Minimally Invasive Versus open AbdominoThoracic Esophagectomy for esophageal carcinoma (MIVATE) — study protocol for a randomized controlled trial DRKS00016773

The primary endpoint will be postoperative morbidity assessed as the comprehensive complication index (CCI) within 30 days after index operation [22], which enables to compare the severity of postoperative complications [23].

Postoperative morbidity is defined as any deviation from the normal postoperative course according to the Dindo-Clavien classification [24]. Specifically, it includes anastomotic insufficiency or loss of anastomotic integrity verified by either CT scan with detection of contrast agent externally from the anastomosis within the abdominal or thoracic cavity, endoscopy, or the detection of methylene blue in the drainage after oral application. Also, it includes pneumonia with radiological verification of pneumonic infiltrates and a minimum of 3 of 4 possible symptoms including a body core temperature above 37.5 °C, purulent expectoration, leucocyte count above 12,000 or below 4500/ml, or increased C-reactive protein (CRP) levels. Postoperative complications also include pancreatic fistula, which is defined by the International Study Group for Pancreatic Surgery (ISGPS) as the “drain output of any measurable volume of fluid with an amylase level > 3 times the upper limit of institutional normal serum amylase activity, associated with a clinically relevant development/condition related directly to the postoperative pancreatic fistula.” The former grade A fistula is now called a “biochemical leak,” as it has no clinical relevance. Fistula grades B and C are defined more precisely. Grade B requires drains that are either left in place > 3 weeks or repositioned. Grade C requires reoperation or leads to single or multiple organ failure [25, 26]. Recommendations for reporting of complications after esophagectomy will be obeyed in order to improve comparability with future trials [27]. Other aspects are postoperative bleeding with a hemoglobin relevant decrease beyond 3 g/dl or the necessity for transfusion of erythrocyte concentrates due to bleeding into the abdominal or thoracic cavity. Wound healing disorders with special wound treatment, abscess, and lymphatic fistula caused by damage to the lymphatic system with leakage of chyle fluid into the cavities (defined as a milky-colored fluid from a drain, drain site, or wound on or after POD 3, with a triglyceride content ≥ 110 mg/dL respectively ≥ 1.2 mmol/L) also accounts for postoperative morbidity [28, 29]. Further aspects are tracheal injuries with fistula between the esophagus and trachea and loss of tracheal integrity as well as radiologically confirmed deep leg vein thrombosis and pulmonary embolism. Acute kidney failure in direct context to surgery defined as a doubling of plasma creatinine levels or necessity for hemodialysis as well as stroke and myocardial infarction are further criteria included in postoperative morbidity.

The CCI will be reported with mean and standard deviation.

Secondary endpoints can be separated into short-term endpoints and long-term endpoints. Short-term endpoints include operation time, length of hospital stay, duration of stay on intensive or intermediate care unit (ICU), postoperative recovery assessed with QoL-15, postoperative pain assessed with the visual analog scale (VAS), the necessity for vasopressor agents for circulatory support, length of single-lung ventilation, number of days with invasive ventilation, fluid management, postoperative demand for analgesic drugs, and levels of acute-phase proteins in the serum. The successful adherence to an already established fast-track protocol with several sub-categories will also be a secondary endpoint (Additional Tables 1 and 2) [3, 30]. Short-term oncological endpoints are number of removed lymph nodes and rate of R0-resections.

Long-term endpoints are QoL and oncological outcomes such as disease-free-survival, rate of local recurrence and overall-survival. QoL will be assessed with different questionnaires. SF-36 and CAT EORTC QLQ-C30 measure general aspects of health with scores ranging from 0 to 100 and with higher scores representing better well-being. CAT EORTC QLQ-OES18 assesses several aspects of esophageal function, ranging from 0 to 100 with lower scores indicating better function [31].

Extended details of the secondary endpoints can be found in Table 1. Several other scoring systems from other institutions have been included in the design of the MIVATE trail such as the surgical site infection classification according to the CDC (Center for Disease Control and Prevention) (https://​www.​cdc.​gov/​hai/​ssi/​ssi.​html) [32], the ASEPSIS score for wound infection [33], and the standardization of data collection for complications associated with esophagectomy from the Esophagectomy Complications Consensus Group (ECCG) [27].

Based on a t test with a two-sided significance level of α = 0.05, a sample size of n = 34 patients (17 per group) is required in the analysis dataset in order to achieve a power of 80% (calculations performed with Prism 8.0, G*Power and SPSS). To compensate for early trial termination, drop-outs, and loss-to-follow-ups, further 15% of patients will be randomized leading to a total randomization and allocation size of 40 patients (20 per group). The number of patients to be screened and assessed for eligibility (n = 200; 100 per group) was calculated with an assumed 20% of exclusions due to exclusion criteria and a 75% of interfering circumstances (200 × 0.8 × 0.25 = 40; 20 per group). These interfering circumstances are due to the fact that MIVATE is an expertise-based trial which only allows the institution’s single best surgeon for each allocated technique. Consequently, both surgeons have to be available at the time of randomization which is not possible in 3 of 4 cases.

There will be regular meetings by the investigators every 3 months in order to optimize recruitment and ensure sufficient enrolment.

Superiority of the intervention versus the control will be assessed using a two-sided t test. The primary analysis will be based on the intention-to-treat population. If values do not display normal distribution, the Mann-Whitney U test will be used. A per protocol and an as treated set will be evaluated as a sensitivity analysis. Missing data for the primary outcome variable will be replaced by using imputation [40]. The primary analysis will test the following hypotheses:

CCI_open and CCI_{minimally invasive} are the mean of the indices of both groups at different time points.

There will be no interim analysis for the primary endpoint. However, the primary endpoint will be analyzed as soon as all relevant data has been obtained. There will be interim analyses for the secondary endpoints.