Real-Life Data on the Efficacy and Safety of Letermovir for Primary Prophylaxis of Cytomegalovirus in Allogeneic Hematopoietic Stem Cell Recipients: A Single-Center Analysis

Real-Life Data on the Efficacy and Safety of Letermovir for Primary Prophylaxis of Cytomegalovirus in Allogeneic Hematopoietic Stem Cell Recipients: A Single-Center Analysis [Turk J Hematol]

Turk J Hematol. 2024; 41(1): 9-15 | DOI: 10.4274/tjh.galenos.2024.2024.0026

Real-Life Data on the Efficacy and Safety of Letermovir for Primary Prophylaxis of Cytomegalovirus in Allogeneic Hematopoietic Stem Cell Recipients: A Single-Center Analysis

Martyna Wlodarczyk, Agata Wieczorkiewicz Kabut, Krzysztof Bialas, Anna Koclega, Izabela Noster, Patrycja Zielinska, Grzegorz Helbig
Medical University of Silesia, Faculty of Medicine in Katowice, Department of Hematology and Bone Marrow Transplantation, Katowice, Poland

Objective: Cytomegalovirus (CMV) reactivation is a life-threatening complication after allogeneic hematopoietic stem cell transplantation (HSCT). Introduction of letermovir (LMV) seems to improve posttransplant outcomes, but delayed-onset CMV reactivation still remains a challenge. In this study, we report on our first experience with LMV prophylaxis in 93 CMV-seropositive adult patients receiving HSCT in our center.
Materials and Methods: We retrospectively analyzed the data of 93 adult CMV-seropositive recipients receiving LMV as CMV prophylaxis after HSCT for hematological malignancies between 2019 and 2023. The starting LMV dose was 480 mg daily, reduced to 240 mg daily for those receiving cyclosporin A co-administration. CMV DNA in the blood was measured by real-time polymerase chain reaction weekly for the first 2 months after transplantation, then every other week until the end of immunosuppressive treatment. LMV was continued to day +100 or to CMV reactivation.
Results: The median recipient age at the time of transplant was 51 (range: 20-71) years. All patients received grafts from peripheral blood, mostly for acute myeloid leukemia (60%). The median time from transplantation to LMV initiation was 3 (range: 0-24) days. While 55% of patients were transplanted from matched related donors, 32% had unrelated donors and 13% underwent haploidentical HSCT. Four patients (4%) had CMV �blips� while on LMV, but the drug was continued and repeated assays were negative. Only 2 patients (2%) experienced CMV reactivation while on LMV, on days 48 and 34 after HSCT, respectively. Seven patients (7%) developed late-onset CMV reactivation after a median of 124 days after HSCT (range: 118- 152 days) and they were successfully treated with ganciclovir. CMV disease was not observed. Grade III-IV acute graft-versus-host disease occurred in 6 patients (6%) during LMV treatment. LMV treatment was free of side effects.
Conclusion: The median recipient age at the time of transplant was 51 (range: 20-71) years. All patients received grafts from peripheral blood, mostly for acute myeloid leukemia (60%). The median time from transplantation to LMV initiation was 3 (range: 0-24) days. While 55% of patients were transplanted from matched related donors, 32% had unrelated donors and 13% underwent haploidentical HSCT. Four patients (4%) had CMV �blips� while on LMV, but the drug was continued and repeated assays were negative. Only 2 patients (2%) experienced CMV reactivation while on LMV, on days 48 and 34 after HSCT, respectively. Seven patients (7%) developed late-onset CMV reactivation after a median of 124 days after HSCT (range: 118- 152 days) and they were successfully treated with ganciclovir. CMV disease was not observed. Grade III-IV acute graft-versus-host disease occurred in 6 patients (6%) during LMV treatment. LMV treatment was free of side effects.

Keywords: Allogeneic hematopoietic stem cell transplantation, Antiviral prophylaxis, Cytomegalovirus reactivation, Letermovir

Allojenik Hematopoetik K�k H�cre Al�c�lar�nda Sitomegalovir�s�n Primer Profilaksisi i�in Letermovirin Etkilili�i ve G�venirli�ine �li�kin Ger�ek Ya�am Verileri: Tek Merkezli Bir Analiz

Ama�: Sitomegalovir�s (CMV) reaktivasyonu allojenik hematopoetik k�k h�cre transplantasyonu (HKHT) sonras�nda hayat� tehdit eden bir komplikasyondur. Letermovir (LMV) kullan�m�n�n nakil sonras� sonu�lar� iyile�tirdi�i g�r�lmektedir, ancak gecikmi� ba�lang��l� CMV reaktivasyonu hala bir sorun olmaya devam etmektedir. Bu �al��mada, merkezimizde HKHT olan 93 CMV-seropozitif yeti�kin hastada LMV profilaksisi ile ilgili ilk deneyimimizi bildiriyoruz.
Gere� ve Y�ntem: 2019-2023 y�llar� aras�nda hematolojik maligniteler i�in HKHT sonras� CMV profilaksisi olarak LMV ba�lanan 93 yeti�kin CMV-seropozitif al�c�n�n verilerini retrospektif olarak analiz ettik. Ba�lang�� LMV dozu g�nde 480 mg olup siklosporin A ile birlikte uygulananlar i�in g�nde 240 mg�a d��r�lm��t�r. Kandaki CMV DNA�s� ger�ek zamanl� polimeraz zincir reaksiyonu ile transplantasyondan sonraki ilk 2 ay boyunca haftada bir, daha sonra imm�nosupresif tedavinin sonuna kadar iki haftada bir �l��lm��t�r. LMV profilaksisi +100. g�ne kadar veya CMV reaktivasyonuna kadar devam ettirilmi�tir.
Bulgular: Nakil s�ras�ndaki ortanca al�c� ya�� 51 (aral�k: 20-71) idi. T�m hastalar, �o�unlukla miyeloid akut l�semi (%60) nedeniyle periferik kandan nakil yap�lm��t�r. Transplantasyondan LMV ba�lang�c�na kadar ge�en medyan s�re 3 (aral�k: 0-24) g�nd�. Hastalar�n %55�ine doku tipi uyumlu akraba vericilerden nakil yap�l�rken, %32�sine akraba olmayan vericiler ve %13��ne haploidentik HKHT uygulanm��t�r. D�rt hastada (%4) LMV kullan�rken CMV �blips� g�r�ld�, ancak ilaca devam edildi ve tekrarlanan testler negatif ��kt�. Sadece 2 hastada (%2) LMV kullan�rken, s�ras�yla HKHT�den sonraki 34. ve 48. g�nlerde CMV reaktivasyonu g�r�lm��t�r. Yedi hastada (%7) HKHT�den ortanca 124 g�n sonra (aral�k: 118-152 g�n) ge� ba�lang��l� CMV reaktivasyonu geli�mi� ve bu hastalar gansiklovir ile ba�ar�l� bir �ekilde tedavi edilmi�tir. Bu hastalarda CMV hastal�� g�zlenmemi�tir. LMV tedavisi s�ras�nda 6 hastada (%6) grade III-IV akut graft-versus-host hastal�� meydana gelmi�tir. LMV tedavisi boyunca yan etki g�r�lmemi�tir.
Sonu�: LMV profilaksisi, olumlu bir g�venlik profili ile CMV reaktivasyonunu �nlemede etkili olmu�tur. CMV reaktivasyonu �o�unlukla LMV kesildikten sonra meydana gelmi�tir; bu nedenle profilaksi s�resinin 100 g�n�n �tesine uzat�lmas� faydal� olabilir.

Anahtar Kelimeler: Allojenik hematopoietik k�k h�cre transplantasyonu, Antiviral profilaksi, Sitomegalovir�s reaktivasyonu, Letermovir

Martyna Wlodarczyk, Agata Wieczorkiewicz Kabut, Krzysztof Bialas, Anna Koclega, Izabela Noster, Patrycja Zielinska, Grzegorz Helbig. Real-Life Data on the Efficacy and Safety of Letermovir for Primary Prophylaxis of Cytomegalovirus in Allogeneic Hematopoietic Stem Cell Recipients: A Single-Center Analysis. Turk J Hematol. 2024; 41(1): 9-15

Corresponding Author: Martyna Wlodarczyk

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