Re-staging and follow-up of rectal cancer patients with MR imaging when “Watch-and-Wait” is an option: a practical guide

The concept of “locally-advanced rectal cancer” is intrinsically linked with a clinical indication for neoadjuvant therapy (NAT). It traditionally applies to all clinically staged T3/T4 and/or N+ tumours, although in the UK and other centres across Europe criteria may be more strict [1, 2]. NAT regimens were initially designed with the sole purpose of downsizing/downstaging tumours in order to increase the likelihood of an R0 resection and diminish the risk of local recurrence [3], but the 10–25% pathologic complete response (pCR) rates have led clinicians to question the utility of radical surgery itself in such cases [4]. In fact, the real pCR odds may be even higher, given most patients included in reported studies were operated at 6–8 weeks while pCR rates increase significantly when the interval to surgery is lengthened to > 12 weeks post-radiotherapy (RT) [5]. This means that if patients are re-staged and no signs of tumour persistence are present, deferral of surgery may be a reasonable option, and “Watch-and-Wait” (W&W) programs have grown increasingly available and popular during the past almost 20 years [4]. For willing and able patients, this decision is largely based on re-staging rectal endoscopy and MR imaging assessments [6]. Strict follow-up afterwards is founded on the same grounds [6]. The overall survival of clinical complete responders appears similar to that of patients who undergo surgery and have a pCR [7]. Furthermore, out of the approximately 30% clinical complete responders who later on present with tumour regrowth, 95% are salvageable [8]. However, patients with local regrowth may present with a higher rate of distant metastatic disease compared to sustained clinical complete responders [9]. Whether this phenomenon is a reflection of the tumour biology or a consequence of an uncontrolled primary is not yet known [9]. Magnetic resonance (MR) imaging, as part of response assessment, should aim to distinguish “true” complete responders from patients with persistent, even if subclinical, disease, who need surgery for cure as early as possible. This educational review has three purposes: the first is to provide radiologists with the main relevant information to re-stage rectal cancer patients after NAT based on standard MR imaging; the second is to guide them through W&W follow-up MR imaging assessments in order to detect pelvic regrowths /recurrences as early as possible; the third is to present and discuss our proposed report template.

Before MR imaging acquisition, there are two preparatory steps which may significantly contribute to improve image quality. The first step is to ask patients to perform a small enema for rectal emptying before entering the MR equipment [10]. The second is to administer a spasmolytic agent such as butylscopolamine or glucagon before acquisition [10]. These two preparation steps are meant to minimise susceptibility artefacts due to air content and movement artefacts from peristalsis, respectively, given both adversely impact image interpretation, of diffusion-weighted imaging (DWI) in particular [10]. They are considered optional according to both ESGAR and SAR guidelines [11, 12]. When despite these measures patients still present with rectal air at tumour bed level and if they agree, a lubricated cannula can be inserted in the rectum for further emptying, and then removed before acquisition.

The use of endoluminal gel is not advocated routinely because distension of the rectum may result in misinterpretation of the distance between the tumour bed and circumferential resection margin (CRM), an essential re-staging information when surgery is a possibility [13]. If considered useful, gel should not exceed 60 ml to prevent excessive compression of the mesorectal fat [14].

Regarding technique, examinations should be performed on a 1.5T or 3T equipment using an external coil [11, 12]. 2D high-resolution T2-WI with a slice thickness \(\le\)3 mm should be acquired in sagittal, axial and coronal planes, the two latter angulated perpendicular and parallel to the long axis of the tumour, respectively [11, 12]. In low tumours, additional high-resolution T2-WI angulated perpendicular and parallel to the anal canal may be acquired to better assess its involvement [11, 12]. A DWI acquisition including a high b value (≥ 800) should also be acquired, preferably with the same orientation as the axial high resolution T2-WI to ease finding co-localisation [11, 12]. Intravenous paramagnetic contrast administration is not routinely recommended [11, 12] but it may be useful in particular situations such as pelvic sepsis or fistulisation. Detailed acquisition protocols for our 1.5T and 3T Ingenia Philips Healthcare®, Best, The Netherlands clinical scanners are provided in Table 1.

The issue of when to first assess tumour response is controversial. While the rate of pCR may increase after 12 weeks post-RT [5] some surgical teams are reluctant to operate beyond 8 weeks due to concerns about radiation-induced pelvic fibrosis and related surgical complications [15], which implies identifying poor/incomplete responders early. To move the decision timepoint from 6–8 weeks to 10–12 weeks post-RT may have no impact on surgery-related morbidity or mortality [16], and the extended period of surveillance may allow the start of consolidation chemotherapy on metastatic high-risk patients that may benefit from total NAT.

Although clinical and laboratory evaluation is relevant, re-staging relies heavily on rectal endoscopy and MR imaging. If the two are to be performed on the same day and given endoscopy requires the insufflation of air into the rectum, to perform MR imaging first may be preferable in order to minimise air-induced susceptibility artefacts.

Endoscopic assessment [16] may be standardised according to a 5-point ordinal scale defined by the international W&W database consortium: responses may be graded, from best to worse response, as 0 (flat white scar with telangiectasia), 1 (shallow ulcer/red scar), 2 (ulcerated residual lesion or adenomatous residual mucosal abnormality), 3 (excavated ulcer with elevated edges) or 4 (persistent infiltrative lesion).

Our proposed re-staging and follow-up reporting template is shown in Fig. 11. Please keep in mind that it is a mere suggestion and has not been validated in a prospective and multi-institutional setting.

Compared to the re-staging report template provided by ESGAR [10], ours is more complex, time-consuming and cumbersome to use because it includes multiple methods reported for response assessment and also contemplates follow-up imaging after re-staging. It involves recording thickness, volume, depth angle and their variation compared to the previous examination, given its potential, unvalidated utility in the early prediction of a non-sustained complete response, as discussed above. Also, our response assessment of the primary tumour is based on separate mrTRG, split scar sign and 3-point ordinal scale DWI evaluation, while ESGAR recommends using a 3-point combined T2-WI/DWI ordinal scale.

“Watch-and-Wait” rectal cancer programs are growing around the world and revolve around endoscopy and pelvic MR imaging, both for re-staging and patient follow-up. Radiologists involved in such programs should be familiar with the imaging findings that suggest a poor/incomplete response, a complete response or a “near-complete” response and their prognostic implications. They should also be equipped for the early detection of local regrowths, in depth at tumour bed or extra-rectal in particular, given their invisibility at rectoscopy.