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ABO incompatible living donor liver transplant with antibody titer of 1:4: First case report from Pakistan

INTRODUCTION AND IMPORTANCE: The most common reason for live liver donor rejection is ABO incompatibility. With breaching this incompatibility barrier, probably an additional 25%–35% of liver transplantation (LT) procedures would become possible. Also, ABOi-LT can be lifesaving in acute settings. In...

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Autores principales: Dogar, Abdul Wahab, Ullah, Kaleem, Bilal, Hafiz, Sarwar, Muhammad Shahzad, Uddin, Shams, Ochani, Sidhant, Abbas, Syed Hasnain
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Elsevier 2022
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9486708/
https://www.ncbi.nlm.nih.gov/pubmed/36147097
http://dx.doi.org/10.1016/j.amsu.2022.104463
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author Dogar, Abdul Wahab
Ullah, Kaleem
Bilal, Hafiz
Sarwar, Muhammad Shahzad
Uddin, Shams
Ochani, Sidhant
Abbas, Syed Hasnain
author_facet Dogar, Abdul Wahab
Ullah, Kaleem
Bilal, Hafiz
Sarwar, Muhammad Shahzad
Uddin, Shams
Ochani, Sidhant
Abbas, Syed Hasnain
author_sort Dogar, Abdul Wahab
collection PubMed
description INTRODUCTION AND IMPORTANCE: The most common reason for live liver donor rejection is ABO incompatibility. With breaching this incompatibility barrier, probably an additional 25%–35% of liver transplantation (LT) procedures would become possible. Also, ABOi-LT can be lifesaving in acute settings. Initially, ABOi-LT reported a poor prognosis secondary to antibody-mediated rejection (AMR) which is more common in ABOi allograft recipients. AMR may be avoided by desensitization. Various desensitization protocols are practiced globally, however, there is no consensus available on the optimal desensitization protocol for the ABOi-LT. The ABO-incompatible (ABOi) can expand the liver donor pool tremendously. We report the first case of ABO incompatible-liver transplantation (ABOi-LT) from Pakistan. CASE PRESENTATION: A 48 years old male, presented with decompensated liver diseaseand hepatocellular carcinoma secondary to HCV infection. LT was advised as the optimal modality of treatment. Due to the non-availability of a compatible donor, ABOi-LT was planned.His daughter agreed to donate.Pre-LT desensitization was started on the 23rd-day pre-LT with intravenous (I/V) rituximab 700 mg/body (375 mg/m(2)) along with I/V Bortezomib 2mg (1.3 mg/m(2)). Bortezomib was repeated subcutaneously (S/C) on the 20th, 16th, and 13th days pre-LT. One week before LT oral Mycophenolate mofetil 500 mg and Tacrolimus 1 mg were started twice daily. Therapeutic plasmapheresis was done on the 5th, 3rd, and 1st-day pre-LT. Per-operatively, Basiliximab was administeredI/V with a dose of 0.8 gm/kg during the anhepatic phase. Anti-A & Anti-B titer level was determined on the 5th day before plasmapheresis and repeated on the 2nd and 1st-day pre-LT. Then post-LT plasmapheresis was done onthe 15th day and at 3 months. The CD 19 activity was determined one day before LT and on the 15th-day post-LT. His LT was performed uneventfully and was discharged on the 15th postoperative day (POD). However, on the 26th POD, he was diagnosed with left subclavian vein thrombosis which was treated successfully with anticoagulation therapy for 6 months. Till the last follow up patient is doing well. CLINICAL DISCUSSION: Desensitization is the removal of preformed anti-ABO antibodies and depleting serum B cells production. Antibody-mediated rejection irreversibly damages the graft and predisposes it to graft failure. The prognosis of ABOi-LT has dramatically improved since the introduction of desensitization protocols. CONCLUSION: Antibody-mediated rejection may be avoided by desensitization. The intravascular infusion therapies and splenectomy can be omitted from the desensitization protocol. ABO-i LT can tremendously increase the liver donor pool.
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spelling pubmed-94867082022-09-21 ABO incompatible living donor liver transplant with antibody titer of 1:4: First case report from Pakistan Dogar, Abdul Wahab Ullah, Kaleem Bilal, Hafiz Sarwar, Muhammad Shahzad Uddin, Shams Ochani, Sidhant Abbas, Syed Hasnain Ann Med Surg (Lond) Case Report INTRODUCTION AND IMPORTANCE: The most common reason for live liver donor rejection is ABO incompatibility. With breaching this incompatibility barrier, probably an additional 25%–35% of liver transplantation (LT) procedures would become possible. Also, ABOi-LT can be lifesaving in acute settings. Initially, ABOi-LT reported a poor prognosis secondary to antibody-mediated rejection (AMR) which is more common in ABOi allograft recipients. AMR may be avoided by desensitization. Various desensitization protocols are practiced globally, however, there is no consensus available on the optimal desensitization protocol for the ABOi-LT. The ABO-incompatible (ABOi) can expand the liver donor pool tremendously. We report the first case of ABO incompatible-liver transplantation (ABOi-LT) from Pakistan. CASE PRESENTATION: A 48 years old male, presented with decompensated liver diseaseand hepatocellular carcinoma secondary to HCV infection. LT was advised as the optimal modality of treatment. Due to the non-availability of a compatible donor, ABOi-LT was planned.His daughter agreed to donate.Pre-LT desensitization was started on the 23rd-day pre-LT with intravenous (I/V) rituximab 700 mg/body (375 mg/m(2)) along with I/V Bortezomib 2mg (1.3 mg/m(2)). Bortezomib was repeated subcutaneously (S/C) on the 20th, 16th, and 13th days pre-LT. One week before LT oral Mycophenolate mofetil 500 mg and Tacrolimus 1 mg were started twice daily. Therapeutic plasmapheresis was done on the 5th, 3rd, and 1st-day pre-LT. Per-operatively, Basiliximab was administeredI/V with a dose of 0.8 gm/kg during the anhepatic phase. Anti-A & Anti-B titer level was determined on the 5th day before plasmapheresis and repeated on the 2nd and 1st-day pre-LT. Then post-LT plasmapheresis was done onthe 15th day and at 3 months. The CD 19 activity was determined one day before LT and on the 15th-day post-LT. His LT was performed uneventfully and was discharged on the 15th postoperative day (POD). However, on the 26th POD, he was diagnosed with left subclavian vein thrombosis which was treated successfully with anticoagulation therapy for 6 months. Till the last follow up patient is doing well. CLINICAL DISCUSSION: Desensitization is the removal of preformed anti-ABO antibodies and depleting serum B cells production. Antibody-mediated rejection irreversibly damages the graft and predisposes it to graft failure. The prognosis of ABOi-LT has dramatically improved since the introduction of desensitization protocols. CONCLUSION: Antibody-mediated rejection may be avoided by desensitization. The intravascular infusion therapies and splenectomy can be omitted from the desensitization protocol. ABO-i LT can tremendously increase the liver donor pool. Elsevier 2022-08-19 /pmc/articles/PMC9486708/ /pubmed/36147097 http://dx.doi.org/10.1016/j.amsu.2022.104463 Text en © 2022 The Authors https://creativecommons.org/licenses/by/4.0/This is an open access article under the CC BY license (http://creativecommons.org/licenses/by/4.0/).
spellingShingle Case Report
Dogar, Abdul Wahab
Ullah, Kaleem
Bilal, Hafiz
Sarwar, Muhammad Shahzad
Uddin, Shams
Ochani, Sidhant
Abbas, Syed Hasnain
ABO incompatible living donor liver transplant with antibody titer of 1:4: First case report from Pakistan
title ABO incompatible living donor liver transplant with antibody titer of 1:4: First case report from Pakistan
title_full ABO incompatible living donor liver transplant with antibody titer of 1:4: First case report from Pakistan
title_fullStr ABO incompatible living donor liver transplant with antibody titer of 1:4: First case report from Pakistan
title_full_unstemmed ABO incompatible living donor liver transplant with antibody titer of 1:4: First case report from Pakistan
title_short ABO incompatible living donor liver transplant with antibody titer of 1:4: First case report from Pakistan
title_sort abo incompatible living donor liver transplant with antibody titer of 1:4: first case report from pakistan
topic Case Report
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9486708/
https://www.ncbi.nlm.nih.gov/pubmed/36147097
http://dx.doi.org/10.1016/j.amsu.2022.104463
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