Abstract
Despite significant technical improvements in the management of patients with locoregionally-advanced head and neck cancers, too many patients fail to achieve durable remissions that ultimately translate into cures. Loco-regional recurrence and/or metastatic relapse after intensive local therapies remain the scourge of those who suffer from this disease, and the surgeons and physicians who treat them. Regrettably, until now, we have failed to develop effective adjuvant therapies that can be delivered after the completion of definitive loco-regional treatment in order to reduce the risk of disease relapse. In this chapter, approaches based on cytotoxic chemotherapy, targeted therapies directed against c-erbB/HER receptors and immune checkpoint inhibition will be discussed. Neither cytotoxic chemotherapy nor anti-HER-family targeted therapies have proven to be successful as adjuvant therapies for locoregionally-advanced head and neck cancers, but there is significant hope that anti-PD1/anti-PD-L1-targeted antibody therapies may deliver progress in this area for the first time.
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Keywords
- Adjuvant
- c-erbB
- Cytotoxic chemotherapy
- Epidermal growth factor receptor
- Head and neck cancer
- Immune checkpoint inhibition
- Immunotherapy
Introduction
Although surgery and radiotherapy are the main curative treatment modalities in patients with locoregionally-advanced squamous cell cancers of the head and neck (LA-SCCHN), their use as single modality therapies or combined as dual modality (surgery and adjuvant post-operative radiotherapy) treatment is associated with unacceptably poor outcomes for many patients. Consequently, the development of curative therapies for LA-SCCHN has seen an inexorable shift towards combinatorial approaches that include systemic treatments delivered alongside surgery and/or radiotherapy.
As is frequently the case in oncology, clinicians have used the lessons learned in treating patients in the context of relapsed and/or metastatic head and neck cancer to provide useful indicators towards therapeutic approaches that can be employed effectively in the locoregionally-advanced setting. Building on data demonstrating the benefit of systemic platin-based chemotherapy [1, 2] with or without epidermal growth factor receptor (EGFR) inhibition [3, 4] in patients with relapsed and/or metastatic head and neck cancer, clinicians have established a robust body of evidence to support the use of systemic agents in the context of treating LA-SCCHN. Thus, multimodality regimens in which radiotherapy is delivered with the addition of concomitant platin-based chemotherapy [5, 6] or a monoclonal antibody that targets EGFR [7, 8] have become standards-of-care in younger patients of good performance status. However, similar approaches involving the use of either chemotherapy or EGFR inhibition in the context of adjuvant therapy delivered after definitive or post-operative (chemo)radiotherapy have not, as yet, resulted in practice-changing outcomes.
In the case of immune checkpoint inhibitors (ICPI), there have also been attempts to extend the principle of applying that which is effective in the relapsed and/or metastatic setting to earlier time points within the patient pathway. ICPIs have been shown to be more effective than standard-of-care chemotherapy in both first- [9] and second-line [10,11,12,13] treatment of relapsed and/or metastatic head and neck cancer and have become new global gold-standard therapies. Importantly, in each of the practice-changing trials of ICPIs in head and neck cancer, patients have received prolonged dosing with immunotherapy and many have achieved durable and possibly permanent remissions. In many ways, the use of prolonged dosing regimens with ICPIs, even in patients who have achieved radiological complete remissions, can be seen as mimicking a course of adjuvant therapy. It is, therefore, no surprise that a number of clinical trials are currently addressing the question of using ICPIs in the adjuvant setting after the delivery of curative-intent treatment regimens, including studies involving adjuvant therapy after definitive chemoradiotherapy or surgery followed by post-operative chemoradiotherapy.
Therefore, in this chapter, we will discuss the potential role of adjuvant therapies in patients with LA-SCCHN. Data on the use of cytotoxic chemotherapy agents will be reviewed first in order to provide a context for more recent attempts to develop effective adjuvant approaches based on EGFR-targeted therapies and ICPIs.
Adjuvant Post-Operative Chemoradiotherapy Improves Outcomes in LA-SCCHN
Post-operative radiotherapy (PORT) is considered when the risk of recurrence of disease above the clavicles exceeds 20% (either at the mucosal site or in surgically-treated and -untreated nodal levels). Absolute indications for PORT include close (less than 5 mm) or involved (positive) margins at the primary tumour resection site, two or more involved cervical lymph nodes, extracapsular spread and invasion of the soft tissues of the neck. The presence of lymphovascular space invasion and perineurial invasion are relative indications for PORT that are considered in association with other factors [14].
The role of adjuvant post-operative chemoradiotherapy (POCRT), as opposed to PORT, was clarified in two seminal studies published in 2004 [15, 16] and summarised in Fig. 14.1. It is important to emphasise that, in both of these trials, the delivery of chemotherapy was restricted solely to the period of time during which the patient received adjuvant post-operative radiotherapy. In other words, there was no use of chemotherapy in a fashion that might be considered as true adjuvant therapy. The inclusion criteria for the RTOG 9501 [15] and EORTC 22931 [16] studies were slightly different, but the overall findings were remarkably similar. In the RTOG study, loco-regional control and disease-free survival were increased by the addition of concomitant cisplatin to PORT. There was a 10% improvement in 2-year loco-regional control (82% vs 72%) in favour of POCRT. In the EORTC study, 5-year progression-free and overall survival rates were increased by the addition of concomitant cisplatin to PORT.
The authors of those two studies subsequently amalgamated the datasets to derive consensus indications for POCRT [17]. They found that extracapsular spread in lymph node disease and the presence of microscopically involved resection margins were the only risk factors for which the impact of POCRT was significant in both trials. Therefore, these two factors have been widely adopted as absolute indications for POCRT across the globe. The combined analysis also suggested a trend in favour of POCRT in patients with stage III/IV disease, those with perineurial invasion, lymphovascular space emboli or level IV and V lymph nodes in the case of oral cavity or oropharyngeal cancers. These factors have not been accepted widely as absolute indications for POCRT.
Adjuvant Chemotherapy Is Not Effective in LA-SCCHN
The Meta-Analysis of Chemotherapy on Head and Neck Cancer (MACH-NC) collaborative group was originally published in 2000 and represented a landmark study that fundamentally changed the standard-of-care treatment paradigms for patients with stage III/IV disease [5]. That meta-analysis addressed three specific issues: (i) the effect on survival outcomes of adding chemotherapy to locoregional treatment; (ii) the effect of different chemotherapy schedules; and (iii) the role of induction/neoadjuvant chemotherapy in laryngeal preservation. Data relating to the first two questions have provided clear guidance on the absence of a defined role for adjuvant cytotoxic chemotherapy in LA-SCCHN. Thus, although the meta-analysis, which included 63 trials involving 10,741 patients, demonstrated that survival following definitive local therapy was significantly improved with the addition of chemotherapy, neither induction nor adjuvant chemotherapy was seen to have had a significant effect on survival outcomes.
In view of the heterogeneity of the studies included in the original MACH-NC meta-analysis, a further study was conducted in which the group updated their results by including individual patient data from randomised trials that were conducted between 1994 and 2000 [6]. Data from a total of 87 randomised trials were available for the analyses. Because some trial arms were used more than once in the analysis, the total number of comparisons in the updated meta-analysis was 108 comprising data on 17,493 patients. The majority of new trial data were specifically related to the use of concomitant chemotherapy and resulted in the meta-analysis being able to draw much clearer conclusions about the value of this treatment approach. As with the previous analysis, there was a significant effect of the timing of chemotherapy with concomitant chemotherapy clearly offering the greatest benefit (hazard ratio 0.81 (95% CI 0.78–0.86). Once again, neither induction (hazard ratio 0.96 (95% CI 0.90–1.02) nor adjuvant (hazard ratio 1.06 (95% CI 0.95–1.18) chemotherapy was found to be better than locoregional therapy alone. As a consequence, there is broad agreement across the globe that adjuvant chemotherapy has no established role when delivered after definitive surgery, radiotherapy, or radical/post-operative chemoradiotherapy.
Epidermal Growth Factor Receptor-Targeted Therapies in LA-SCCHN
SCCHN very frequently show upregulated EGFR signalling. EGFR is a member of the c-erbB/HER family of transmembrane type I receptor tyrosine kinases, which comprises a total of four members (EGFR/c-erbB-1/HER1, c-erbB-2/neu/HER-2, c-erbB-3/HER-3, c-erbB-4/HER-4 [18, 19]). HER-family receptor proteins share a common structure, consisting of a glycosylated extracellular ligand-binding domain, a hydrophobic trans-membrane component and an intracellular domain with tyrosine kinase activity. When the specific (cognate) ligand binds to its ligand-binding domain on the extracellular component of a HER-family member, it causes receptor dimerization and activation of the kinase domain. This, in turn, mediates phosphorylation of target proteins, which triggers a cascade of intracellular secondary messengers that alter patterns of gene expression. In this way, binding of a protein on the cell surface can influence the cell’s behaviour. It is important to note that there is no ligand for the c-erbB2/HER2 receptor and that the c-erbB3/HER3 receptor has no kinase activity. Nonetheless, these receptors are able to participate in signalling by dimerizing with appropriate partners. For example, EGFR:c-erbB3 (HER1/HER3) and c-erbB-2:c-erbB-3 (HER2/HER3) heterodimers can exploit ligand binding to the HER3 component and kinase-mediated signalling from the EGFR or HER2 component of the partnership.
Normally, activation of HER-family receptors by their cognate ligands (growth factors) is very tightly controlled—through regulation of the expression of the receptor, the availability of the ligand and the ability of the cell to de-phosphorylate activated receptors. In this way, proliferation of normal tissues is carefully regulated to avoid unnecessary or unscheduled cell growth. In contrast, in SCCHN there is very frequently a state of independence from normal regulatory mechanisms that is driven through a number of different processes. These include: (i) manufacture and release of growth factors that stimulate HER-family receptors on the malignant cell (autocrine signalling) and on neighbouring malignant (and normal) cells (paracrine signalling); (ii) altering the number, structure or function of the surface growth factor receptors expressed on tumour cells; and (iii) by altering the signalling pathways downstream of the receptor. In contrast to other tumour types, in which EGFR gene amplification or mutation is common (e.g. lung adenocarcinoma), overexpression of the receptor, without gene amplification, is the dominant process whereby EGFR affects the pathobiology of SCCHN. The roles of HER2, HER3 and HER4 in SCCHN remain unclear. However, it is known that HER2/HER3 heterodimers are potent inducers of the PI3-kinase anti-apoptotic pathway [20] and this may be relevant to particular subsets of SCCHN, including human papillomavirus (HPV)-related disease37.
Irrespective of the fact that SCCHN rarely shows evidence of EGFR mutation, the evidence of single-agent responses to HER-family-targeted therapies strongly supports the notion that these tumours can be reliant on signalling through these pathways in order to maintain the malignant phenotype. This reliance on activation of an oncogenic driver has been called “oncogene addiction” [21] and is seen as a potential point of therapeutic attack against a range of tumour types. Therefore, HER-family receptors represent attractive therapeutic targets in SCCHN and two main classes of drugs, monoclonal antibodies (MAB) and small molecule tyrosine kinase inhibitors (smTKI), have been developed. MAB are large molecules directed against the extracellular domain of the receptor, while smTKI inhibit the intracellular kinase domain of the receptor.
Anti-EGFR Monoclonal Antibodies Are Not Used as Adjuvant Therapies for LA-SCCHN
Anti-EGFR-targeted monoclonal antibodies (cetuximab, zalutumumab, panitumumab, nimotuzumab) have been extensively tested in patients with relapsed and/or metastatic head and neck cancers. Cetuximab has been shown to improve the outcome of first-line palliative chemotherapy [3]. In the EXTREME study, 442 eligible patients with untreated recurrent and/or metastatic SCCHN received cisplatin or carboplatin plus 5-fluorouracil every 3 weeks for a maximum of 6 cycles. Cetuximab (400 mg/m2 loading dose, then 250 mg/m2 per week) was administered to 222 randomly selected patients. Patients in the cetuximab arm who showed stable disease or treatment response were planned to continue with maintenance cetuximab until disease progression or unacceptable toxicity. This study showed that the cetuximab/platinum/5-fluorouracil combination prolonged median overall survival from 7.4 months to 10.1 months (P = 0.04). There were also increases in the median progression-free survival time (3.3 to 5.6 months; P < 0.001) and the response rate (20% to 36%; P < 0.001) [3]. Consequently, the EXTREME regimen was adopted as a gold-standard treatment for relapsed/metastatic head and neck cancer. In contrast, neither panitumumab [22] nor zalutumumab [23] has been registered for the treatment of relapsed and/or metastatic head and neck cancer following negative phase III trials, although the data from those trials was strongly suggestive of activity of those agents. The use of nimotuzumab is largely restricted to India and there are very limited data relating to its use in recurrent and/or metastatic SCCHN [24].
Cetuximab has also been approved as part of a curative regimen for LA-SCCHN. In a phase III study of 424 subjects with locally or regionally advanced SCCHN, locoregional control (median 24.4 vs. 14.9 months; hazard ratio: 0.68; P = 0.005) and overall survival (median 49.0 vs. 29.3 months; hazard ratio: 0.74; P = 0.03) were significantly prolonged in patients receiving radiotherapy and cetuximab compared to those treated with radiotherapy alone [7, 8]. However, in this study, there was no continued, adjuvant use of cetuximab beyond the completion of radiotherapy. In addition, both zalutumumab and panitumumab have been tested in combination with radiation/chemoradiation, again without any attempt to use them in an adjuvant phase beyond the completion of definitive treatment. Neither of these agents improved outcomes when compared to the standard therapy arms and they have not been approved in the context of LA-SCCHN [25,26,27]. Nimotuzumab is widely used with chemoradiotherapy in India, following the publication of a positive randomised phase III trial. However, once again, there was no use of nimotuzumab following completion of definitive loco-regional therapy [28] and, therefore, there is no evidential basis on which to deliver this therapy in an adjuvant setting.
Small Tyrosine Kinase Inhibitors Are Not Effective Adjuvant Therapies in LA-SCCHN
A number of agents have been developed to target HER-family members across a variety of different tumour types. In the context of head and neck cancer, gefitinib and erlotinib (EGFR/HER1 inhibitors) [29,30,31], lapatinib (HER1/HER2 inhibitor) [32, 33] and afatinib (pan-HER inhibitor) [34] have been most extensively investigated. Studies have included assessments of agents in the palliative setting for relapsed and/or metastatic disease. Despite the fact that these agents demonstrate single-agent activity in phase I/II trials, randomised studies have failed to demonstrate clinically meaningful survival advantage relative to standard-of-care treatment and none of them is in routine clinical use for patients with relapsed and/or metastatic disease. Specifically, a randomised phase III study was conducted to compare survival in 486 patients with recurrent or metastatic SCCHN treated with gefitinib 250 or 500 mg/day or standard-of-care single-agent weekly methotrexate [35]. Neither of the gefitinib doses improved overall survival compared with methotrexate (hazard ratios 1.22 (95% CI 0.95–1.57 and 1.12 (95% CI, 0.87–1.43), respectively. The median overall survivals were 5.6, 6.0, and 6.7 months for gefitinib 250 mg/day, gefitinib 500 mg/day, and intravenous methotrexate, respectively. Afatinib has been assessed in the phase III LUX head and neck-1 study in patients receiving second-line therapy for relapsed/metastatic SCCHN [36]. A total of 583 patients were treated with afatinib (322 patients) or methotrexate ((161 patients). Afatinib significantly increased median progression-free survival (2.6 versus 1.7 months, p = 0.03) but did not improve median overall survival (6.8 versus 6.0 months) relative to methotrexate. In an integrated analysis of quality of life, afatinib showed a delay in deterioration of global health status, pain and swallowing problems (all p ≤ 0.03) but such data were of insufficient weight to lead to regulatory approval of this therapy.
In the context of adjuvant maintenance therapy using HER-family-targeted therapies, there have been significant attempts to develop lapatinib and afatinib. A randomised phase III study of lapatinib administered concomitantly with chemoradiotherapy and as maintenance monotherapy in patients with high-risk surgically-treated SCCHN has been reported [37, 38]. Patients with resected stage II-IVA SCCHN, with a surgical margin ≤5 mm and/or extracapsular extension in metastatic cervical nodal disease were randomized to chemoradiotherapy (66 Gy total dose and 100 mg/m2 cisplatin administered on days 1, 22 and 43) plus placebo or lapatinib (1500 mg/day) prior to and during chemoradiotherapy, followed by 12 months of maintenance monotherapy (either placebo or lapatinib). Six hundred and eighty-eight patients were enrolled; 346 received lapatinib and 342 received placebo. With a median follow-up of 35.3 months, the study was terminated early due to the apparent plateauing of disease-free survival events. Median disease-free survivals were 53.6 months and “not reached” for lapatinib and placebo, respectively; hazard ratio 1.10 (95% CI 0.85–1.43). No significant differences in disease-free survival by HPV status or overall survival were observed between the two treatment arms. Similar numbers of patients in both treatment arms experienced adverse events, with more patients in the lapatinib arm experiencing serious events (48% vs 40%). This study demonstrated that adding lapatinib to chemoradiotherapy and its use as long-term adjuvant therapy was safe, but did not offer any efficacy benefits compared with placebo in patients with surgically-treated high-risk SCCHN.
In the LUX head and neck-2 study, 617 patients were randomised to treatment (411 to afatinib and 206 to placebo) in a true adjuvant context [39, 40]. Eligible patients had histologically or cytologically confirmed LA HNSCC (Stage III, IVa or IVb SCC of the oral cavity, oropharynx or hypopharynx, or Stage IVa or IVb SCC of the larynx). Since HPV status was not determined for eligibility, unfavourable risk was defined as non-oropharynx primary site or oropharynx cancer in heavy smokers (>10 pack years). Patients were required to have unresected disease prior to chemoradiotherapy. Concomitant definitive chemoradiotherapy had to have been completed no longer than 24 weeks prior to randomisation, comprising radiotherapy with curative intent to a minimum dose of 66 Gy in 33 fractions, and cisplatin or carboplatin. No evidence of disease was required on clinical and radiographic examinations (defined as no residual tumour after chemoradiotherapy (with or without R0 resection at the primary site or neck dissection). A pre-planned futility analysis, showed the study was unlikely to demonstrate a significant advantage with afatinib and the trial was halted early on the recommendation of the independent data-monitoring committee. Patients were discontinued from treatment and follow-up for disease recurrence and survival was stopped. The percentage of patients taking at least 80% of the planned study medication was lower for the afatinib group (85.3%) than the placebo group (98.5%), almost certainly reflecting the appreciable toxicity associated with chronic administration of this pan-HER-targeted oral medication. Median disease-free survival (DFS) by investigator review was 43.4 months (95% CI 37.4–not estimable) with afatinib versus “not estimable” (95% CI 40.1–not estimable) with placebo (HR 1.13, 95% CI 0.81–1.57; stratified log-rank test p = 0.48). The DFS rate at 2 years was evaluated using the Kaplan-Meier method; the probability of being disease-free at 2 years was 67.2% in the afatinib group and 73.5% in the placebo group (estimated difference: −6.3%, 95% CI -15.0–2.5; p = 0.16). At the time of data cut-off for the futility analysis, overall survival data were immature. The effect of afatinib versus placebo on DFS was explored in pre-planned subgroup analyses based on stratification factors, biomarker status, demographics, baseline disease characteristics and prior anti-cancer chemotherapy. These subgroup analyses were generally consistent with the primary analysis and showed no clear trend of benefit in any subgroup, although there was a slight benefit for afatinib patients with nodal status N2b–N3 (HR 0.82, 95% CI 0.55–1.21).
Immune Checkpoint Inhibitors as Adjuvant Therapies in LA-SCCHN
In recent years, immunotherapy has emerged as a new pillar in the treatment of many solid cancers [41]. This renewed interest in immunotherapy has been underscored by huge advances in our understanding of the fundamental biological principles that guide the activity of the immune system. In particular, specific immune checkpoints have been discovered that are integral components of normal immune responses. In normal health, these checkpoints function as negative regulators or “brakes” on the normal immune response and prevent T cells from becoming chronically activated or aberrantly targeted against normal tissues. Many cancers exploit these inhibitory pathways in order to escape from immunosurveillance.
Proteins that are expressed on activated T cells, such as cytotoxic T-lymphocyte-associated protein-4 (CTLA-4) and programmed death-1 (PD-1), are key players that allow many cancers to evade anti-tumour immunity by interfering with the activation and effector phases of immune responses, respectively. In the context of relapsed and/or metastatic head and neck cancer, we have clear evidence that blockade of signalling through the PD-1 pathway (mediated by programmed death ligand-1 (PD-L1) expressed on the surface of cancer and other cells) can yield significant clinical responses. Indeed, we now have positive phase III trial data, initially in the second-line and, more recently, in the first-line setting, to show that anti-PD-1-targeted therapies are capable of significantly improving overall survival in patients with relapsed and/or metastatic head and neck cancers [9,10,11,12,13]. As with chemotherapy and HER-family-targeted therapies, such data have spurred on investigators to investigate the potential value of immune checkpoint inhibitors (ICPI) as adjuvant therapies for cancer.
A number of lines of evidence can be invoked to support the hypothesis that adjuvant ICPI therapy might be beneficial in patients treated for LA-SCCHN. First, there are data in patients with melanoma that demonstrate that the “baseline tumour size” is an independent, statistically significant predictor of overall survival in patients treated with anti-PD-1 ICPI [42]. In addition, phase III clinical trials have shown improvement in progression-free and overall survival endpoints for tumour types such as melanoma and lung cancer [43,44,45,46]. As a guide to the management of SCCHN, the data from the PACIFIC trial in lung cancer are most compelling because the patient population comprised those with locally-advanced, stage III non-small-cell lung cancer who had not progressed on chemoradiotherapy delivered with curative intent [45, 46]. Interestingly, patients were required to commence adjuvant anti-PD-L1 therapy (durvalumab) within 42 days of completion of chemoradiotherapy.
At the time of writing, there are at least 3 major trials that have either completed recruitment or are still ongoing that address the question of adjuvant/maintenance ICPI in locally-advanced head and neck cancer. The designs of these trials are summarised in Figs. 14.2, 14.3 and 14.4.
The Javelin Head and Neck 100 study was a randomized, double-blind, placebo-controlled, parallel-arm, superiority study of the anti-PD-L1 agent, avelumab, versus placebo. Patients with LA-SCCHN (oral cavity, oropharynx, larynx, or hypopharynx) who were eligible for definitive chemoradiotherapy were enrolled (details of patient groups are provided in Fig. 14.2). Patients were randomized to receive either avelumab or placebo plus standard-of-care chemoradiotherapy. Randomization was stratified by tumour stage (<T4 vs T4), nodal stage (N0/N1/2aN2b vs N2c/N3), and HPV status (positive vs negative). There were three treatment phases in the study: lead-in phase; treatment phase; and maintenance phase. The primary endpoint of Javelin Head and Neck 100 is the progression-free survival (PFS) per modified Response Evaluation Criteria in Solid Tumours (RECIST) version v1.1 by investigator assessment. Secondary endpoints include overall survival, pathologic complete response, neck dissection, locoregional failure, objective response, distant metastatic failure, and duration of response, per modified RECIST v1.1 by investigator assessment. In March 2020, the study sponsors accepted the recommendation of the independent Data Monitoring Committee to terminate the JAVELIN Head and Neck 100 trial, as the study is unlikely to show a statistically significant improvement in the primary endpoint of PFS based on a pre-planned interim analysis [47]. A detailed analysis of the study findings are likely to be available for examination by the scientific community in 2021.
KEYNOTE-412 (ClinicalTrials.gov, NCT03040999) has a similar design to Javelin Head and Neck 100 (Fig. 14.3). It is a randomized, double-blind, placebo-controlled, phase III study of pembrolizumab 200 mg or placebo every 3 weeks in combination with chemoradiotherapy and as maintenance/adjuvant therapy for a total of 17 doses over one year [48]. Study recruitment has now closed, but patients remain in follow-up as the data mature. Eligible patients were randomly assigned 1:1 to pembrolizumab or placebo with stratification according to radiotherapy regimen (accelerated versus standard fractionation), tumor site, p16 status (oropharynx—p16 positive vs oropharynx—p16 negative or larynx/hypopharynx/oral cavity cancer), and tumour stage (III vs IV, AJCC TNM Version 7). Treatment is continued until centrally confirmed disease progression, unacceptable toxicity, intercurrent illness that prevents further administration of treatment, investigator’s decision to withdraw the patient, non-adherence to treatment or trial procedures, administrative reasons requiring cessation of treatment, or the patient has received 17 administrations of pembrolizumab/placebo (approximately 1 year). The trial is split into three treatment phases. The first phase includes the pembrolizumab/placebo priming dose, followed by chemoradiotherapy in combination with two additional pembrolizumab/placebo doses given every 3 weeks (duration, 8 weeks). The second phase includes pembrolizumab/placebo maintenance/adjuvant dosing (14 doses over about a year) during post-treatment follow-up. The third phase includes post-treatment follow-up. The primary end point of the trial is event-free survival (EFS) using RECIST v1.1. EFS is defined as the time from the date of randomization to the date of first record of (1) progression per RECIST v1.1 by blinded independent central review ([a] locoregional progression or recurrence or [b] distant metastasis), (2) salvage surgery at the primary tumour site when invasive cancer is present, (3) neck dissection performed >20 weeks after completion of CRT when invasive cancer is present, or (4) death from any cause. The key secondary end point is overall survival, which is defined as the time from randomization to death from any cause. Other secondary end points include safety and patient-reported outcomes (PROs); PROs are assessed using the European Organisation for the Research and Treatment of Cancer Quality of Life Questionnaire (EORTC QLQ) core 30 items (C30) and head and neck module (H&N35) as well as the EuroQoL-5D (EQ-5D). Exploratory end points include potential predictive biomarkers and immune dynamics in the subgroup of patients with oropharyngeal p16-negative or larynx/hypopharynx/oral cavity HNSCC and the overall population.
The ImVoke-10 study (ClinicalTrials.gov NCT03452137) is a phase III, multicentre, randomized, double-blind, placebo-controlled trial of the anti-PD-L1 ICPI, atezolizumab, as adjuvant therapy following definitive local therapy for high-risk LA-SCCHN [49]. Its design is depicted in Fig. 14.4. Approximately 400 patients will be randomised between atezolizumab and placebo given in a truly adjuvant setting (Fig. 14.4). The co-primary endpoints are independent review facility assessed EFS (per RECIST v1.1) or death from any cause and overall survival.
Summary and Conclusions
Despite relatively poor outcomes for many patients who present with LA-SCCHN, we have, thus far, failed to develop effective adjuvant therapies to prevent loco-regional and/or metastatic relapse following definitive local therapy. Extensive effort has been exerted in attempting to develop adjuvant chemotherapy schedules, but to no avail. Similarly, attempts to exploit the concept of “oncogene addiction” by using adjuvant HER-family-targeted therapies have not been successful. There is no evidence that either small molecule inhibitors or monoclonal antibodies given in the adjuvant situation can favourably alter recurrence rates or survival outcomes. Currently, most effort is being channeled into studies that seek to evaluate the potential role of ICPI as adjuvant therapies. Considerations around these trial designs are complex, since both the Javelin Head and Neck 100 and the KEYNOTE-412 studies involve a combination of concomitant (with chemoradiotherapy) and adjuvant ICPI therapy. Neither study is designed to allow separate evaluation of the role of the concomitant versus the adjuvant components of the therapeutic package. Nevertheless, given the remarkable results in the context of relapsed and/or metastatic head and neck cancer, there is cause for optimism that we may be able to improve outcomes for our patients.
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Harrington, K.J. (2021). Is there a Role for Adjuvant Targeted and Immunotherapies in Patients with Locoregionally-Advanced Head and Neck Cancer?. In: Vermorken, J.B., Budach, V., Leemans, C.R., Machiels, JP., Nicolai, P., O’Sullivan, B. (eds) Critical Issues in Head and Neck Oncology. Springer, Cham. https://doi.org/10.1007/978-3-030-63234-2_14
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