Paroxysmal Nocturnal Hemoglobinuria is an acquired clonal hematopoietic stem cell disorder that can present with hemolytic anaemia, thrombosis and aplastic anaemia. There are different therapeutic approaches for PNH which do not cure the disease but can decrease its complications. Allogeneic bone marrow transplantation (BMT) can cure PNH [1] especially for younger PNH patients with aplastic phenotype [2].
37 yrs – old male patient presented with jaundice and passing cola colored urine. His blood parameters show Hb-6.5, WBC 6400, platelet count 2.6 lakhs, MCV-115, bilirubin-3.0, LDH-4980, Coombs test negative, Urine hemosiderin positive. Bone marrow showed marked Erythroid hyperplasia, PNH screen positive of 56% (CD55, CD59).
He received multiple transfusions and trial of steroids with no benefit. He developed shortness of breath on exertion despite maintaining haemoglobin more than 10 g/dl. His Echocardiogram showed normal LV function. His pulmonary function tests revealed restrictive lung disease. He had high BNP (Brain natriuretic peptide) likely due to pulmonary hypertension with ongoing haemolysis, however, pulmonary pressures were not measured. He had options of Eculizumab and Bone marrow transplant. In view of cost, he chose to go with the Bone marrow transplant. Androgen therapy and Immuno suppressants can be tried [3] in the early part of diagnosis which is not offered in view of the failure to respond to steroids and pulmonary hypertension.
He had fully matched 10/10 Sibling Allogenic Hematopoietic Stem Cell Transplant with Fludarabine, Busulfan and ATG Conditioning. During conditioning chemotherapy, he had further rise in BNP to 5430 and had ST-T ischemic changes. Managed conservatively.
Neutrophil engraftment occurred on day 12 and platelet engraftment on day 14. Patient discharged on day 18 post-transplant. He attained complete morphological recovery by day 20 and not needed any transfusions posttransplant. He continued immunosuppression with cyclosporine for 3 months maintaining target therapeutic levels between 100-200. He had not experienced any GVHD. Additional antimicrobial prophylaxis included acyclovir and septran for 1 year.
Post-transplant assessment after 30 days he had 100% donor chimerism and his PNH clone is RBC of 5-7%. After 6 months’ flow cytometry was negative for PNH clone in all three cell lines with Hb-13.0, LDH-239. His Pulmonary functions, Echocardiogram was noted to be normal. After one year of HSCT patient quality of life was improved without any symptoms with negative PNH clone.
Overall survival was 70% in matched unrelated donor allogenic bone marrow transplant among patients with paroxysmal nocturnal hemoglobinuria previously treated with eculizumab from a retrospective study of 21 patients from SFGM-TC centers [4].
We conclude Sibling allogeneic bone marrow transplant is a relatively safe and cost-effective alternative upfront treatment for transfusion-dependent classical PNH patients who can not afford Eculizumab treatment.