Application of HLA molecular level mismatching in ethnically diverse kidney transplant recipients receiving a steroid-sparing immunosuppression protocol

被引:2
|
作者
Santos, Eva [1 ]
Spensley, Katrina [2 ,3 ]
Gunby, Nicola [1 ]
Worthington, Judith [4 ]
Roufosse, Candice [3 ,5 ]
Anand, Arthi [1 ]
Willicombe, Michelle [2 ,3 ]
机构
[1] Hammersmith Hosp, Histocompatibil & Immunogenet Lab, Northwest London Pathol NHS Trust, London, England
[2] Hammersmith Hosp, Imperial Coll Healthcare NHS Trust, Imperial Coll Renal & Transplant Ctr, London, England
[3] Imperial Coll London, Ctr Inflammatory Dis, Dept Immunol & Inflammat, Hammersmith Campus, London, England
[4] Manchester Royal Infirm, Transplantat Lab, Oxford Rd, Manchester, England
[5] Charing Cross Hosp, Dept Histopathol, Northwest London Pathol NHS Trust, London, England
关键词
molecular mismatch; epitopes; de novo donor specific antibodies; ethnicity; kidney transplant outcomes; steroid sparing; ANTIBODIES; REJECTION; LOAD;
D O I
10.1016/j.ajt.2024.02.019
中图分类号
R61 [外科手术学];
学科分类号
摘要
Defining HLA mismatch at the molecular compared with the antigen level has been shown to be superior in predicting alloimmune responses, although data from across different patient populations are lacking. Using HLA-Matchmaker, HLA-EMMA and PIRCHE-II, this study reports on the association between molecular mismatch (MolMM) and de novo donorspecific antibody (dnDSA) in an ethnically diverse kidney transplant population receiving a steroid-sparing immunosuppression protocol. Of the 419 patients, 51 (12.2%) patients had dnDSA. De novo DSA were seen more frequently with males, primary transplants, patients receiving tacrolimus monotherapy, and unfavorably HLA-matched transplants. There was a strong correlation between MolMM load and antigen mismatch, although significant variation of MolMM load existed at each antigen mismatch. MolMM loads differed significantly by recipient ethnicity, although ethnicity alone was not associated with dnDSA. On multivariate analysis, increasing MolMM loads associated with dnDSA, whereas antigen mismatch did not. De novo DSA against 8 specific epitopes occurred at high frequency; of the 51 patients, 47 (92.1%) patients with dnDSA underwent a pretreatment biopsy, with 21 (44.7%) having evidence of alloimmune injury. MolMM has higher specificity than antigen mismatching at identifying recipients who are at low risk of dnDSA while receiving minimalist immunosuppression. Immunogenicity consideration is important, with more work needed on identification, especially across different ethnic groups.
引用
收藏
页码:1218 / 1232
页数:15
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