Factors associated with rituximab-mediated B cell depletion in ABO-incompatible adult living donor liver transplantation.

Q4 Medicine Korean Journal of Transplantation Pub Date : 2023-09-30 Epub Date: 2023-09-11 DOI:10.4285/kjt.23.0031
Suk Kyun Hong, Kwang-Woong Lee, Jae-Yoon Kim, Jaewon Lee, Jiyoung Kim, Hyun Hwa Choi, Su Young Hong, Jeong-Moo Lee, YoungRok Choi, Nam-Joon Yi, Kyung-Suk Suh
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Abstract

Background: Pretransplant therapies such as rituximab and plasmapheresis have led to an increase in ABO-incompatible (ABOi) living donor liver transplantation (LDLT), thus helping to overcome organ shortages. This study evaluated the changes in anti-A/B titers and CD19 levels over time in patients undergoing ABOi LT and aimed to understand the effect of single-nucleotide polymorphisms (SNPs) in Fc gamma receptor (FcγR) on rituximab therapy.

Methods: Two SNPs of FCGR2A (131H/R) and FCGR3A (158F/V) were identified. The clinical data on 44 patients who underwent ABOi LDLT between May 2019 and October 2021 at Seoul National University Hospital were reviewed retrospectively.

Results: Following desensitization with rituximab and subsequent LDLT, the anti-A/B titer recovered within 1 week, but decreased thereafter. The CD19 level increased at 3 months after LT. The genotyping data for FCGR3A (158F/V) indicated that two patients had the V/V genotype, and 42 had the F/V genotype. In the genotyping data for FCGR2A (131H/R), 21 patients had the H/H genotype, three had the R/R genotype, and 20 had the H/R genotype. However, there were no significant differences in anti-A/B and CD19 levels, bacteremia rates, T cell-mediated rejection, antibody-mediated rejection, or the survival rate among the FCGR2A types.

Conclusions: There were significant changes in the anti-A/B titers and CD19 levels over time in each patient after ABOi LDLT. The difference in outcomes following LT according to the FcγR SNP type for rituximab was unclear. Further studies with larger sample sizes are needed to confirm the effect of FcγR SNPs on rituximab therapy.

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ABO血型不合成人活体肝移植中利妥昔单抗介导的B细胞耗竭的相关因素。
背景:利妥昔单抗和血浆置换等移植前治疗导致ABO血型不合(ABOi)活体供肝移植(LDLT)的增加,从而有助于克服器官短缺。本研究评估了ABOi LT患者抗A/B滴度和CD19水平随时间的变化,旨在了解Fcγ受体(FcγR)单核苷酸多态性(SNPs)对利妥昔单抗治疗的影响。方法:鉴定FCGR2A(131H/R)和FCGR3A(158F/V)两个SNPs。回顾性回顾了2019年5月至2021年10月在首尔国立大学医院接受ABOi-LDLT的44名患者的临床数据。结果:利妥昔单抗脱敏和随后的LDLT后,抗A/B滴度在1周内恢复,但此后下降。LT后3个月CD19水平升高。FCGR3A(158F/V)的基因分型数据表明,两名患者具有V/V基因型,42名患者具有F/V基因型。在FCGR2A(131H/R)的基因分型数据中,21例患者具有H/H基因型,3例具有R/R基因型,20例具有H/R基因型。然而,在FCGR2A类型之间,抗A/B和CD19水平、菌血症率、T细胞介导的排斥反应、抗体介导的拒绝反应或存活率没有显著差异。结论:ABOi-LDLT后,每个患者的抗A/B滴度和CD19水平都随时间发生了显著变化。根据利妥昔单抗FcγR SNP类型,LT后的结果差异尚不清楚。需要对更大样本量的进一步研究来证实FcγR SNPs对利妥昔单抗治疗的影响。
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来源期刊
Korean Journal of Transplantation
Korean Journal of Transplantation Medicine-Transplantation
CiteScore
0.80
自引率
0.00%
发文量
32
审稿时长
24 weeks
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