ADAMTS13 recovery in acute thrombotic thrombocytopenic purpura after caplacizumab therapy

被引:11
作者
Mingot-Castellano, Maria-Eva [1 ,2 ]
Garcia-Candel, Faustino [3 ]
Martinez-Nieto, Jorge [4 ]
Garcia-Arroba, Jose [5 ]
de la Rubia-Comos, Javier [6 ]
Gomez-Segui, Ines [6 ]
Paciello-Coronel, Maria-Liz [7 ]
Valcarcel-Ferreiras, David [8 ]
Jimenez, Moraima [8 ]
Cid, Joan [9 ]
Lozano, Miquel [9 ]
Garcia-Gala, Jose-Maria [10 ]
Angos-Vazquez, Sonia [11 ]
Vara-Pampliega, Miriam [12 ]
Guerra-Dominguez, Luisa [13 ]
Avila-Idrobo, Laura-Francisca [14 ]
Oliva-Hernandez, Ana [15 ]
Zalba-Marcos, Saioa [16 ]
Tallon-Ruiz, Inmaculada [17 ]
Ortega-Sanchez, Sandra [18 ]
Goterris-Viciedo, Rosa [19 ]
Moreno-Jimenez, Gemma [20 ]
Dominguez-Acosta, Lourdes [21 ]
Araiz-Ramirez, Maria [22 ]
Hernandez-Mateos, Luis [23 ]
Flores-Ballesteros, Elena [24 ]
del Rio-Garma, Julio [25 ]
Pascual-Izquierdo, Cristina [26 ,27 ]
机构
[1] Hosp Univ Virgen Rocio, Dept Hematol, Seville, Spain
[2] Inst Biomed Sevilla, Seville, Spain
[3] Hosp Univ Virgen Arrixaca, Dept Hematol, Murcia, Spain
[4] Hosp Clin San Carlos, Dept Hematol, Madrid, Spain
[5] Hosp Univ Joan XXIII, Banc Sang & Teixits, Tarragona, Spain
[6] Univ Catolica San Vicente Martir, Hosp Univ La Fe, Dept Hematol, IIS La Fe, Valencia, Spain
[7] Hosp Univ 12 Octubre, Dept Hematol, Madrid, Spain
[8] Hosp Univ Vall Hebron, Dept Hematol, Barcelona, Spain
[9] Hosp Clin Barcelona, Clin Inst Hematol & Oncol Dis, Dept Hemotherapy & Hemostasis, Apheresis & Cellular Therapy Unit,Inst Invest Bio, Barcelona, Spain
[10] Hosp Univ Cent Asturias, Inst Bio Hlth Invest Asturias, Dept Hematol, Oviedo, Spain
[11] Hosp Univ Zaragoza, Dept Hematol, Zaragoza, Spain
[12] Hosp Univ Cruces, Dept Hematol, Baracaldo, Spain
[13] Hosp Univ Dr Negrin, Dept Hematol, Las Palmas Gran Canaria, Spain
[14] Hosp Univ Canarias, Dept Hematol, Tenerife, Spain
[15] Hosp Univ Nuestra Senora Candelaria, Dept Hematol, Tenerife, Spain
[16] Hosp Univ Navarra, Dept Hematol, Pamplona, Spain
[17] Hosp Univ Virgen Macarena, Dept Hematol, Seville, Spain
[18] Banc Sang & Teixits, Barcelona, Spain
[19] Hosp Clin Univ Valencia, Dept Hematol, Valencia, Spain
[20] Hosp Univ Ramon & Cajal, Dept Hematol, Madrid, Spain
[21] Hosp Univ Jerez De La Frontera, Dept Hematol, Jerez de la Frontera, Spain
[22] Hosp Univ Donostia, Dept Hematol, Donostia San Sebastian, Spain
[23] Hosp Gen Univ Alicante, Dept Hematol, Alicante, Spain
[24] Hosp Univ Principe Asturias, Dept Hematol, Alcala De Henares, Madrid, Spain
[25] Complejo Hosp Univ Ourense, Dept Hematol, Orense, Spain
[26] Hosp Gen Univ Gregorio Maranon, Dept Hematol, Madrid, Spain
[27] Inst Invest Gregorio Maranon, Madrid, Spain
关键词
CONSENSUS;
D O I
10.1182/blood.2023022725
中图分类号
R5 [内科学];
学科分类号
1002 ; 100201 ;
摘要
Caplacizumab prevents the interaction between von Willebrand factor and platelets and is used to treat immune thrombotic thrombocytopenic purpura (iTTP). Its administration has been associated with a delay in ADAMTS13 activity restoration after plasma exchange (PEX) suspension. We analyzed the outcomes of 113 iTTP episodes, 75 of which were treated with caplacizumab, in 108 patients from the Spanish Registry of Thrombotic Thrombocytopenic Purpura. Caplacizumab shortened the time to platelet count normalization and reduced PEX requirement, exacerbations, and relapses. There was no difference in the time to achieve ADAMTS13 activity >= 20% after PEX end between caplacizumabtreated and nontreated episodes (median [interquartile range], 14.5 [7.7-27.2] vs 13.0 [8.0-29.0] days, P = .653). However, considering the 36 episodes in which caplacizumab was started <= 3 days after iTTP diagnosis, the time for ADAMTS13 restoration from PEX end was higher than in those episodes in which caplacizumab was started >3 days after iTTP diagnosis (20.0 [12.0-43.0] vs 11.0 [3.5-20.0] days, P = .003) or than in non-caplacizumab-treated episodes (P P = .033). This fi nding could be related to a significantly fi cantly shorter duration of PEX in early caplacizumab-treated episodes than in late caplacizumab-treated episodes (5.5 [4.0-9.0] vs 15.0 [11.0-21.5] days, P < .001) or noncaplacizumab-treated episodes (11.0 [6.0-26.0] days, P < .001). There were no differences in time to ADAMTS-13 restoration from PEX start (28.0 [17.2-47.5], 27.0 [19.0-37.5] and 29.5 [15.2-45.0] days in early caplacizumab-treated, late caplacizumab-treated and non-caplacizumab-treated episodes). Early administered caplacizumab does not prevent the requirement for immunosuppression but has beneficial fi cial effects by shortening PEX requirement without major safety concerns.
引用
收藏
页码:1807 / 1815
页数:9
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