Predictors of Individual Symptom Scores in Myeloproliferative Neoplasms: A Real-World Retrospective Cohort Study

Introduction

Symptom burden in myeloproliferative neoplasms (MPN) is quantified using total symptom scores (TSS) calculated from the patient-reported scores for clinically meaningful symptoms. The impact of demographic, clinical, and laboratory features on these symptoms remains unclear and warrants further investigation.

Methods

Patients with polycythemia vera (PV), essential thrombocythemia (ET), and myelofibrosis (MF) were identified from the retrospective chart review. TSS, scores of individual symptoms (fatigue, early satiety, abdominal discomfort, inactivity, concentration difficulties, fever, night sweats, itching, bone pain, weight loss), demographic characteristics (race, ethnicity, age, and gender), clinical features (time since diagnosis, depression status, obesity status), laboratory results and season at the time of visit when the first TSS assessment was performed were recorded. Multicollinearity and homoscedasticity were assessed using variance inflation factors and visual inspection of the data, respectively. A multivariable regression analysis was performed using a robust variance estimator. A p-value <0.05 indicated a statistically significant association with the symptom scores.

Results

The chart review identified 557 (PV: 201; ET: 191; MF: 165) patients. The median age of patients with PV, ET, and MF was 65 (range: 27-93), 65 (20-96), and 69 (27-96) years, respectively. Most patients were white (PV: 92%; ET: 90%; MF: 93%) and non-Hispanic or Latino (PV: 93%; ET: 96%; MF: 92%). Most patients with PV and ET were female (PV: 51%; ET: 73%), while most patients with MF were male (55%). Among the included patients 22% (PV: 21%; ET: 27%; MF: 18%) had the diagnosis of depression at the time of the clinical visit. TSS was highest in MF (mean (SD): 18.1±14.6), followed by PV (15.7±14.5) and ET (15.1±14.0) patients. Fatigue was the most reported symptom by the patients (PV: 81%; ET: 82%; MF: 84%), whereas weight loss was the least reported symptom (PV: 4.5%; ET: 6.3%; MF: 16%).

With regards to the TSS multivariable regression analysis showed that age (beta coefficient: 0.2; p=0.01), depression (7.2; 0.008), and low hemoglobin (1.2; 0.003) in PV, depression (11.7; 0.001) in ET, and depression (9.5; 0.001), splenomegaly (6.9; 0.01), and WBC count (0.16; 0.048) in MF patients were significantly associated with TSS.

In terms of individual symptoms in PV, depression was associated with fatigue (beta coefficient: 1.31; p-value: 0.01) and concentration difficulties (1.7; <0.001), high WBC count was associated with early satiety (0.09; 0.03), and non-white race was associated with fever (1.4; 0.007). In ET, depression was associated with fatigue (1.6; <0.001), abdominal discomfort (1.4; <0.001), inactivity (2.5; <0.001), concentration difficulties (2.4; <0.001) and night sweats (1.4; <0.001), anemia was associated with fatigue (1.2; 0.03), fewer months since diagnosis was associated with inactivity (0.01; 0.02) and young age was associated with bone pain (0.02; 0.03). In MF, depression was associated with fatigue (1.8; 0.001), concentration difficulties (1.3; 0.01), fever (1.1; 0.02), and night sweats (2.2; 0.03), low hemoglobin was associated with fatigue (0.46; <0,001) and early satiety (0.31; 0.003), high WBC count was associated with fatigue (0.03; 0.04) and early satiety (0.04; 0.02), low platelet count was associated with abdominal discomfort (0.002; 0.03), splenomegaly was associated with inactivity (2.27; 0.003) and female gender was associated with itching (0.57; 0.01).

Conclusions

This study demonstrates that depression in PV and ET and depression, low hemoglobin, and a high WBC count in MF contribute to multiple symptoms seen in these patients. Identifying demographic groups at risk of a higher symptom burden and addressing the comorbidities that drive symptoms, in addition to disease-directed therapy, is crucial to improving the quality of life in these patients.