Time to Surgery and Survival in Head and Neck Cancer.

BACKGROUND: The COVID-19 pandemic has required triage and delays in surgical care throughout the world. The impact of these surgical delays on survival for patients with head and neck squamous cell carcinoma (HNSCC) remains unknown.
METHODS: A retrospective cohort study of 37 730 patients in the National Cancer Database with HNSCC who underwent primary surgical management from 2004 to 2016 was performed. Uni- and multivariate analyses were used to identify predictors of overall survival. Bootstrapping methods were used to identify optimal time-to-surgery (TTS) thresholds at which overall survival differences were greatest. Cox proportional hazard models with or without restricted cubic splines were used to determine the association between TTS and survival.
RESULTS: The study identified TTS as an independent predictor of overall survival (OS). Bootstrapping the data to dichotomize the cohort identified the largest rise in hazard ratio (HR) at day 67, which was used as the optimal TTS cut-point in survival analysis. The patients who underwent surgical treatment longer than 67 days after diagnosis had a significantly increased risk of death (HR, 1.189; 95% confidence interval [CI], 1.122-1.261; P < 0.0001). For every 30-day delay in TTS, the hazard of death increased by 4.6%. Subsite analysis showed that the oropharynx subsite was most affected by surgical delays, followed by the oral cavity.
CONCLUSIONS: Increasing TTS is an independent predictor of survival for patients with HNSCC and should be performed within 67 days after diagnosis to achieve optimal survival outcomes.

The novel 2019 coronavirus disease (COVID-19) pandemic has led to delays in the surgical care of patients with head and neck squamous cell carcinoma (HNSCC) Accordingly, the current climate has raised urgent questions for patients as well as the head and neck oncologic community. How long can surgery be delayed, and at what time point does further delay have a significant impact on survival outcomes?

Previous study has shown that the time from diagnosis to initiation of definitive treatment for HNSCC is increasing, adversely affecting survival.1–5 Treatment package times, which cover the time from diagnosis to completion of treatment including adjuvant therapy, also have correlated with survival.5–10 Although these data collectively show the deleterious effect of delayed treatment on patients, both surgically and nonsurgically, current events have demonstrated a need to study the specific impact of surgical delay on HNSCC survival so that surgeons can appropriately schedule surgeries while balancing risks and vital resources.

From a large national database of patients with HNSCC, this study included only patients treated with primary surgery. The study aimed to analyze the impact of increasing time to surgery (TTS) on overall survival (OS) in HNSCC.

Materials and methods

Data Source

The National Cancer Database (NCDB) is a hospital-based cancer registry database that collects data from more than 1500 Commission on Cancer-accredited facilities. The NCDB database captures more than 80% of newly diagnosed head and neck cancers each year in the United States.11 We reviewed the NCDB for patients from 2004 to 2016 with primary oral cavity, oropharynx, larynx, or hypopharynx squamous cell carcinoma (SCC) who received definitive primary surgical treatment and investigated the effect of TTS on OS. The Ohio State University College of Medicine Institutional Review Board deemed this study exempt from review.

Inclusion and Exclusion Criteria

A retrospective review of the NCDB was performed for adults with previously untreated SCC of the oral cavity, oropharynx, larynx, or hypopharynx diagnosed between 2004 and 2016 (Fig. S1). Squamous cell carcinoma was identified with International Classification of Diseases for Oncology, third edition, histologic codes 8052, 8070–8076, 8078, 8083, and 8084. Only entries with subsite information were included, and the subsites were grouped by International Classification of Diseases for Oncology-3 codes.

The oral cavity primary site codes included C02.2, C02.3, C03.0, C03.1, C03.9, C04.0, C04.1, C04.8, C04.9, C05.0, C06.0, C06.1, and C06.2.12 The oropharynx primary site codes included C01.9, C02.4, C05.1, C05.2, C09.0, C09.1, C09.8, C09.9, C10.2, C10.3, and C10.9.13 The hypopharynx primary site codes included C12.9, C13.0, C13.1, C13.2, C13.8, and C13.9. The larynx primary site codes included C10.1, C32.1, C32.0, C32.2, C32.8 and C32.9. In the subset analysis of the oropharynx, patients with documented high-risk human papilloma virus (HPV), including HPV-16, HPV-18, and high-risk HPV not otherwise specified [NOS]), were considered positive for HPV.

Tumors involving the lip were excluded due to the risk of misclassification from skin cancers. Subsite codes including tongue NOS (C02.9), overlapping tongue lesion (C02.8), border of tongue (C02.1), and overlapping lesion of the mouth (C06.8) were excluded because these may represent either oral cavity or oropharyngeal subsites, and subsite analysis was an important covariate in this study.

Defining Definitive Primary Surgery in the NCDB

We sought to further filter the aforementioned cohort to ensure that patients included in this study underwent definitive primary surgery.13,14 Patients who had undergone preoperative chemotherapy, radiation therapy, or both were excluded. To ensure that patients received definitive surgery, the primary-site surgical codes from the Surveillance, Epidemiology, and End Results (SEER) Program Code Manual (3rd edition, revision 1) then were selected for each subsite that were unlikely to denote diagnostic biopsies.15 The codes for oral cavity are 30, 40, 41, 42, and 43, and the codes for the oropharynx are 30, 31, 32, 40, 41, 42, 43, 50, 51, and 52. Due to concerns that a proportion of patients classified as 30 or 31 did not receive definitive surgery, patients were included only if they also had more than 10 lymph nodes examined during surgery.13 The larynx codes were 30, 31, 32, 33, 40, 41, 42, 50 and 80. The hypopharynx codes were 32, 40, 41, 42, 43, 50, 51, and 52. The patients who had multiple primary cancers or distant metastatic disease treated with palliative intent were excluded (Fig. S1).

Variables

The covariates for the survival analyses were age, TTS, sex, race, insurance, urban residence, facility type, Charlson-Deyo score, income, education level, surgical margin status, pathologic stage, adjuvant treatment, and primary site. The TTS is defined as the number of days between the date of diagnosis, which is the first date the cancer is either clinically described in the medical record or histologically confirmed, and the date of the most definitive surgical procedure performed on the primary site. The patients with an interval of 0 days from diagnosis to definitive surgery were excluded due to accuracy concerns.2 Intervals longer than 180 days also were excluded from the analysis due to concerns of bias if these patients did not receive up-to-date imaging to rule out distant metastases.

Statistical Methods

Descriptive statistics were used to characterize the overall study population using median and interquartile range for continuous variables or frequencies and proportions for categorical variables. The primary outcome of this study was OS, determined from the date of definitive surgery to death or last follow-up visit.

Univariate analysis was used to identify potential predictors for death. Variables with a p value lower than 0.10 were entered into a multivariable model. Variables were removed sequentially from the multivariable model using the backward selection method, based upon p value. Cox proportional hazard models with or without restricted cubic splines were used to determine the association between TTS and survival, with control for the significant predictors from backward selection. An optimal threshold for TTS was determined by taking 100 bootstrap samples of the data and calculating adjusted hazard ratios (HRs) for each cut-point of TTS between 50 and 90 days. Locally estimated scatterplot smoothing was used to visualize the overall trend in TTS thresholds compared with adjusted HRs. Adjusted survival curves were plotted by optimal TTS thresholds. Interactions of TTS with stage, surgical margins, and tumor subsite were tested, and significant interactions were visualized using lattice plots. All p values lower than 0.05 were considered statistically significant. To plot restricted cubic splines, R statistical software (version 3.6.0) (R Foundation for Statistical Computing, Vienna, Austria) was used, and SAS (9.4) (Cary, NC) was used for the remainder of the analysis.

Results

Baseline Population Demographics

Baseline demographics are shown in Table 1. The median TTS in the United States for HNSCC from 2004 to 2016 was 33 days (IQR, 21– 49 days). The TTS was 30 days for 45% of the patients, 30 to 60 days for 41% of the patients,, and longer than 60 days for 14% of the patients. The most frequent subsite was the oral cavity (49%), followed by the oropharynx (28%), larynx (20%), and hypopharynx (2%).

Table 1

Baseline characteristics of patients with head and neck squamous cell carcinoma treated with primary surgery (n = 37 730)

Characteristic	N (%)
Age at diagnosis
Median (IQR)	60 (53–68)
TTS (days)
Median (IQR)	33 (21–49)
1–30	16 957 (45)
30–60	15 348 (41)
60–90	3881 (10)
91+	1544 (4)
Great circle distance
Median (IQR)	18.1 (7.1–47.9)
Sex
Male	26 833 (71)
Female	10 897 (29)
Race (n = 37 311)
White	32 978 (88)
Black	3140 (8)
Other	1193 (3)
Median household income (n = 37 082)
<$40 227	7539 (20)
$40 227–50 353	9010 (24)
$50 354–63 332	8616 (23)
≥$63 333	11 917 (32)
Percent with no high school degree (n = 37 186)
≥17.6	7943 (21)
10.9–17.5	10 210 (27)
6.3–10.8	10 456 (28)
<6.3	8577 (23)
Insurance status (n = 36 570)
Not insured	2042 (6)
Private insurance	16 464 (45)
Public insurance	18 064 (49)
Urban status (n = 36 853)
Nonmetropolitan	7218 (20)
Metropolitan	29 635 (80)
Facility type (n = 36 651)
Community cancer program	1491 (4)
Comprehensive community cancer program	8668 (24)
Academic/research program	23 110 (63)
Integrated network cancer program	3382 (9)
Charlson-Deyo score
0	28 028 (74)
1	7297 (19)
2	1746 (5)
3+	659 (2)
Surgical margin status (n = 35 902)
Negative	30 244 (84)
Positive	5658 (16)
TNM pathologic stage (n = 32 394)
1	5112 (16)
2	3677 (11)
3	5183 (16)
4	18 422 (57)
Adjuvant treatment
No adjuvant treatment	16 451 (44)
Adjuvant radiation	9860 (26)
Adjuvant chemoradiation	11 419 (30)
Primary site
Oral cavity	18 672 (49)
Oropharynx	10 697 (28)
Larynx	7641 (20)
Hypopharynx	720 (2)

IQR interquartile range, TTS time to surgery; TNM tumor-node-metastasis

Increasing TTS and Survival

An adjusted cubic spline was used to assess the relationship between TTS and survival given that we did not want to assume it was a simple linear association (Fig. 1a). This showed that the HR for death was lowest near day 24, with a gradual rise in the HR of death after day 40 and beyond, even when control was used for pathologic stage, surgical margins, primary site, adjuvant treatment, age, sex, race, income, insurance status, and Charlson-Deyo score. Bootstrapping the data determined an optimal threshold for dichotomizing TTS based on an OS of 67 days (Fig. 2a) . Adjusted OS is demonstrated in Fig. 2b, showing that a TTS longer than 67 days independently predicted a shorter OS than surgery performed within 67 days after diagnosis (HR, 1.189; 95% CI, 1.122–1.261).

Fig. 1

Relationship of time to surgery and hazard ratio (HR) of death. a Adjusted restricted cubic spline shows that the HR for the overall cohort was lowest on day 24, with the HR steadily increasing with time after day 40. Cubic splines for the oral cavity, oropharynx, and larynx/hypopharynx subsites are shown in b, c, and d, respectively

Fig. 2

Cohort validation and survival analysis. a The threshold for time to surgery (TTS) was determined by 100 bootstrap samples of the data and calculation of adjusted hazard ratios (HRs) for each cut-point of TTS between 50 and 90 days. Locally estimated scatterplot smoothing shows the overall trend in TTS thresholds versus adjusted HRs indicating a peak at 67 days. b Adjusted overall survival showing that patients undergoing surgery longer than 67 days after diagnosis have a poorer overall survival than those undergoing surgery within 67 days after diagnosis (HR, 1.189; 95% confidence interval [CI], 1.122–1.261; p < 0.0001)

The uni- and multivariate analyses are shown in Table 2. In the multivariable analysis, longer TTS was significantly associated with worse OS even after control for age, sex, race, income level, insurance, distance to the hospital, Charlson-Deyo score, pathologic stage, surgical margins, adjuvant treatment, and primary site. For each increase in TTS by 30 days, the hazard of death increased by 4.6% (eTable S1).

Table 2

Uni- and multivariate analysis of factors associated with overall survival

	Univariate analysis			Multivariate analysis
		95% CI			95% CI
Characteristic	HR	Lower	Upper	HR	Lower	Upper
Age	1.033	1.032	1.035	1.022	1.02	1.024
Great circle distance per 10 miles	0.999	0.997	1.00	0.998	0.996	1.00
Sex
Male	Ref	–	–	Ref	–	–
Female	1.037	1.00	1.077	0.873	0.836	0.912
Race
White	Ref	–	–	Ref	–	–
Black	1.44	1.363	1.521	1.06	0.994	1.131
Other	0.965	0.869	1.07	0.9	0.801	1.011
Median household income
<$40 227	1.59	1.516	1.669	1.196	1.130	1.266
$40 227–50 353	1.412	1.347	1.48	1.157	1.097	1.220
$50 354–63 332	1.264	1.204	1.327	1.128	1.068	1.191
≥$63 333	Ref	–	–	Ref	–	–
Percent with no high school degree
≥17.6	1.557	1.478	1.641	–	–	–
10.9–17.5	1.367	1.3	1.438	–	–	–
6.3-10.8	1.235	1.174	1.3	–	–	–
<6.3	Ref	–	–	–	–	–
Insurance
Not insured	0.781	0.726	0.84	0.981	0.903	1.065
Private insurance	0.429	0.413	0.445	0.708	0.675	0.743
Public insurance	Ref			Ref
Urban status
Nonmetropolitan	Ref	–	–	–	–	–
Metropolitan	0.897	0.86	0.935	–	–	–
Facility type
Community	Ref	–	–	–	–	–
Comprehensive Community	0.905	0.83	0.988	–	–	–
Academic/research	0.925	0.851	1.006	–	–	–
I ntegrated network	0.922	0.836	1.018	–	–	–
Charlson-Deyo score
0	Ref	–	–	Ref	–	–
1	1.498	1.439	1.56	1.2135	1.161	1.272
2	1.953	1.824	2.092	1.485	1.375	1.603
3+	2.311	2.084	2.563	1.674	1.492	1.878
Surgical margins
Negative	Ref	–	–	Ref	–	–
Positive	1.39	1.33	1.452	1.414	1.346	1.486
TNM pathologic stage
1	Ref	–	–	Ref	–	–
2	1.432	1.317	1.557	1.469	1.345	1.604
3	1.614	1.496	1.741	2.148	1.977	2.333
4	2.388	2.243	2.543	3.15	2.929	3.388
Adjuvant treatment
no adjuvant treatment	Ref	–	–	Ref	–	–
Adjuvant radiation	1.058	1.014	1.103	0.776	0.738	0.816
Adjuvant chemoradiation	1.037	0.996	1.079	0.9	0.854	0.949
Primary sites
Oral cavity	Ref	–	–	Ref	–	–
Oropharynx	0.406	0.386	0.427	0.368	0.347	0.39
Larynx	1.128	1.084	1.174	0.854	0.814	0.896
Hypopharynx	1.834	1.667	2.018	1.201	1.08	1.336
TTS (days)
1-67	Ref	Ref	–	Ref	–	–
67+	1.371	1.302	1.444	1.189	1.122	1.261

HR hazard ratio, CI confidence interval, TNM tumor-node-metastasis, TTS time to surgery

Interaction of TTS With Stage, Charlson-Deyo Score, Surgical Margins, and Tumor Subsite

Interaction testing was performed to assess mortality risk according to TTS by overall stage group, Charlson-Deyo score, surgical margins, and tumor subsite. No significant interactions were found between TTS and American Joint Committee on Cancer (AJCC) stage (p = 0.3870) or between TTS and Charlson-Deyo score (p = 0.2694). However, a significant interaction between TTS and tumor subsite was identified (p ≤ 0.0001) as well as surgical margin status (p = 0.0076). Adjusted restricted cubic spline analysis by tumor subsite was performed, and the results are presented in Fig. 1a–d.

The association of TTS with mortality was observed at the earliest time point in the oropharynx subsite, followed closely by the oral cavity. A relatively later time point of association between TTS and survival was observed in the larynx/hypopharynx subsite (Fig. 1d). Within the oropharynx subset, we also performed an analysis, stratifying by HPV-positive and HPV-negative tumors, which showed no interaction between TTS and survival (p = 0.93).

The interaction between tumor subsite and TTS was further explored by categorizing TTS into 0 to 30 days, 31 to 60 days, 61 to 90 days, and longer than 90 days. Hazard ratios stratified by tumor subsite and TTS for unadjusted tumor stage and surgical margin status, partial adjustment for these factors (model M1), and full adjustment for all significant covariates (model M2) are shown in Fig. 3. Unadjusted HRs for TTS categories relative to the baseline category (0–30 days) were significant for both oral cavity and oropharynx subsites, but not the larynx/hypopharynx. After adjustment for tumor stage and surgical margin status, HRs for TTS in oral cavity cancers were reduced by approximately half but remained significant for 61 to 90 days (HR, 1.18; 95% CI, 1.09–1.28) and longer than 90 days (HR, 1.19; 95% CI, 1.07–1.34) compared with 0 to 30 days. In the oral cavity, HRs were further reduced for TTS after adjustment for all additional significant covariates (61–90 vs 0–30 days: HR, 1.09; 95% CI, 1.00–1.18; > 90 vs 0–30 days: HR, 1.10; 95% CI, 0.98–1.23). Conversely, the HRs for TTS in the oropharynx were relatively unchanged even in the fully adjusted model (31–60 vs 0–30 days: HR, 1.29; 95% CI, 1.14–1.46; 61–90 vs 0-30 days: HR, 1.47; 95% CI, 1.21–1.79; > 90 days vs 0–30 days: HR, 1.98; 95% CI, 1.44–2.73).

Fig. 3

Relationship of time to surgery (TTS) and hazard ratio of death by tumor subsite. Hazard ratio is shown by tumor subsite in the unadjusted, adjusted M1 (partially adjusted for surgical margins and tumor stage only), and adjusted M2 (fully adjusted) models. The oropharynx subsite showed greater mortality when surgery was performed beyond 30 days, whereas the oral cavity subsite showed greater mortality when surgery was performed beyond 60 days. Control for surgical margins and tumor stage in the oral cavity subsite caused a 50% reduction in hazard ratios for TTS in the partially adjusted model

Discussion

In the United States, TTI in HNSCC, including surgical and nonsurgical methods, is on the rise and associated with concurrent chemoradiation treatment, treatment at academic facilities, advanced-stage disease, and transitions in treatment.1 Murphy et al.2 found that an increase in TTI was an independent predictor of survival, and that a threshold of TTI longer than 46 to 52 days introduced the increased risk of death, which was most detrimental at a TTI longer than 67 days.

Important differences exist between the current study and the paper published by Murphy et al.2 The cohort described by Murphy et al.2 was composed of patients receiving both nonsurgical (53%) and primary surgical (44%) treatment with or without adjuvant radiation or chemoradiation therapy, and 2.5% of their cohort received adjuvant chemotherapy, preoperative radiation therapy, preoperative CRT, or preoperative chemotherapy.2

Additional differences in the study populations exist, with the study by Murphy et al.2 composed mostly of laryngeal cancers (42%), followed by oral cavity (29%), oropharynx (22%), and hypopharynx (7%) cancers, likely as a result of including surgical and nonsurgical treatment methods.2 The current study was composed mostly of oral cavity cancers (49%), followed by oropharynx (28%), larynx (20%), and hypopharynx (2%) cancers. Murphy et al.2 performed a subset analysis of the patients in their cohort treated with surgery alone, which showed an increased risk of death in delays longer than 60 days.2 Despite differences in study populations, our findings also show a significant association with surgical delay and increased mortality, with the largest increase in HR at day 67.

Ho et al. 5 investigated the impact of radiation duration, radiation delays, and surgical delays on OS for patients undergoing primary surgery and adjuvant radiation or chemoradiation treatment. The findings showed that prolonged radiation intervals and time to radiation were associated with overall mortality, whereas surgical delays did not increase the risk of mortality.5 Because the goal was collective investigation of surgical delays, radiation delays, and radiation duration and their impact on survival, the study included only patients receiving surgery and adjuvant therapy.5 Patients who received surgery alone were excluded, which may have resulted in selection of a different cohort than the current study, which included all patients undergoing primary surgical treatment with or without adjuvant treatment. Our cohort was comprised of 16 451 patients (44%) treated with surgery alone. This study population was selected to investigate the impact of TTS on OS for external validity purposes because it is often difficult to discern preoperatively whether adjuvant therapy will be indicated.

Xiao et al.4 showed that surgical delays are associated with clinical-to-pathologic upstaging. These authors also showed that compared with a TTS of 1 to 6 days, increasing TTS significantly predicts T upstaging, even for intervals as short as 7 to 13 days.4 They also showed that patients experiencing tumor progression and clinical-to-pathologic upstaging had significantly poorer survival than the patients who did not experience tumor progression, solidifying tumor progression as a mechanism of mortality in the surgically delayed HNSCC population.4

After adjustment for all known confounders, our analysis showed that surgical delays longer than 67 days independently predicted increased risk of death (HR, 1.189; 95% CI, 1.122–1.261). Delays beyond this time point resulted in poorer survival that cannot be accounted for solely by factors such as tumor stage, positive margin rates, medical comorbidities, and insurance status. Because the current study adjusted for patients by pathologic staging as determined at the time of surgery, the survival difference also is not explained by pathologic upstaging. When the analysis was performed with the TTS variable grouped in 30-day increments, with each increase in TTS by 30 days, the hazard of death increased by 4.6% (eTable S1).

Primary surgical treatment longer than 67 days after diagnosis increases the risk of mortality by 18.9%. Although the magnitude of the HR is relatively small, the strength of the findings exist in the ability of the treating team to modify the TTS covariate, compared with other tumor-intrinsic factors such as tumor stage, subsite, and HPV status.

When analyzed by subsite, the oropharynx showed the greatest association with increasing TTS, and this association did not vary by HPV status. These data suggest that oropharyngeal surgery wait times should be minimized when possible because wait times longer than 30 days showed a 29% increase in mortality relative to surgery performed within 30 days. Oral cavity cancers also showed a significant increase in mortality with surgical delays, although this was noted at a later time point, when surgery was delayed longer than 60 days. In contrast, the larynx/hypopharynx subsites showed the least association between OS and TTS (Fig. 1D), potentially due to protection from local tumor progression offered from the cartilaginous framework of the larynx.

To investigate the potential impact of increasing pathologic stage and rate of positive surgical margins with increasing TTS, we also created a partially adjusted model (Fig. 3, model M1) that adjusted only for stage and surgical margins. This showed a 50% reduction in HR in the oral cavity subsite compared with the unadjusted model at 61 days, suggesting that increasing pathologic stage and surgical margins are additional negative prognosticators associated with surgical delay in the oral cavity subsite that are not conveyed by the HR in the fully adjusted model. Conversely, the oropharynx subsite showed little reduction in the HR when control was used for stage and surgical margins, and thus delays in this cohort resulted in increased mortality that could not be explained by stage progression or increased positive margins.

One potential mechanism whereby increased TTS affected survival in our fully adjusted model was the potential for increased risk of distant metastasis for patients with longer TTS undetected at the time of diagnosis and surgery that became clinically apparent later in the treatment course. Additionally, with longer surgical delays, patients are potentially at greater risk of perineural invasion, lymphovascular invasion, and greater depth of invasion, all of which are not measured in this NCDB cohort.

Previous studies have shown an association between delayed postoperative radiation and increased mortality.6,7 Additionally, total treatment package time is associated with mortality, particularly with package lengths longer than 100 days.5,8,16 Treatment package time should be distinguished from TTS because treatment package time includes key variables out of surgeons’ control. These include dental and preoperative clearance, coordination/availability of medical oncology and radiation oncology appointments, delayed pathology results, and prolonged wound healing. Under normal circumstances, relatively fewer barriers are present with regard to TTS (e.g., timely surgical evaluation, performance of biopsies, operating room time, and availability), which remain more closely associated with surgeons’ purview.

In clinical practice, TTS often is balanced by the perioperative optimization process (i.e., adequate nutrition, tobacco and alcohol cessation, medical clearance, imaging), which is critical for patient treatment. Patients with greater comorbidities are likely at risk for greater surgical delay, and our analysis showed significant differences in TTS among Charlson-Deyo score categories (p < 0.0001). As a result, we controlled for Charlson-Deyo scores in our multivariable model and also tested the interaction between TTS and Charlson-Deyo scores in the survival model, which was not significant (p = 0.2694), suggesting that the association between TTS and OS did not differ significantly across Charlson-Deyo score categories.

These results raise an important question: Should TTS be implemented as an institutional quality metric? Although it has been shown that high-volume centers offer specialized care with better outcomes than low-volume institutions, they also are potentially associated with longer wait times.2,17–21 Through institutional TTS tracking initiatives, it may be possible to describe more clearly the individual components that result in prolonged TTS and serve better to inform future quality improvement projects. Although TTS has been considered as a quality measure at other sites, it has yet to be considered in HNSCC, perhaps partly due to a lack of clear data to support such a measure.22 Although establishing TTS as a quality metric at this time is not a priority, these and other data suggest that TTS should be considered as a quality metric in the future.

The current study had important limitations. Due to the multidisciplinary nature of HNSCC management, TTS is relevant only for patients managed with primary surgery. Although challenging to achieve in the NCDB, we placed increased importance on isolating a primary surgical cohort as outlined in the Methods section. Despite every effort to adjust for numerous variables included in the database, unmeasured confounders still could exist as variables such as tobacco and alcohol exposure that are not recorded in the NCDB. More data are needed because the NCDB does not record disease-free or disease-specific survival. Because the NCDB records the date of diagnosis as either the first day that the cancer is mentioned in the record or the date of histologic diagnosis, variability between patients exists. Additionally, the authors recognize that significant heterogeneity exists among mucosal HNSCCs, and although understanding tumor growth could assist in triaging of surgical cases, these factors are difficult to discern at the time of initial evaluation. Biomarkers or other predictors of tumor growth rates could potentially further define the urgency for timely surgery and individualized wait times. A prospective trial designed to randomize patients receiving surgical treatment to differing wait times and TTS is neither ethical nor feasible. Therefore, we believe this analysis of the NCDB provides the most timely and robust data available.

Conclusions

Increasing TTS independently predicts worse survival for patients with HNSCC. The patients in this study who had TTS longer than 67 days were independently predicted to experience worse overall survival than the patients with TTS of 67 days or less. Although surgical delays are inevitable during the COVID-19 pandemic, all reasonable efforts should be made to expedite primary surgery for HNSCC, especially in the oropharynx and oral cavity subsites.

Below is the link to the electronic supplementary material.

Supplementary material 1 (DOCX 252 kb)