Cotton Cary C, Wolf W Asher, Overholt Bergein F, Li Nan, Lightdale Charles J, Wolfsen Herbert C, Pasricha Sarina, Wang Kenneth K, Shaheen Nicholas J
From the University of North Carolina at Chapel Hill, Center for Esophageal Diseases and Swallowing, Division of Gastroenterology and Hepatology, Chapel Hill, North Carolina.
Gastrointestinal Associates, Knoxville, Tennessee.
Gastroenterology. 2017 Sep;153(3):681-688.e2. doi: 10.1053/j.gastro.2017.05.044. Epub 2017 Jun 1.
BACKGROUND & AIMS: The goal of treatment for Barrett's esophagus (BE) with dysplasia is complete eradication of intestinal metaplasia (CEIM). The long-term durability of CEIM has not been well characterized, so the frequency and duration of surveillance are unclear. We report results from a 5-year follow-up analysis of patients with BE and dysplasia treated by radiofrequency ablation (RFA) in the randomized controlled Ablation of Intestinal Metaplasia Containing Dysplasia (AIM) trial.
Participants for the AIM Dysplasia trial (18-80 years old) were recruited from 19 sites in the United States and had endoscopic evidence of non-nodular dysplastic BE ≤8 cm in length. Subjects (n = 127) were randomly assigned (2:1 ratio) to receive either RFA (entire BE segment ablated circumferentially) or a sham endoscopic procedure; patients in the sham group were offered RFA treatment 1 year later, and all patients were followed for 5 years. We collected data on BE recurrence (defined as intestinal metaplasia in the tubular esophagus) and dysplastic BE recurrence among patients who achieved CEIM. We constructed Kaplan-Meier estimates and applied parametric survival analysis to examine proportions of patients without any recurrence and without dysplastic recurrence.
Of 127 patients in the AIM Dysplasia trial, 119 received RFA and met inclusion criteria. Of those 119, 110 (92%) achieved CEIM. Over 401 person-years of follow-up (mean, 3.6 years per patient; range, 0.2-5.8 years), 35 of 110 (32%) patients had recurrence of BE or dysplasia, and 19 (17%) had dysplasia recurrence. The incidence rate of BE recurrence was 10.8 per 100 person-years overall (95% CI, 7.8-15.0); 8.3 per 100 person-years among patients with baseline low-grade dysplasia (95% CI, 4.9-14.0), and 13.5 per 100 person-years among patients with baseline high-grade dysplasia (95% CI 8.8-20.7). The incidence rate of dysplasia recurrence was 5.2 per 100 person-years overall (95% CI 3.3-8.2); 3.3 per 100 person-years among patients with baseline low-grade dysplasia (95% CI 1.5-7.2), and 7.3 per 100 person-years among patients with baseline high-grade dysplasia (95% CI 4.2-12.5). Neither BE nor dysplasia recurred at a constant rate. There was a greater probability of recurrence in the first year following CEIM than in the following 4 years combined.
In this analysis of prospective cohort data from the AIM Dysplasia trial, we found BE to recur after CEIM by RFA in almost one third of patients with baseline dysplastic disease; most recurrences occurred during the first year after CEIM. However, patients who achieved CEIM and remained BE free at 1 year after RFA had a low risk of BE recurrence. Studies are needed to determine when surveillance can be decreased or discontinued; our study did not identify any BE or dysplasia recurrence after 4 years of surveillance.
治疗伴有发育异常的巴雷特食管(BE)的目标是彻底根除肠化生(CEIM)。CEIM的长期持久性尚未得到充分描述,因此监测的频率和持续时间尚不清楚。我们报告了在随机对照的含发育异常的肠化生消融(AIM)试验中接受射频消融(RFA)治疗的BE和发育异常患者的5年随访分析结果。
AIM发育异常试验的参与者(18 - 80岁)来自美国的19个地点,内镜检查有长度≤8 cm的非结节性发育异常BE的证据。受试者(n = 127)被随机分配(2:1比例)接受RFA(环形消融整个BE段)或假内镜手术;假手术组的患者在1年后接受RFA治疗,所有患者随访5年。我们收集了实现CEIM的患者中BE复发(定义为管状食管中的肠化生)和发育异常BE复发的数据。我们构建了Kaplan-Meier估计值并应用参数生存分析来检查无任何复发和无发育异常复发的患者比例。
在AIM发育异常试验的127名患者中,119名接受了RFA并符合纳入标准。在这119名患者中,110名(92%)实现了CEIM。在超过401人年的随访中(平均每位患者3.6年;范围0.2 - 5.8年),110名患者中有35名(32%)出现BE或发育异常复发,19名(17%)出现发育异常复发。BE复发的总体发病率为每100人年10.8例(95% CI,7.8 - 15.0);基线为低级别发育异常的患者中为每100人年8.3例(95% CI,4.9 - 14.0),基线为高级别发育异常的患者中为每10只人年13.5例(95% CI 8.8 - 20.7)。发育异常复发的发病率为每100人年5.2例(95% CI 3.3 - 8.2);基线为低级别发育异常的患者中为每100人年3.3例(95% CI 1.5 - 7.2),基线为高级别发育异常的患者中为每100人年7.3例(95% CI 4.2 - 12.5)。BE和发育异常均未以恒定速率复发。CEIM后的第一年复发概率高于接下来4年的总和。
在对AIM发育异常试验的前瞻性队列数据的分析中,我们发现基线有发育异常疾病的患者中,近三分之一在RFA实现CEIM后BE复发;大多数复发发生在CEIM后的第一年。然而,在RFA后1年实现CEIM且无BE的患者BE复发风险较低。需要进行研究以确定何时可以减少或停止监测;我们的研究在4年监测后未发现任何BE或发育异常复发。
