Background: Eltrombopag is an oral thrombopoietin receptor agonist (TPO-RA) drug approved in primary chronic ITP. Lack of clinical trials in secondary ITP avoids a clear demonstration of its potential in terms of safety and efficacy on secondary ITP.

Aims: To evaluate the efficacy and safety of eltrombopag in secondary ITP patients in daily clinical practice in Spain.

Methods: Ninety-eight secondary ITP patients (aged 18 years or more) from 30 Spanish centers, treated with eltrombopag and included in the Spanish Eltrombopag Registry were retrospectively evaluated. Our study was performed in accordance with the standards of the Helsinki declaration and approved by the Hospital Universitario de Burgos Ethics Committee.

Results:

Our case series included 98 patients we allocated to four categories: immune disorders (n=47), infections (n=23), lymphoproliferative disorders (n=20), and neoplasms (n=8).

The median age of the cohort was 62 (IQR, 40-71) years with 38 men and 60 women. At diagnosis, 34 patients had a Charlson Comorbidity Index score of 2 or more. Median time from ITP diagnosis to eltrombopag initiation was 13 (IQR, 2-66) months. Median number of therapies against thrombocytopenia before eltrombopag was 2 (IQR, 1-3), including rituximab (24), splenectomy (18) and romiplostim (13). Median platelet count when treatment started was 15 x 109/L (IQR, 5-43 x 109/L). Meanwhile, 44 patients had bleeding symptoms. Concomitant therapy was administered to 55 ITP (corticoids in 33) (Table I).

Whole cohort eltrombopag response rate was 59% of responses (R; platelet count ≥30 x109/L and at least 2-fold increase the baseline count and absence of bleeding) with 52% of complete responses (CR; platelet count >100 x 109/L). Regarding the disease associated to ITP we observed high response rates in immune disorders and infection groups (67% of R, 76 % of R, respectively). Nevertheless, in lymphoproliferative disorders and neoplastic groups efficacy rates were much lower (36 % of R, 37 % of R respectively). The proportion of patients achieving platelet response was quite similar regardless the other studied parameters: age, sex, concomitant treatment, bleeding and platelet count at start of eltrombopag treatment.

30 adverse events were reported with eltrombopag, being 18 of them grade 3-4. 14 deaths were observed but only two were caused by bleeding. The remaining causes of death were: 4 because of bacterial sepsis and another 4 due to progression of basal disease. 2 secondary neoplasms, 1 aspergillosis and one death due to a non-treated severe anemia were also reported (Table II).

Conclusion:

The use of eltrombopag for treating secondary ITP is effective and safe. To point out, its efficacy in lymphoproliferative disorders and in neoplasm-associated ITP is lower than in benign diseases.

Certainly, more studies are needed to confirm usefulness of TPO-RAs in secondary ITP cases.

Table 1.

Patient characteristics

VariableTotal
(n = 98)
Type of disease, n  
Immune disorders  
 SLE 13 
 Evans Syndrome 
 Antiphospholipid Syndrome 
 Sjögren Syndrome 
 Rheumatoid Arthritis 
 Immunodeficiencies 
 Autoimmune Hepatitis 
 Primary Biliary Cirrhosis 
 Psoriatic arthritis 
 Evans Syndrome-Immunodeficiencies 
 Evans Syndrome-HCV 
 Graves-Basedow disease 
 Inflammatory Bowel disease 
Lymphoproliferative disorders  
 Lymphoproliferative diseases 16 
 HCV-Lymphoma 
 HIV-Lymphoma 
Infections  
 Hepatitis C Virus 16 
 HIV 
 HCV-HIV 
Neoplasms  
 Myeloid Neoplasms 
Age, years, median [Q1;Q362[40;71] 
Men/Women38/60 
Bleeding at start of eltrombopag treatment,44 
Concomitant treatment,55 
 Corticoids 33 
 Immunoglobulins 
 Corticoids and Immunoglobulins 
VariableTotal
(n = 98)
Type of disease, n  
Immune disorders  
 SLE 13 
 Evans Syndrome 
 Antiphospholipid Syndrome 
 Sjögren Syndrome 
 Rheumatoid Arthritis 
 Immunodeficiencies 
 Autoimmune Hepatitis 
 Primary Biliary Cirrhosis 
 Psoriatic arthritis 
 Evans Syndrome-Immunodeficiencies 
 Evans Syndrome-HCV 
 Graves-Basedow disease 
 Inflammatory Bowel disease 
Lymphoproliferative disorders  
 Lymphoproliferative diseases 16 
 HCV-Lymphoma 
 HIV-Lymphoma 
Infections  
 Hepatitis C Virus 16 
 HIV 
 HCV-HIV 
Neoplasms  
 Myeloid Neoplasms 
Age, years, median [Q1;Q362[40;71] 
Men/Women38/60 
Bleeding at start of eltrombopag treatment,44 
Concomitant treatment,55 
 Corticoids 33 
 Immunoglobulins 
 Corticoids and Immunoglobulins 

Table 2.

Adverse events with Eltrombopag

Variablen
Total, n 30 
Serious Adverse Events (Grade 3-4), n 18 
 Progression of basal disease 
 Severe Bacterial Infections 
 Deep venous thrombosis 
 Stroke 
 Medullary fibrosis 
 Severe Bleeding 
 Aspergillosis 
 Pulmonary Embolism 
 Secondary neoplasms 
 Acute Pancreatitis 
 Acute Myocardial Infarction 
Deaths, n 14 
 Bacterial Infections 
 Progression of basal disease 
 Secondary neoplasms 
 Severe Bleeding 
 Aspergillosis 
  Severe Anemia due to negative of patient to transfusion 
Variablen
Total, n 30 
Serious Adverse Events (Grade 3-4), n 18 
 Progression of basal disease 
 Severe Bacterial Infections 
 Deep venous thrombosis 
 Stroke 
 Medullary fibrosis 
 Severe Bleeding 
 Aspergillosis 
 Pulmonary Embolism 
 Secondary neoplasms 
 Acute Pancreatitis 
 Acute Myocardial Infarction 
Deaths, n 14 
 Bacterial Infections 
 Progression of basal disease 
 Secondary neoplasms 
 Severe Bleeding 
 Aspergillosis 
  Severe Anemia due to negative of patient to transfusion 

Disclosures

Off Label Use: We describe the possibility of using eltrombopag, an oral thrombopoietin receptor analog, for secondary ITP patients..

Author notes

*

Asterisk with author names denotes non-ASH members.

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