and overall survival in both p16+ and p16– subgroup.
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