Belyayev Leonid, Hawksworth Jason, Khan Khalid, Kaufman Stuart, Subramanian Sukanya, Kroemer Alexander, Loh Katrina, Girlanda Raffaele, Fishbein Thomas M, Matsumoto Cal S
MedStar Georgetown Transplant Institute, MedStar Georgetown University Hospital and the Center for Translational Transplant Medicine, Georgetown University Medical Center, Washington, DC.
Department of Surgery, Walter Reed National Military Medical Center, Bethesda, MD.
Transplant Direct. 2020 May 21;6(6):e556. doi: 10.1097/TXD.0000000000001006. eCollection 2020 Jun.
Despite improved outcomes in the modern era of targeted immunotherapy, intestinal failure and chronic parenteral nutrition remains a significant burden for patients with Crohn's disease (CD) worldwide. Transplantation is a key component of management when a patient with CD suffers from life-threatening complications of parenteral nutrition. Nucleotide-binding oligomerization domain 2 (NOD2) mutation is a risk factor for both development of CD and intestinal allograft rejection.
A retrospective review of a prospectively maintained database of intestinal transplants at a single center from 2003 to 2015 was conducted. Eleven adult patients with CD were identified and were compared with 103 adult control recipients. A sub-analysis was performed comparing the 11 CD recipients to the 13 NOD2 mutant non-CD recipients.
Patient and allograft characteristics were similar between the CD and control recipients. Although overall rejection-free survival was not significantly different, patients with CD suffered from more frequent, earlier, and more severe rejection compared with control patients. The onset, severity, and frequency of rejection was comparable between patients with CD and NOD2 mutant non-CD patients. There was a trend toward lower 5-year allograft survival for CD compared with control recipients (33% versus 63.3%; = 0.19) and NOD2 mutant non-CD recipients (33% versus 57.14%; = 0.41).
Patients with CD remain a challenging population in intestine transplantation, and NOD2 mutant non-CD patients appear to have a similar immunologic phenotype. These high-risk recipients may require specialized immunosuppression protocols and management at experienced transplant centers.
尽管在靶向免疫治疗的现代时代治疗效果有所改善,但肠衰竭和长期肠外营养仍然是全球克罗恩病(CD)患者的重大负担。当CD患者出现危及生命的肠外营养并发症时,移植是治疗的关键组成部分。核苷酸结合寡聚化结构域2(NOD2)突变是CD发生和肠道同种异体移植排斥反应的危险因素。
对2003年至2015年单一中心前瞻性维护的肠道移植数据库进行回顾性分析。确定了11例成年CD患者,并与103例成年对照受者进行比较。进行了一项亚分析,将11例CD受者与13例NOD2突变的非CD受者进行比较。
CD受者和对照受者的患者及移植物特征相似。虽然总体无排斥生存率无显著差异,但与对照患者相比,CD患者排斥反应更频繁、更早且更严重。CD患者和NOD2突变的非CD患者之间排斥反应的发生时间、严重程度和频率相当。与对照受者(33%对63.3%;P = 0.19)和NOD2突变的非CD受者(33%对57.14%;P = 0.41)相比,CD患者5年移植物生存率有降低趋势。
CD患者在肠道移植中仍然是一个具有挑战性的群体,NOD2突变的非CD患者似乎具有相似的免疫表型。这些高危受者可能需要在经验丰富的移植中心采用专门的免疫抑制方案和管理。
