1. Introduction

Administration of preoperative radiotherapy, either short-course (scRT) or long-course, has been important in decreasing local recurrence rates after rectal cancer surgery [1,2,3,4,5]. In locally advanced rectal cancer (LARC), the addition of chemotherapy to long-course radiotherapy (CRT) further decreases local recurrence rates, whereas the impact on overall survival (OS), except possibly in the most advanced (ugly) cases, is unclear [6,7,8]. An impact on distant metastasis-free survival rates has only been seen when preoperative chemotherapy (CTX) is added to scRT/CRT, i.e., total neoadjuvant therapy (TNT) [9,10].

The tumour response to neoadjuvant treatment is highly heterogenous, ranging from complete shrinkage of the tumour to lack of effect and, occasionally, to progression. In approximately 10–28% of patients, neoadjuvant treatment results in the disappearance of the rectal tumour with no signs of residual tumour on MRI, proctoscopy, and digital examination (clinical complete response, cCR) or no residual viable cancer cells in the surgical specimen and pathologic complete response (pCR, also denoted ypCR) [9,10,11]. Patients who achieve pCR exhibit significantly more favourable oncological outcomes with higher 5-year disease-free survival rates (DFS, 83% if pCR versus 66% if non-pCR) and OS rates (88% with pCR versus 76% non-pCR) [12,13]. The achievement of a complete remission provides the possibility for organ-preserving surgery or a non-operative, watch-and-wait (W&W) approach. Research efforts have been directed toward identification of clinical and other parameters that could help predict pCR after preoperative treatment [14,15,16,17,18,19]. However, several unclear issues, particularly related to the importance of clinical T-stage (cT-stage), tumour length, presence of extramural vascular invasion (cEMVI+), mesorectal fascia (cMRF+) involvement, and clinical laboratory values need to be clarified [14,15,16,17,18,19].

The primary aim of this study was to identify clinical and imaging factors that can be used to predict pCR (and would thus also be applicable to cCR with the possibility of a W&W strategy), by combining data from two population-based Swedish cohorts, and comparing the three most commonly used schedules, scRT, CRT, or scRT/CRT + CTX; all with a ≥4-week interval to surgery. A secondary aim was to explore if a model based on clinical factors predicting pCR could be built.

2. Materials and Methods

Our study consisted of two independent population-based retrospectively collected cohorts from Uppsala-Dalarna (Cohort A) and Stockholm (Cohort B). All patients living in these regions at the time of diagnosis constituted the study base and were included if they had received preoperative RT with or without chemotherapy with a minimum delay of 4 weeks to surgery. Patients in Cohort A were treated between 1 January 2010 and 31 December 2018; a detailed description of this cohort has been published previously [15]. Cohort B consisted of data for consecutive patients with rectal cancer in the Stockholm region diagnosed between 1 January 2006 and 31 December 2016. Patients were followed for recurrence and survival until 24 March 2022. Several patients in both cohorts were included in randomized trials such as Stockholm III (42 in Cohort A and 54 in Cohort B), EXPERT-C (0/33), or RAPIDO (106/35) [9,20,21].

The results of cohort A have been published [15]; we initially sought to determine whether the two patient datasets demonstrated similar associations between the explored variables and pCR; if so, they could be combined to increase statistical power in the calculations of importance for, above all, the three different treatment schedules most commonly used today.

The study was approved by the local ethical committee at Karolinska Institutet as an extension to the approval by the ethical committee at Uppsala University for the Uppsala/Dalarna study. Through approval, we gained access to the prospectively maintained quality register database including all patients in these regions diagnosed with colorectal cancer. This database is part of the national quality register (Swedish Colorectal Cancer Registry [SCRCR] defined in detail at https://scrcr.se/) (accessed on 7 November 2022).

The same inclusion criteria were applied for both cohorts, except that, patients who achieved cCR (n = 22) and were monitored in a W&W strategy were included in the Uppsala/Dalarna study. However, in this analysis, the cCR patients were excluded to achieve histopathological data from the resected specimen for all patients. The differences in collected data between the cohorts included the presence of metastatic lateral lymph nodes according to MRI and thrombocytes collected only in Cohort B. Of the total 361 cases in cohort A, two patients were inadvertently missed before fusion with Cohort B, leaving 359 patients from cohort A for final analysis. Patients with rectal cancer and M0 disease treated with curative intent who received preoperative neoadjuvant or conversion treatment (hereafter referred to as preoperative) followed by delayed surgery performed ≥4 weeks after completion of the RT were eligible. This study excluded patients with concurrent malignant disease and crucial missing information about pathological staging.

Rectal tumours were defined as those located with the caudal limit within 15 cm above the anal verge, the distance being measured by rigid proctoscopy. Low rectal tumours were defined as those 0–5 cm above the anal verge, middle rectum as 6–10 cm, and high tumours as more than 10 cm above the anal verge. The database contains information about clinical, radiological, and histopathological staging, information on all treatments, relapse sites and timepoints, and survival information. This information was retrieved from the SCRCR and the patient’s medical files. Cut-off ≤ 3.5 cm for tumour length was defined with the ROC/Youden method (area under curve [AUC] 0.55; 95% CI 0.50–0.61, p = 0.050). The other cut-offs were defined as previously published [22,23,24].

For both cohorts, neoadjuvant treatment was given according to one of three different protocols:

A: scRT: short-course hypo-fractionated 5 Gy × 5 in one week, and delayed surgery.

B: CRT: Chemoradiation 1.8 Gy × 28 or 2 × 25 Gy concomitant with capecitabine 825 mg/m² twice daily, days 1–38 or 900 mg/m² on RT days, and delayed surgery.

C: scRT/CRT + CTX: neoadjuvant scRT or CRT preceded or followed by chemotherapy as part of the clinical trials EXPERT-C and RAPIDO. The EXPERT-C randomised phase II trial administered four cycles of capecitabine and oxaliplatin (CAPOX) alone or with cetuximab, followed by CRT, TME-surgery, and further four cycles of adjuvant CAPOX [21]. The RAPIDO study compared CRT as standard arm versus an experimental arm starting with 5 Gy × 5, followed by six courses of CAPOX before surgery [9]. Adjuvant chemotherapy using 8 cycles of CAPOX was provided in the standard arm.

Radiology included pelvic MRI and chest, abdominal, and pelvic CT at baseline used as a basis in these analyses. Restaging 3–6 weeks after completion of the neoadjuvant treatment served as grounds for decision making regarding curative surgery during a multidisciplinary team (MDT) conference, but these results were not included in the analyses.

Statistics

Data were analysed with SPSS (IBM SPSS Statistics for Windows, 2020, Version 27.0.0.1, IBM Corporation, Armonk, NY, USA). Patient demographics are presented as absolute values and percentages, and, for continuous variables, also as median and range. Comparisons of groups were performed by applying the Χ² test for categorical variables. For continuous variables, we applied the non-parametric Mann–Whitney U test or the Wilcoxon signed rank test. Laboratory tests (haemoglobin, leucocytes, thrombocytes, C-reactive protein, and CEA) were analysed as categorical factors. With pCR as a dependent parameter, we used models of binary logistic regression for univariate analyses and calculated odds ratios (OR) and 95% confidence intervals (CI) to predict whether covariates influenced the achievement of pCR. Variables that were associated with pCR in the univariate analyses with p < 0.05 for all patients and <0.10 for treatment groups, and with missing values less than 18% were included in the multivariate logistic regression analyses. Receiver operating characteristics (ROC) with Youden optimization and AUC were calculated to discriminate for the model’s predictive power. The cut-offs for the factors from the multivariate analysis added to the model were the ones used in the Sorbye consensus [22] and those optimized by the Youden method as described above. Relapse-free survival (RFS), overall survival (OS), and disease-specific survival (DSS) were calculated with Kaplan–Meier survival estimates and the Cox proportional hazards model. All p-values were two-sided and considered statistically significant when p < 0.05.

3. Results

3.1. Patient Characteristics

Patient and tumour characteristics for the 359 patients in Cohort A and the 635 in Cohort B are described in Table S1. Minor differences in age and baseline MRI-derived factors, such as cN-stage, cMRF+, cEMVI+ and mucinous tumour, as well as clinical factors such as elevated carcinoembryonic antigen (CEA) distribution were noted. The proportion of patients treated with the three alternatives, scRT, CRT, or scRT/CRT + CTX, varied between the cohorts because of the differences in inclusion times, with Cohort A formed in 2010–2018, and Cohort B in 2006–2016. Prior to June 2011, when the RAPIDO trial comparing CRT and scRT + CTX was initiated, most LARCs were treated with CRT and after June 2016, and when the trial had closed patient entry, these patients continued to be treated with scRT + CTX within the LARCTC-US study (https://clinicaltrials.gov/ct2/show/NCT03729687) (accessed on 23 November 2022). Different treatment schedules resulted in varying times to surgery. Patient and tumour characteristics in the treatment groups (scRT, CRT, and scRT/CR + CTX) in the two cohorts were also in line.

When the associations between the characteristics and the probability of reaching pCR (12.8% in Cohort A and 12.3% in Cohort B) were compared between the cohorts, similar results were observed (Table S2). Because of this, we concluded that the findings reported from Cohort A [15] were confirmed in an independent cohort (Cohort B) and the two cohorts could be pooled.

The clinical characteristics of the pooled cohort (A + B) by treatment group are described in Table 1. Patients treated with scRT were older and had less advanced tumours (cT1-3, cN0, cMRF-, or cEMVI-) according to treatment indication, and had fewer mucinous tumours and shorter tumour lengths, but higher C-reactive protein (CRP) levels. The most advanced tumours were observed in the scRT/CRT + CTX group.

Survival was compared between the pCR and non-pCR groups. The median reverse Kaplan–Meier follow-up was at 64 months (95% CI 63–65). RFS was significantly better in the pCR group (HR 0.22; 95% CI 0.13–0.37), with 5-year RFS rates of 96% in pCR versus 79% in non-pCR groups (Figure S1A). OS was better in the pCR group with a 5-year OS rate of 92% compared with 70% in the non-pCR group (Figure S1B). DSS, considering CRC deaths and censoring deaths from other causes, was also higher in the pCR arm, with a 5-year DSS rate of 96% in the pCR group versus 79% in the non-pCR group (Figure S1C).

3.2. Clinical Factors and pCR

pCR was achieved in 12% of the 994 patients. pCR was noted in 8% (33/435) with scRT, in 13% (48/358) with CRT, and in 21% (43/201) with scRT/CRT + CTX (p < 0.001).

Characteristics of the patients who achieved pCR compared to those who did not are presented in Table 2. Tumour characteristics such as cT-stage (p = 0.027) and tumour length (p = 0.010) were statistically significantly associated with pCR. Furthermore, laboratory parameters, including leucocytosis (p = 0.014), thrombocytosis (p = 0.023), elevated CRP (p < 0.001), and CEA (p = 0.001) were statistically significantly different between the pCR and non-pCR groups. The cohort did not show any difference.

Data regarding the probability of reaching pCR according to treatment are shown in Table 3. Significant differences for all patients were noted for age, cT-stage, cN-stage, cMRF, cEMVI, mucinous tumour, and weeks from RT to surgery for treatment (exact p-values not shown). Differences in pCR rates for the scRT group were noted for cT-stage, cMRF, cEMVI, and CEA. For the CRT group, differences in pCR versus non-pCR were noted for cT-stage, tumour length, and elevated CEA. For the scRT/CRT + CTX arm, only sex was statistically significant in the pCR versus non-pCR comparison.

3.3. Univariate and Multivariate Analyses for pCR

Patients achieving pCR were compared to non-pCR patients for clinical and tumour-related factors (Table 4). In the univariate binary logistic regression analyses for pCR, statistical significance was noted for age ≤ 70 years (OR 2.09, 95% CIs in Table 4), cT1-2 (OR 2.47, with T4 as reference), tumour length ≤3.5 cm (OR 1.84), time from RT to surgery (OR 1.57), normal leucocytes (OR 2.37), normal thrombocytes (OR 4.57), normal CEA (OR 2.03), or CRT (OR 1.89, with scRT as reference), and scRT/CRT + CTX (OR 3.32 with scRT as reference).

In multivariate analysis (n = 735 with 98 events), seven covariates with p-value < 0.05 in the univariate analyses were included, excluding thrombocytes not collected in Cohort A. Factors that were statistically significant for pCR in the multivariate model included cT1-2 (OR 3.37 with cT4 as reference), tumour length ≤ 3.5 cm (OR 2.27), non-elevated CEA (OR 1.73), and CRT (OR 2.61 with scRT as reference) or scRT/CRT + CTX (OR 4.70 with scRT as reference). Interaction terms for the significant factors were not significant and thus not included in the multivariate model (p-value for cT-stage + tumour length was 0.963, cT-stage + CEA was 0.957, and cT-stage + treatment group was 0.850).

We examined predictive factors associated with pCR for the three treatments separately. In the scRT group (n = 435), univariate analyses demonstrated that age ≤ 70 years, cT1-2, cMRF-, cEMVI-, and normal thrombocytes were associated with higher pCR rates (Table S3), with none of the factors remaining statistically significant in the multivariate analysis (n = 294). In the CRT population (n = 358), cT1-2, tumour length ≤ 3.5 cm, and normal CEA were associated with a higher pCR rate in the univariate analyses, and cT1-2 (OR 5.94) remained statistically significant in the multivariate analysis (n = 301, Table S4). In the scRT/CRT + CTX group (n = 201), female sex with OR 2.00 was the only statistically significant factor in the univariate analyses (Table S5).

3.4. Predictive Model for pCR

A predictive model for pCR was developed based on factors identified in the multivariable analysis (Table S6, Figure S2). Cut-offs were based on TNM classification, the literature, and the ROC defined.

The scoring points for cT-stage (cT1-2 = 0, cT3 = 0.5, and cT4 = 1), tumour length (≤3.5 cm = 0, 4–7 cm = 0.5, and >7 cm = 1), CEA (≤3 µg/L = 0, 3–5 µg/L = 0.5, and >5 µg/L = 1), and leucocytes (≤8.2–10⁹/L = 0, 8.3–10⁹/L = 0.5, and >10⁹/L = 1) were combined, thus resulting in a maximum score of 4. ORs and 95% CIs are presented in Table S6.

The performance of the combined pCR effects model obtained an AUC of 0.65 (95% CI 0.60–0.71), with cut-off < 1.75 points for the whole cohort (p < 0.001), of which 25% had pCR. In the subgroup treated with scRT, AUC was 0.73 (0.62–0.83) and cut-off < 1.25 points and 16% had pCR; in the CRT group, AUC was 0.67 (0.58–0.76) with cut-off < 1.75 points and 31% had pCR; and for scRT/CRT + CTX, AUC was 0.65 (0.55–0.75) with cut-off < 1.75 points and 50% had pCR (all statistically significant).

4. Discussion

The highest pCR rates of 21% were achieved with scRT/CRT + CTX compared with 13% with CRT and 8% with scRT in this pooled analysis of rectal cancer patients who underwent surgery after a delay following pre-treatment. Independent factors associated with pCR were cT1-2, tumour length ≤ 3.5 cm, normal CEA, and treatment modality. Leucocytosis also adds to the model. This may have practical importance when discussing whether a non-surgical W&W approach could be recommended prior to treatment initiation.

Our population-based results indicate that treatment with RT, either preceded or followed by systemic chemotherapy, i.e., TNT, is the most effective treatment modality for achieving pCR. In recent years, the focus has been directed towards more extensive administration of chemotherapy in the neoadjuvant setting and several clinical trials have been performed or are ongoing [9,10,25,26]. Results from the RAPIDO study demonstrated the superiority of scRT + CTX versus CRT in preventing disease-related events, predominantly systemic recurrences, and support our findings regarding the hierarchy of preoperative treatments in achieving pCR [9]. Despite a two-fold higher chance of pCR in the experimental group (28% versus 14%) [9], a 5-year update of the trial has revealed more locoregional failures in the experimental group (12% vs. 8%, p = 0.07) [27]. Results from the US OPRA study with CRT and chemotherapy either as induction or consolidation showed better organ preservation rates (3-year TME-free survival rate 41% vs. 53%), when the chemotherapy was given as consolidation after CRT [11].

Several studies have reported cT-stage as an independent variable to predict pCR [28,29], in line with our findings. Our cohort of patients with cT1-2 tumours was limited (n = 62, as most patients with cT1-2 tumours underwent surgery directly or were treated with scRT without a delay to surgery and were thus excluded from analysis), but achieved a pCR rate of 23%, and this was as high as 50% in the CRT group. With a corresponding rate for cT3 tumours of 13% we can conclude that, not surprisingly, cT1-2-stage can be used as predictive factor for pCR when using scRT or CRT. Most cT2-stage patients are regularly not candidates for pre-surgical treatment, and too few patients with cT1-2 tumours were treated with scRT/CRT + CTX to draw any conclusions. In Cohort A, a subdivision of cT3-stage into the substages a-d was explored [15]; however, this was not recorded in cohort B. It is possible that the best discriminator is not between cT2 and cT3 but rather within cT3. Separation of cT2 from cT3a is also difficult using MRI [30].

Length of tumour persistently demonstrated statistically significant associations with pCR in our examination for the entire cohort. We found a cut-off of ≤3.5 cm to be a break point for tumours responding with pCR. The calculated AUC 0.55 indicates, however, a limited discriminative strength and necessitates incorporation of other parameters when predicting pCR. A study by Jankowski et al. [31] showed that a tumour length > 7 cm and circumferent extension of the tumour meant that only 1.6% could achieve a sustained cCR with a sensitivity as low as 23% [31]. In our study, we did not retrieve data for the extent of circumferential tumour engagement of the rectal wall; thus, our results are not comparable with the Polish study. It is fully plausible that cT-stage and tumour length overlap as larger tumours are more often associated, but not necessarily always (reflected in non-significant interaction term), with higher cT-stage with deeper invasion into the rectal wall. In this way, their significance as predictive factors may intertwine.

The serum marker CEA has been used to predict prognosis both pre- and post-operatively, and it is an important tool for surveillance of colorectal patients to detect recurrence post-operatively [24]. CEA has also been the subject of interest as a predictor for response to neo-adjuvant therapy in rectal cancer, most studies of which have found associations with pCR rates [14,15,28,32,33,34]. In a report from Joye et al., a CEA cut-off of 4.6 µg/L was applied and an association between pre-treatment CEA and probability for pCR was found in a multivariable analysis [14]. Furthermore, in our study, a pre-treatment CEA value below reference (≤5 µg/L) had a positive association with an OR of 1.28 for reaching pCR (whereas the ROC-defined subgroup with ≤3 µg/L had an OR of 2.39). CEA was the only laboratory parameter in the full cohort that demonstrated statistically significant associations with pCR in both univariate and multivariable analyses; however, the number of patients with missing values for the other laboratory tests was quite high (9–45%).

The significance of age in univariate analyses is probably related to the active selection of younger fit patients for more intense treatment. Older patients, often with comorbidities, may not always tolerate these treatments and are left with scRT alone, which has less cell killing effect and, thus, fewer pCRs, as seen in a systematic review [35].

Our findings of both leucocytosis and thrombocytosis being significant covariate factors in univariate analyses are in accordance with previous reports in LARC [17,36,37,38,39]. These associations were most pronounced in the scRT/CRT + CTX-group. Thrombocytosis could not be added to the multivariate model as this information was available only in Cohort B. Pre-treatment haemoglobin value and its relation to oncologic treatment response (particularly RT) and prognosis in solid tumours, including rectal cancer, have been the focus of several studies [14,28,40]. A higher pre-treatment haemoglobin value is associated with pCR likelihood [14,28], in line with a trend in our study. Clinically, haemoglobin values are probably of limited relevance.

MRI-defined cMRF+ and cEMVI+ were significantly associated with pCR in the scRT group but not in the CRT or scRT/CRT + CTX groups. Both involved MRF and positive EMVI indicate a more advanced tumour and the reference treatment is either CRT or scRT/CRT + CTX. Thus, scRT was provided only to fragile patients not tolerating the reference treatment. Therefore, if a suboptimal treatment must be given, with scRT for an advanced tumour, both MRF+ and EMVI+ mean a lower chance of pCR. If the reference treatment is applied, neither of these factors are important for predicting pCR (or potentially for a cCR if a W&W policy is applied).

In summary, besides treatment protocol, early tumour stage (cT1-2), tumour length ≤ 3.5 cm, normal routine blood counts, and CEA can assist in predicting pCR and, ultimately, cCR state in a setting before neoadjuvant treatment initiation. The decision to aim for organ preservation by giving more active neoadjuvant treatment than indicated can thus be supported by our model, with the caveat of its limitation as AUCs were in the range of 0.65–0.73, sensitivity and specificity 59–70%, and pCR carried rates of 16–50%. The predictive factors and the model also need to be validated in other large patient series, preferably prospective, and we will start with the RAPIDO [9] dataset. In this regard, other markers, serial examinations with MRI, PET-CT, and functional radiology measuring the tumour’s metabolic activity before and early during the treatment could improve the baseline model in the future [41].

Better survival has also been observed in patients achieving pCR [12,13] in line with our findings for OS, DSS, and RFS (with 5-year rates of 92%, 96%, and 92%, respectively). pCR status thus helps in decisions to omit adjuvant therapy [42]. A third decision our prognostic factors may support is to sustain from surgery in cCR and offer a W&W strategy. Today, this is normally based on tumour-free proctoscopy, digital examination, and MRI. Still, in this situation, there is a clear risk that tumour cells persist [43]. It has been reported that a near-pCR situation is not associated with the same favourable prognosis as pCR [44,45]. This adds to the dilemma and necessitates incorporation of further tools to judge durable tumour control probability with better certainty.

Our study has limitations associated with retrospective studies. The exclusion of cCR patients also reduced the number of favourable outcome patients in cohort A. Undeniably, there has been a selection bias as many patients were selected for different treatment protocols based on age and comorbidities. In terms of strengths, this was a comprehensive study that included a large number of patients treated with the three most widely utilized neoadjuvant protocols after up-to-date staging, including an MRI for all patients.

5. Conclusions

The choice of neoadjuvant treatment in combination with low CEA, short tumour length, low cT-stage, and normal leucocytes provide support in predicting pCR and, thus, could offer guidance for selection of patients for organ preservation strategies at baseline, i.e., to provide neoadjuvant rather than adjuvant treatments and W&W strategies.

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Supplementary Materials

The following supporting information can be downloaded at: https://www.mdpi.com/article/10.3390/cancers14246238/s1, Table S1: Comparison of major clinical and imaging characteristics of cohort A and cohort B; Table S2: Comparison of clinical, laboratory, and imaging-defined characteristics between pCR vs. non-pCR groups for cohort A (n = 359) and cohort B (n = 635); Table S3: Univariate and multivariate analyses of the scRT cohort (n = 435) for clinical, laboratory, and imaging-defined factors predicting pCR status; Table S4: Univariate and multivariate analyses of the CRT cohort (n = 358) for clinical, laboratory, and imaging-defined factors predicting pCR status; Table S5: Univariate and multivariate analyses of the scRT/CRT + CTX cohort (n = 201) for clinical, laboratory, and imaging-defined factors predicting pCR status; Table S6: Score board for the predictive pCR model; Figure S1: Relapse-free survival (RFS; panel A), overall survival (OS; panel B), and disease-specific survival (DSS) of patients with tumours achieving a pathologic complete response (pCR) compared to non-pCR; Figure S2: Receiver operator characteristics (ROC) and area under the curve (AUC) with cut-offs optimized by Youden for the model including MRI cT-stage, tumour length, elevated CEA, and leucocytosis for all patients (ALL; panel A), short-course radiotherapy (scRT; panel B), chemoradiation (CRT, panel C), and scRT/CRT aS2: and chemotherapy (scRT/CRT + CTX, panel D) groups.

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