AI Article Synopsis
- ABO incompatible kidney transplantation (ABOi-KT) was once deemed too risky for end-stage kidney disease patients due to the high rejection rates, but its success has grown, expanding donor options and reducing wait times for deceased donors.
- Advances in immunosuppression and better understanding of immunology have improved desensitization protocols, making ABOi-KT outcomes comparable to traditional ABO compatible transplants.
- Despite these improvements, challenges remain, such as increased costs, lingering immunological risks, and potential health implications, prompting ongoing discussions about the future role of ABOi-KT in kidney transplantation.
Article Abstract
ABO incompatible kidney transplantation (ABOi-KT) was previously considered to be an absolute contraindication for patients with end-stage kidney disease (ESKD) due to hyperacute rejection related to blood type barrier. Since the first successful series of ABOi-KT was reported, ABOi-KT is performed increasingly all over the world. ABOi-KT has led to an expanded donor pool and reduced the number of patients with ESKD awaiting deceased kidney transplantation (KT). Intensified immunosuppression and immunological understanding has helped to shape current desensitization protocols. Consequently, in recent years, ABOi-KT outcome is comparable to ABO compatible KT (ABOc-KT). However, many questions still remain unanswered. In ABOi-KT, there is an additional residual immunological risk that may lead to allograft damage, despite using current diverse but usually intensified immunosuppressive protocols at the expense of increasing risk of infection and possibly malignancy. Notably, in ABOi-KT, desensitization and antibody reduction therapies have increased the cost of KT. Reassuringly, there has been an evolution in ABOi-KT leading to a simplification of protocols over the last decade. This review provides an overview of the history, outcome, protocol, advantages and disadvantages in ABOi-KT, and focuses on whether ABOi-KT should be recommended as a therapeutic option of KT in the future.
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| http://www.ncbi.nlm.nih.gov/pmc/articles/PMC3964193 | PMC |
| http://dx.doi.org/10.5500/wjt.v4.i1.18 | DOI Listing |
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