Eintrag weiter verarbeiten
Verfügbar über Online-Ressource

PB1867 USE OF THERAPY WITH COMPLEMENT INHIBITOR AND THROMBOPOIETIN RECEPTOR AGONISTS IN TREATMENT OF PATIENT WITH SAA/PNH. CLINICAL CASE.

Gespeichert in:

Bibliographische Detailangaben
Zeitschriftentitel: HemaSphere
Personen und Körperschaften: Shilova, E., Glazanova, T., Chubukina, Z., Zenina, M., Romanenko, N., Khorsheva, I., Voloshin, S.
In: HemaSphere, 3, 2019, S1, S. 850-851
Format: E-Article
Sprache: Englisch
veröffentlicht:
Wiley
Schlagwörter:
Hematology
author_facet Shilova, E.
Glazanova, T.
Chubukina, Z.
Zenina, M.
Romanenko, N.
Khorsheva, I.
Voloshin, S.
Shilova, E.
Glazanova, T.
Chubukina, Z.
Zenina, M.
Romanenko, N.
Khorsheva, I.
Voloshin, S.
author Shilova, E.
Glazanova, T.
Chubukina, Z.
Zenina, M.
Romanenko, N.
Khorsheva, I.
Voloshin, S.
spellingShingle Shilova, E.
Glazanova, T.
Chubukina, Z.
Zenina, M.
Romanenko, N.
Khorsheva, I.
Voloshin, S.
HemaSphere
PB1867 USE OF THERAPY WITH COMPLEMENT INHIBITOR AND THROMBOPOIETIN RECEPTOR AGONISTS IN TREATMENT OF PATIENT WITH SAA/PNH. CLINICAL CASE.
Hematology
author_sort shilova, e.
spelling Shilova, E. Glazanova, T. Chubukina, Z. Zenina, M. Romanenko, N. Khorsheva, I. Voloshin, S. 2572-9241 2572-9241 Wiley Hematology http://dx.doi.org/10.1097/01.hs9.0000565972.20744.8e <jats:sec><jats:title>Background:</jats:title><jats:p>Aplastic anemia (AA) is severe blood system disease, in which more than half of patients may have PNH clone, and there may occur associated variants AA with PNH (AA/PNH). The most frequently observed is the development of classical hemolytic PNH at AA remission, but possibly a combination of the two diseases. For such cases, there is a positive experience of AA combined treatment with immunosupressive therapy (IST) and targeted therapy using complement activation inhibitors. With resistant AA a therapeutic optionis possible using thrombopoietin receptor agonists.</jats:p></jats:sec><jats:sec><jats:title>Aims:</jats:title><jats:p>To treat of patient with SAA/PNH in absence of possibility of full use of IST</jats:p></jats:sec><jats:sec><jats:title>Methods:</jats:title><jats:p>A clinical observation of a 53‐year‐old female with AA/PNH in the course of the disease is presented. Since 1994 patient, aged 53 yrs, has been under our supervision. The diagnosis was established according to a comprehensive examination, with severity determination in accordance to international criteria. The examination used morphological, histological, immunological (including highly sensitive flow cytometry), biochemical methods. No compatible donor for bone marrow transplantation was found. Anti‐lymphocyte globulin (ALG), cyclosporin‐A (CyA), Eculizumab and thrombopoietin receptor agonists were used in treatment.</jats:p></jats:sec><jats:sec><jats:title>Results:</jats:title><jats:p>ALG and cyclosporine treatment gave only a temporary effect – an improvement in hemogram parameters and a reduction in transfusion dependence. CyA doses were reduced (about 3 mg per day) due to adverse effects. The possibilities of active IST were also limited by comorbidities, including chronic hepatitis B. Since 1999, signs of chronic intravascular hemolysis and hemolytic crises have been observed. Flow cytometry have detected PNH clone. Subsequently, according to ICNN protocol testing data, from 2011 to the present, the clone size was determined 96‐99% with a predominance of type III erythrocytes. According to repeated bone marrow assessments, severe aplasia with pancytopenia in the peripheral blood was maintained. Anemia persisted up to 65 g/dL with transfusion dependence (up to 12‐16 doses of red blood cells per year), leukopenia within 0.9‐1.5 x10<jats:sup>9</jats:sup>/l and thrombocytopenia 5‐15 x10<jats:sup>9</jats:sup>/l with cutaneous hemorrhagic syndrome. On 2013, after vaccination with meningococcal vaccine, Eculizumab treatment was started according to the standard scheme with achievement of an adequate control of hemolysis. Clinical manifestations of hemolysis are absent; the level of LDH does not exceed 1.5 ULN. Therapy continues to the present. Until 2015, CyA therapy was periodically resumed due to the persistence of SAA criteria. In 2013‐2015 the patient additionally received thrombopoetin agonist therapy: Romiplostimum (4‐6 ug/kg once a week) with breaks every 3‐4 months. Two months after the start of therapy, a clinical effect was obtained – a decrease in hemorrhagic syndrome. After 3 months, there was a trend towards an increase in platelet levels. At present, severe leukopenia (1.0 – 2.2 x10<jats:sup>9</jats:sup>/l) and neutropenia (0.5‐0.7x10<jats:sup>9</jats:sup>/l) persist. At the same time, the platelet level is 30‐70 x10<jats:sup>9</jats:sup>/l without spontaneous hemorrhages, since January 2018 the patient does not receive blood transfusions and hemoglobin stays at 10.2‐11.0 g/dL. Also there has been a significant improvement in the quality of life.</jats:p></jats:sec><jats:sec><jats:title>Summary/Conclusion:</jats:title><jats:p>This case demonstrates the possibility of a significant improvement in the course of sAA/PNH (including quality of life) in the absence of a sufficient effect of IST, but adequate target control of hemolysis and the use of thrombopoietin receptor agonists.</jats:p></jats:sec> PB1867 USE OF THERAPY WITH COMPLEMENT INHIBITOR AND THROMBOPOIETIN RECEPTOR AGONISTS IN TREATMENT OF PATIENT WITH SAA/PNH. CLINICAL CASE. HemaSphere
doi_str_mv 10.1097/01.hs9.0000565972.20744.8e
facet_avail Online
Free
finc_class_facet Medizin
format ElectronicArticle
fullrecord blob:ai-49-aHR0cDovL2R4LmRvaS5vcmcvMTAuMTA5Ny8wMS5oczkuMDAwMDU2NTk3Mi4yMDc0NC44ZQ
id ai-49-aHR0cDovL2R4LmRvaS5vcmcvMTAuMTA5Ny8wMS5oczkuMDAwMDU2NTk3Mi4yMDc0NC44ZQ
institution DE-L229
DE-D275
DE-Bn3
DE-Brt1
DE-Zwi2
DE-D161
DE-Gla1
DE-Zi4
DE-15
DE-Pl11
DE-Rs1
DE-105
DE-14
DE-Ch1
imprint Wiley, 2019
imprint_str_mv Wiley, 2019
issn 2572-9241
issn_str_mv 2572-9241
language English
mega_collection Wiley (CrossRef)
match_str shilova2019pb1867useoftherapywithcomplementinhibitorandthrombopoietinreceptoragonistsintreatmentofpatientwithsaapnhclinicalcase
publishDateSort 2019
publisher Wiley
recordtype ai
record_format ai
series HemaSphere
source_id 49
title PB1867 USE OF THERAPY WITH COMPLEMENT INHIBITOR AND THROMBOPOIETIN RECEPTOR AGONISTS IN TREATMENT OF PATIENT WITH SAA/PNH. CLINICAL CASE.
title_unstemmed PB1867 USE OF THERAPY WITH COMPLEMENT INHIBITOR AND THROMBOPOIETIN RECEPTOR AGONISTS IN TREATMENT OF PATIENT WITH SAA/PNH. CLINICAL CASE.
title_full PB1867 USE OF THERAPY WITH COMPLEMENT INHIBITOR AND THROMBOPOIETIN RECEPTOR AGONISTS IN TREATMENT OF PATIENT WITH SAA/PNH. CLINICAL CASE.
title_fullStr PB1867 USE OF THERAPY WITH COMPLEMENT INHIBITOR AND THROMBOPOIETIN RECEPTOR AGONISTS IN TREATMENT OF PATIENT WITH SAA/PNH. CLINICAL CASE.
title_full_unstemmed PB1867 USE OF THERAPY WITH COMPLEMENT INHIBITOR AND THROMBOPOIETIN RECEPTOR AGONISTS IN TREATMENT OF PATIENT WITH SAA/PNH. CLINICAL CASE.
title_short PB1867 USE OF THERAPY WITH COMPLEMENT INHIBITOR AND THROMBOPOIETIN RECEPTOR AGONISTS IN TREATMENT OF PATIENT WITH SAA/PNH. CLINICAL CASE.
title_sort pb1867 use of therapy with complement inhibitor and thrombopoietin receptor agonists in treatment of patient with saa/pnh. clinical case.
topic Hematology
url http://dx.doi.org/10.1097/01.hs9.0000565972.20744.8e
publishDate 2019
physical 850-851
description <jats:sec><jats:title>Background:</jats:title><jats:p>Aplastic anemia (AA) is severe blood system disease, in which more than half of patients may have PNH clone, and there may occur associated variants AA with PNH (AA/PNH). The most frequently observed is the development of classical hemolytic PNH at AA remission, but possibly a combination of the two diseases. For such cases, there is a positive experience of AA combined treatment with immunosupressive therapy (IST) and targeted therapy using complement activation inhibitors. With resistant AA a therapeutic optionis possible using thrombopoietin receptor agonists.</jats:p></jats:sec><jats:sec><jats:title>Aims:</jats:title><jats:p>To treat of patient with SAA/PNH in absence of possibility of full use of IST</jats:p></jats:sec><jats:sec><jats:title>Methods:</jats:title><jats:p>A clinical observation of a 53‐year‐old female with AA/PNH in the course of the disease is presented. Since 1994 patient, aged 53 yrs, has been under our supervision. The diagnosis was established according to a comprehensive examination, with severity determination in accordance to international criteria. The examination used morphological, histological, immunological (including highly sensitive flow cytometry), biochemical methods. No compatible donor for bone marrow transplantation was found. Anti‐lymphocyte globulin (ALG), cyclosporin‐A (CyA), Eculizumab and thrombopoietin receptor agonists were used in treatment.</jats:p></jats:sec><jats:sec><jats:title>Results:</jats:title><jats:p>ALG and cyclosporine treatment gave only a temporary effect – an improvement in hemogram parameters and a reduction in transfusion dependence. CyA doses were reduced (about 3 mg per day) due to adverse effects. The possibilities of active IST were also limited by comorbidities, including chronic hepatitis B. Since 1999, signs of chronic intravascular hemolysis and hemolytic crises have been observed. Flow cytometry have detected PNH clone. Subsequently, according to ICNN protocol testing data, from 2011 to the present, the clone size was determined 96‐99% with a predominance of type III erythrocytes. According to repeated bone marrow assessments, severe aplasia with pancytopenia in the peripheral blood was maintained. Anemia persisted up to 65 g/dL with transfusion dependence (up to 12‐16 doses of red blood cells per year), leukopenia within 0.9‐1.5 x10<jats:sup>9</jats:sup>/l and thrombocytopenia 5‐15 x10<jats:sup>9</jats:sup>/l with cutaneous hemorrhagic syndrome. On 2013, after vaccination with meningococcal vaccine, Eculizumab treatment was started according to the standard scheme with achievement of an adequate control of hemolysis. Clinical manifestations of hemolysis are absent; the level of LDH does not exceed 1.5 ULN. Therapy continues to the present. Until 2015, CyA therapy was periodically resumed due to the persistence of SAA criteria. In 2013‐2015 the patient additionally received thrombopoetin agonist therapy: Romiplostimum (4‐6 ug/kg once a week) with breaks every 3‐4 months. Two months after the start of therapy, a clinical effect was obtained – a decrease in hemorrhagic syndrome. After 3 months, there was a trend towards an increase in platelet levels. At present, severe leukopenia (1.0 – 2.2 x10<jats:sup>9</jats:sup>/l) and neutropenia (0.5‐0.7x10<jats:sup>9</jats:sup>/l) persist. At the same time, the platelet level is 30‐70 x10<jats:sup>9</jats:sup>/l without spontaneous hemorrhages, since January 2018 the patient does not receive blood transfusions and hemoglobin stays at 10.2‐11.0 g/dL. Also there has been a significant improvement in the quality of life.</jats:p></jats:sec><jats:sec><jats:title>Summary/Conclusion:</jats:title><jats:p>This case demonstrates the possibility of a significant improvement in the course of sAA/PNH (including quality of life) in the absence of a sufficient effect of IST, but adequate target control of hemolysis and the use of thrombopoietin receptor agonists.</jats:p></jats:sec>
container_issue S1
container_start_page 850
container_title HemaSphere
container_volume 3
format_de105 Article, E-Article
format_de14 Article, E-Article
format_de15 Article, E-Article
format_de520 Article, E-Article
format_de540 Article, E-Article
format_dech1 Article, E-Article
format_ded117 Article, E-Article
format_degla1 E-Article
format_del152 Buch
format_del189 Article, E-Article
format_dezi4 Article
format_dezwi2 Article, E-Article
format_finc Article, E-Article
format_nrw Article, E-Article
_version_ 1792344331860836361
geogr_code not assigned
last_indexed 2024-03-01T17:05:54.733Z
geogr_code_person not assigned
openURL url_ver=Z39.88-2004&ctx_ver=Z39.88-2004&ctx_enc=info%3Aofi%2Fenc%3AUTF-8&rfr_id=info%3Asid%2Fvufind.svn.sourceforge.net%3Agenerator&rft.title=PB1867+USE+OF+THERAPY+WITH+COMPLEMENT+INHIBITOR+AND+THROMBOPOIETIN+RECEPTOR+AGONISTS+IN+TREATMENT+OF+PATIENT+WITH+SAA%2FPNH.+CLINICAL+CASE.&rft.date=2019-06-01&genre=article&issn=2572-9241&volume=3&issue=S1&spage=850&epage=851&pages=850-851&jtitle=HemaSphere&atitle=PB1867+USE+OF+THERAPY+WITH+COMPLEMENT+INHIBITOR+AND+THROMBOPOIETIN+RECEPTOR+AGONISTS+IN+TREATMENT+OF+PATIENT+WITH+SAA%2FPNH.+CLINICAL+CASE.&aulast=Voloshin&aufirst=S.&rft_id=info%3Adoi%2F10.1097%2F01.hs9.0000565972.20744.8e&rft.language%5B0%5D=eng
SOLR
_version_ 1792344331860836361
author Shilova, E., Glazanova, T., Chubukina, Z., Zenina, M., Romanenko, N., Khorsheva, I., Voloshin, S.
author_facet Shilova, E., Glazanova, T., Chubukina, Z., Zenina, M., Romanenko, N., Khorsheva, I., Voloshin, S., Shilova, E., Glazanova, T., Chubukina, Z., Zenina, M., Romanenko, N., Khorsheva, I., Voloshin, S.
author_sort shilova, e.
container_issue S1
container_start_page 850
container_title HemaSphere
container_volume 3
description <jats:sec><jats:title>Background:</jats:title><jats:p>Aplastic anemia (AA) is severe blood system disease, in which more than half of patients may have PNH clone, and there may occur associated variants AA with PNH (AA/PNH). The most frequently observed is the development of classical hemolytic PNH at AA remission, but possibly a combination of the two diseases. For such cases, there is a positive experience of AA combined treatment with immunosupressive therapy (IST) and targeted therapy using complement activation inhibitors. With resistant AA a therapeutic optionis possible using thrombopoietin receptor agonists.</jats:p></jats:sec><jats:sec><jats:title>Aims:</jats:title><jats:p>To treat of patient with SAA/PNH in absence of possibility of full use of IST</jats:p></jats:sec><jats:sec><jats:title>Methods:</jats:title><jats:p>A clinical observation of a 53‐year‐old female with AA/PNH in the course of the disease is presented. Since 1994 patient, aged 53 yrs, has been under our supervision. The diagnosis was established according to a comprehensive examination, with severity determination in accordance to international criteria. The examination used morphological, histological, immunological (including highly sensitive flow cytometry), biochemical methods. No compatible donor for bone marrow transplantation was found. Anti‐lymphocyte globulin (ALG), cyclosporin‐A (CyA), Eculizumab and thrombopoietin receptor agonists were used in treatment.</jats:p></jats:sec><jats:sec><jats:title>Results:</jats:title><jats:p>ALG and cyclosporine treatment gave only a temporary effect – an improvement in hemogram parameters and a reduction in transfusion dependence. CyA doses were reduced (about 3 mg per day) due to adverse effects. The possibilities of active IST were also limited by comorbidities, including chronic hepatitis B. Since 1999, signs of chronic intravascular hemolysis and hemolytic crises have been observed. Flow cytometry have detected PNH clone. Subsequently, according to ICNN protocol testing data, from 2011 to the present, the clone size was determined 96‐99% with a predominance of type III erythrocytes. According to repeated bone marrow assessments, severe aplasia with pancytopenia in the peripheral blood was maintained. Anemia persisted up to 65 g/dL with transfusion dependence (up to 12‐16 doses of red blood cells per year), leukopenia within 0.9‐1.5 x10<jats:sup>9</jats:sup>/l and thrombocytopenia 5‐15 x10<jats:sup>9</jats:sup>/l with cutaneous hemorrhagic syndrome. On 2013, after vaccination with meningococcal vaccine, Eculizumab treatment was started according to the standard scheme with achievement of an adequate control of hemolysis. Clinical manifestations of hemolysis are absent; the level of LDH does not exceed 1.5 ULN. Therapy continues to the present. Until 2015, CyA therapy was periodically resumed due to the persistence of SAA criteria. In 2013‐2015 the patient additionally received thrombopoetin agonist therapy: Romiplostimum (4‐6 ug/kg once a week) with breaks every 3‐4 months. Two months after the start of therapy, a clinical effect was obtained – a decrease in hemorrhagic syndrome. After 3 months, there was a trend towards an increase in platelet levels. At present, severe leukopenia (1.0 – 2.2 x10<jats:sup>9</jats:sup>/l) and neutropenia (0.5‐0.7x10<jats:sup>9</jats:sup>/l) persist. At the same time, the platelet level is 30‐70 x10<jats:sup>9</jats:sup>/l without spontaneous hemorrhages, since January 2018 the patient does not receive blood transfusions and hemoglobin stays at 10.2‐11.0 g/dL. Also there has been a significant improvement in the quality of life.</jats:p></jats:sec><jats:sec><jats:title>Summary/Conclusion:</jats:title><jats:p>This case demonstrates the possibility of a significant improvement in the course of sAA/PNH (including quality of life) in the absence of a sufficient effect of IST, but adequate target control of hemolysis and the use of thrombopoietin receptor agonists.</jats:p></jats:sec>
doi_str_mv 10.1097/01.hs9.0000565972.20744.8e
facet_avail Online, Free
finc_class_facet Medizin
format ElectronicArticle
format_de105 Article, E-Article
format_de14 Article, E-Article
format_de15 Article, E-Article
format_de520 Article, E-Article
format_de540 Article, E-Article
format_dech1 Article, E-Article
format_ded117 Article, E-Article
format_degla1 E-Article
format_del152 Buch
format_del189 Article, E-Article
format_dezi4 Article
format_dezwi2 Article, E-Article
format_finc Article, E-Article
format_nrw Article, E-Article
geogr_code not assigned
geogr_code_person not assigned
id ai-49-aHR0cDovL2R4LmRvaS5vcmcvMTAuMTA5Ny8wMS5oczkuMDAwMDU2NTk3Mi4yMDc0NC44ZQ
imprint Wiley, 2019
imprint_str_mv Wiley, 2019
institution DE-L229, DE-D275, DE-Bn3, DE-Brt1, DE-Zwi2, DE-D161, DE-Gla1, DE-Zi4, DE-15, DE-Pl11, DE-Rs1, DE-105, DE-14, DE-Ch1
issn 2572-9241
issn_str_mv 2572-9241
language English
last_indexed 2024-03-01T17:05:54.733Z
match_str shilova2019pb1867useoftherapywithcomplementinhibitorandthrombopoietinreceptoragonistsintreatmentofpatientwithsaapnhclinicalcase
mega_collection Wiley (CrossRef)
physical 850-851
publishDate 2019
publishDateSort 2019
publisher Wiley
record_format ai
recordtype ai
series HemaSphere
source_id 49
spelling Shilova, E. Glazanova, T. Chubukina, Z. Zenina, M. Romanenko, N. Khorsheva, I. Voloshin, S. 2572-9241 2572-9241 Wiley Hematology http://dx.doi.org/10.1097/01.hs9.0000565972.20744.8e <jats:sec><jats:title>Background:</jats:title><jats:p>Aplastic anemia (AA) is severe blood system disease, in which more than half of patients may have PNH clone, and there may occur associated variants AA with PNH (AA/PNH). The most frequently observed is the development of classical hemolytic PNH at AA remission, but possibly a combination of the two diseases. For such cases, there is a positive experience of AA combined treatment with immunosupressive therapy (IST) and targeted therapy using complement activation inhibitors. With resistant AA a therapeutic optionis possible using thrombopoietin receptor agonists.</jats:p></jats:sec><jats:sec><jats:title>Aims:</jats:title><jats:p>To treat of patient with SAA/PNH in absence of possibility of full use of IST</jats:p></jats:sec><jats:sec><jats:title>Methods:</jats:title><jats:p>A clinical observation of a 53‐year‐old female with AA/PNH in the course of the disease is presented. Since 1994 patient, aged 53 yrs, has been under our supervision. The diagnosis was established according to a comprehensive examination, with severity determination in accordance to international criteria. The examination used morphological, histological, immunological (including highly sensitive flow cytometry), biochemical methods. No compatible donor for bone marrow transplantation was found. Anti‐lymphocyte globulin (ALG), cyclosporin‐A (CyA), Eculizumab and thrombopoietin receptor agonists were used in treatment.</jats:p></jats:sec><jats:sec><jats:title>Results:</jats:title><jats:p>ALG and cyclosporine treatment gave only a temporary effect – an improvement in hemogram parameters and a reduction in transfusion dependence. CyA doses were reduced (about 3 mg per day) due to adverse effects. The possibilities of active IST were also limited by comorbidities, including chronic hepatitis B. Since 1999, signs of chronic intravascular hemolysis and hemolytic crises have been observed. Flow cytometry have detected PNH clone. Subsequently, according to ICNN protocol testing data, from 2011 to the present, the clone size was determined 96‐99% with a predominance of type III erythrocytes. According to repeated bone marrow assessments, severe aplasia with pancytopenia in the peripheral blood was maintained. Anemia persisted up to 65 g/dL with transfusion dependence (up to 12‐16 doses of red blood cells per year), leukopenia within 0.9‐1.5 x10<jats:sup>9</jats:sup>/l and thrombocytopenia 5‐15 x10<jats:sup>9</jats:sup>/l with cutaneous hemorrhagic syndrome. On 2013, after vaccination with meningococcal vaccine, Eculizumab treatment was started according to the standard scheme with achievement of an adequate control of hemolysis. Clinical manifestations of hemolysis are absent; the level of LDH does not exceed 1.5 ULN. Therapy continues to the present. Until 2015, CyA therapy was periodically resumed due to the persistence of SAA criteria. In 2013‐2015 the patient additionally received thrombopoetin agonist therapy: Romiplostimum (4‐6 ug/kg once a week) with breaks every 3‐4 months. Two months after the start of therapy, a clinical effect was obtained – a decrease in hemorrhagic syndrome. After 3 months, there was a trend towards an increase in platelet levels. At present, severe leukopenia (1.0 – 2.2 x10<jats:sup>9</jats:sup>/l) and neutropenia (0.5‐0.7x10<jats:sup>9</jats:sup>/l) persist. At the same time, the platelet level is 30‐70 x10<jats:sup>9</jats:sup>/l without spontaneous hemorrhages, since January 2018 the patient does not receive blood transfusions and hemoglobin stays at 10.2‐11.0 g/dL. Also there has been a significant improvement in the quality of life.</jats:p></jats:sec><jats:sec><jats:title>Summary/Conclusion:</jats:title><jats:p>This case demonstrates the possibility of a significant improvement in the course of sAA/PNH (including quality of life) in the absence of a sufficient effect of IST, but adequate target control of hemolysis and the use of thrombopoietin receptor agonists.</jats:p></jats:sec> PB1867 USE OF THERAPY WITH COMPLEMENT INHIBITOR AND THROMBOPOIETIN RECEPTOR AGONISTS IN TREATMENT OF PATIENT WITH SAA/PNH. CLINICAL CASE. HemaSphere
spellingShingle Shilova, E., Glazanova, T., Chubukina, Z., Zenina, M., Romanenko, N., Khorsheva, I., Voloshin, S., HemaSphere, PB1867 USE OF THERAPY WITH COMPLEMENT INHIBITOR AND THROMBOPOIETIN RECEPTOR AGONISTS IN TREATMENT OF PATIENT WITH SAA/PNH. CLINICAL CASE., Hematology
title PB1867 USE OF THERAPY WITH COMPLEMENT INHIBITOR AND THROMBOPOIETIN RECEPTOR AGONISTS IN TREATMENT OF PATIENT WITH SAA/PNH. CLINICAL CASE.
title_full PB1867 USE OF THERAPY WITH COMPLEMENT INHIBITOR AND THROMBOPOIETIN RECEPTOR AGONISTS IN TREATMENT OF PATIENT WITH SAA/PNH. CLINICAL CASE.
title_fullStr PB1867 USE OF THERAPY WITH COMPLEMENT INHIBITOR AND THROMBOPOIETIN RECEPTOR AGONISTS IN TREATMENT OF PATIENT WITH SAA/PNH. CLINICAL CASE.
title_full_unstemmed PB1867 USE OF THERAPY WITH COMPLEMENT INHIBITOR AND THROMBOPOIETIN RECEPTOR AGONISTS IN TREATMENT OF PATIENT WITH SAA/PNH. CLINICAL CASE.
title_short PB1867 USE OF THERAPY WITH COMPLEMENT INHIBITOR AND THROMBOPOIETIN RECEPTOR AGONISTS IN TREATMENT OF PATIENT WITH SAA/PNH. CLINICAL CASE.
title_sort pb1867 use of therapy with complement inhibitor and thrombopoietin receptor agonists in treatment of patient with saa/pnh. clinical case.
title_unstemmed PB1867 USE OF THERAPY WITH COMPLEMENT INHIBITOR AND THROMBOPOIETIN RECEPTOR AGONISTS IN TREATMENT OF PATIENT WITH SAA/PNH. CLINICAL CASE.
topic Hematology
url http://dx.doi.org/10.1097/01.hs9.0000565972.20744.8e