Patients and study design

This is a post hoc explorative analysis of data from two prospective interventional trials [12,13] approved by the North West – Liverpool East Research and Ethics Committee (11/H1002/12) and registered with ClinicalTrials.gov (NCT01325909 and NCT01859442). Written informed consent was obtained from all patients. Additional consent was sought for a pre-operative MRI and inclusion in these analyses. We recruited patients between August 2012 and August 2014 referred to the Colorectal Multi-Disciplinary Team (MDT), age ≥18 years, with locally advanced (circumferential resection margin threatened – defined as tumor within 1 mm of the mesorectal fascia or if any T3/4 tumor was arising at <5 cm from the anal verge) resectable rectal cancer, scheduled for standardized NACRT on the basis of Tumor, Node, Metastasis (TNM) classification > T2/N + with no distant metastasis [17] and WHO Performance Status < 2 [18]. Exclusion criteria were: inability to give informed consent, non-resectable disease, and patients who declined surgery or NACRT, or who received nonstandard NACRT.

Consenting patients underwent tumor staging (methodology reported elsewhere [12,13]) and completed 5 weeks of NACRT with periodic cardiopulmonary exercise testing (CPET) to evaluate physiological responses and to tailor the responsive exercise intervention (methodology of the standardized chemoradiotherapy regime is reported elsewhere [12]). No patients received brachytherapy. Immediately after NACRT, patients were allocated to the exercise-training group by default. Patients unable to commit to the exercise schedule (residing >15miles from the hospital) were asked to act as contemporaneously recruited controls (no exercise intervention) with the same CPET follow-up. At 9 weeks post-NACRT, patients were restaged using chest, abdomen and pelvic CT and pelvic MRI as per local standard of care rectal cancer pathway. At 14 weeks, post-NACRT patients were restaged using pelvic MRI (additional research scan), prior to surgery at week 15.

Cardiopulmonary exercise testing protocol and exercise intervention

The CPET protocol followed the consensus clinical guidelines on conduct and physiological interpretation defined by the Perioperative Exercise testing and Training Society [19]. The exercise intervention is described in Appendix 1 according to Consensus on Exercise Reporting Template (CERT) [20]. The same method was used for participants during both trials. Exercise adherence is calculated as a percentage of prescribed exercise sessions that were completed by trial participants.

Patients in the exercise group were classified as responders or non-responders to the exercise intervention (responder definition was an increase in oxygen uptake (VO₂) at anaerobic threshold (AT) ≥2.0 ml·kg⁻¹·min⁻¹ between post-NACRT and week 6). Pre-operative CPETs were analyzed by two CPET accredited clinicians, blinded to patient intervention group allocation and any outcome measure. If interpretation of AT varied by >0.5 ml·kg⁻¹·min⁻¹, the CPET was analyzed by a third adjudicator.

MRI technique and image analyses

MRI acquisition technique was performed as described by Patel et al. [21,22]. MR images were reviewed independently both centrally and locally, blinded to each other, the patient intervention group allocation and any other outcome measure. MR image analysis was carried out, using the terms ymrT (T stage on MRI images obtained after NACRT), ymrTRG (tumor regression grade on MRI images obtained after NACRT), ypT (T stage on post-treatment histopathological examination of the resection specimen) and ypTRG (tumor regression grade on post-treatment histopathological examination of the resection specimen) to describe the data [21,23]. The MRI protocol and image analyses are reported elsewhere [24].

Surgical resection

All patients underwent total mesorectal excision (TME) [25] with or without abdominoperineal excision, performed 15 weeks (±4 days) after the completion of NACRT.

Histopathology assessment

After surgical resection, the specimen was fixed in formalin for 48 h, cross-sectioned into 3–5 mm slices, and histologically sampled. A predefined protocol assessed pathological complete response, with a minimum of five blocks of tumor taken. If no tumor was found on the first set of hematoxylin and eosin sections, the rest of the tumor area was embedded, and if no tumor was seen then a final three levels were taken through each block to look for tumor to confirm a complete response. Each specimen was graded by degree of tumor regression, according to the Dworak system and also by ypT stage. As well as grading and staging by the five-point ypTRG and TNM version 7 systems, a simplified pathological grading of favorable and unfavorable pathology was also undertaken. Favorable pathology was defined as ypT stages 0, 1, 2 and 3a or ypTRG stages 3 and 4. Unfavorable pathology was defined as ypT stages 3b, c, d, and 4 or ypTRG stages 0, 1 and 2. ypT3a was included in the favorable group as these tumors have been shown to have a similar prognostic outcome as ypT2 tumors [26,27].

Statistical analysis

Central reviewer (Royal Marsden; GB) data were used for the primary analysis based on validated methodology also used by Patel et al. [21,24]. Data were described as frequency (percentage) and mean (SD), with 95% confidence intervals (95%CIs), as appropriate. To analyze the association between demographic variables (age and sex), CPET parameters (VO₂ at AT and VO₂ at peak exercise), MRI parameters (ymrT, ymrTRG, volume change) and pathologic tumor response (ypT and ypTRG), univariate logistic regression analysis or Fischer’s exact test was used. Univariate logistical regression models with ypT, ypTRG, ymrT and ymrTRG as outcomes, and explanatory variables exercise/control were undertaken. Linear regression models using ymrTRG, ypTRG and ypT as continuous variables were undertaken. Logistic regression enabled calculation of odds ratio (OR) along with 95%CIs where possible. In addition to an intention to treat analyses a per protocol analysis was carried out excluding five patients who deviated from the MRI reporting protocol due to technical MR sequence acquisition standards and one patient in the control group whose VO₂ at AT improved by more than 2.0 ml·kg⁻¹·min⁻¹ between post-NACRT and week 6. Two-tailed p<.05 was considered statistically significant unless specified otherwise. Calculations were performed using Statistical Package for Social Sciences program, version 22.0 (SPSS, IBM, Armonk, NY, USA) and Stata, version 11.2 (StataCorp, College Station, TX, USA). A sample size calculation based on changes in fitness variables was undertaken for the main trial [12]. As these interesting observations arise from post hoc analyses they should be treated as feasibility data to power future work.

T stage, tumor regression grading and volume change at week 9 and week 14 on MRI images obtained after NACRT

Univariate logistical regression models of age, gender, ymrT, ymrTRG and volume change at week 9 and week 14 compared to ypT and ypTRG histopathology grading are reported elsewhere [24].

Changes in objectively measured fitness over time in both exercise and control groups

Table 2 reports changes in selected CPET variables (VO₂ at AT and VO₂ at peak exercise) over time between the exercise and control groups. Figure 1 depicts changes in VO₂ at AT over the whole study period. NACRT was associated with a mean decrease in VO₂ at AT of –2.0 ml·kg⁻¹·min⁻¹ (p < .0001 95%CI –1.3 to –2.6) and VO₂ at peak of –3.4 ml·kg⁻¹·min⁻¹ (p<.0001 95%CI –4.7 to –1.9) across the cohort. Exercise was associated with a significant rescue in these parameters (VO₂ change) (VO₂ at AT +2.3 ml·kg⁻¹·min⁻¹ (p < .0001; 95%CI 1.52–2.95) and VO₂ at peak +3.0 ml·kg⁻¹·min⁻¹ (p=.0004 95%CI 1.48–4.46). Sixteen patients of 26 in the exercise group were classified as exercise responders (2.3 ml·kg⁻¹·min⁻¹ (SD 1.0)).

Exercise prehabilitation may lead to augmented tumor regression following neoadjuvant chemoradiotherapy in locally advanced rectal cancer

All authors

M. A. West, R. Astin, H. E. Moyses, J. Cave, D. White, D. Z. H. Levett, A. Bates, G. Brown, M. P. W. Grocott & S. Jackon behalf of the Fit-4-Surgery Consortium

https://doi.org/10.1080/0284186X.2019.1566775

Published online:

06 February 2019

Figure 1. Line diagram showing fitted means and 95%CI for VO₂ at LT (ml·kg⁻¹·min⁻¹) for the exercise and control groups.

Display full size

A total of 98% of the sessions were completed by participants, according to the prescription. There were no missed neoadjuvant chemo- or radiotherapy sessions due to the exercise and no attributable adverse events.

Tumor outcomes and exercise response

Tables 3 and 4 show MRI (ymrTRG and ymrT stage at weeks 9 and 14) and histopathological outcomes (ypT and ypTRG) in the exercise and control groups, with data treated as either categorical (Table 3) or continuous (Table 4).

There was no significant difference in ymrTRG between exercise and control groups at week 9 (continuous data; OR –0.2 95%CI –1.0 to 0.7, p=.7, categorical data; OR 2.2 95%CI 0.4–10.5, p=.3) or week 14 (continuous data; OR –0.9 95%CI –1.9 to 0.1, p=.1, categorical data; OR 4.4 95%CI 0.8–23.9, p=.09). A linear mixed model comparing ymrTRG in both groups over time showed a significant time effect (coefficient 0.8 95%CI –1.4 to –0.1, p=.02) (Figure 2). At the time of surgery, there was significantly greater histological tumor regression in the exercise group (continuous data OR 1.2 95%CI 0.2–2.2, p=.02, categorical data; OR 8.5 95%CI 1.4–51.5, p=.02). This tumor regression did not result in a significant difference in ypT-stage (continuous data; OR –1.3 95%CI –3.9 to 1.3, p=.3, categorical data; OR 1.1 95%CI 0.2–6.9, p=.9).

Exercise prehabilitation may lead to augmented tumor regression following neoadjuvant chemoradiotherapy in locally advanced rectal cancer

All authors

M. A. West, R. Astin, H. E. Moyses, J. Cave, D. White, D. Z. H. Levett, A. Bates, G. Brown, M. P. W. Grocott & S. Jackon behalf of the Fit-4-Surgery Consortium

https://doi.org/10.1080/0284186X.2019.1566775

Published online:

06 February 2019

Figure 2. A line diagram showing fitted means and 95%CI for ymrTRG for exercise and control groups.

Display full size

Limitations to this study

The main limitations in this study are the small cohort size, intervention participation was on a voluntary basis and the lack of matched controls with similar sample size. This analysis was performed as an explorative post hoc sub-group analysis from a larger published clinical patient cohort which was not powered to detect a significant change in tumor size in association with exercise, exposing analyses to possible type 2 and type 1 errors. Moreover, these findings were discovered with these post hoc intentions to treat and per protocol analyses presented in this study, after publication of findings in West et al. [24]. The findings need to be replicated in an appropriately powered study to confirm our preliminary observations which our group have recently undertaken [51].

No mechanistic investigations were included in the design of this study and so we can offer no insight on possible causation or mechanism of any relationship between exercise and tumor response to NACRT. Further work is required in establishing whether causation exists in the relationship, and its scientific basis.

Confirmation of an effect of exercise in augmenting chemoradiotherapy would have significant impact on treatment pathways in rectal cancer patients, establishing structured exercise as a legitimate anti-cancer therapy in addition to its role in pre-surgical optimization. Understanding the mechanism by which exercise works to augment NACRT would allow training programs to be tailored to individuals to achieve the appropriate response and possibly provide new pharmaco-therapeutic targets for patients undergoing exercise programs.