Abstract
Background. The epidemiology of pain in patients with advanced haematological malignancies followed at home, 469 consecutive patients has been followed over a six years.
Methods. Each pain syndrome (PS) was properly assessed and treated according to the WHO ladder. The pain intensity was reported by a Numerical Analogue Scale, which rated score ranging from 0 (no pain) to 10 (the most severe), or, in less complaint patients, by a verbal description. Each PS was classified as deep somatic, superficial somatic, neuropathic and mixed or unknown.
Results. Of 469 patients, 258 (55%) were males; the median age was 67 (4–95) years. Out of 469 patients, 244 (52%) experienced almost one PS, for a total of 284, which intensity was rated from mild to moderate in 92 (31%) and from moderate to severe in 192 (69%) of them respectively. The 244 patients who experienced pain were significantly younger than those without pain (57 ± 21 versus 69±16, P< 0.0005). Moreover, the group of less than 20 old years patients presented a higher incidence of pain compared to others (85% versus 49%, P=0.0007). The patients affected by Multiple Myeloma (MM), Acute Lymphoblastic Leukaemia (ALL), non Hodgkin’s Lymphomas (NHL) and Blastic Crisis showed a higher incidence of pain compared to other disease groups (P=0.0011). Among acute leukemias, ALL patients presented a higher incidence of pain compared to those affected by myeloblastic forms (79% versus 41%, P= 0.0002). An effective pain control was achieved within 24 hours in 259/284 (92%) without any admission. PS was diagnosed as deep somatic, superficial somatic, visceral, neuropathic and mixed (somatic + neuropathic) in the 56 %, 15 %, 14 %, 7 % and 8 % of the PS respectively. A higher incidence of deep somatic pain was recorded in all diagnosis groups. Moreover, out of the 39 visceral PS, 33 (85%) have been recorded among patients with NHL and 6 (15%) in the others (P=0.0001). MM patients presented a higher rate of the incident pain (P<0.001). The causative mechanisms of PS were directly referable to underlying diseases, to their clinical complications and to concomitant and unrelated conditions in the 69%, 22% and 9% of cases respectively. The most involved sites were: the spine (27%), the abdomen (20%), the legs (15%), the thorax (11%) and orofaringeal tract (10%).
Conclusion. our data show that pain is a relevant problem in advanced onco-haematological patients, which mostly present disease-related PS, reflecting specific pathological activity of the underlying malignancy.
Malignancy . | PP/TP (No) . | Incidence of pain (%) . | Pain Syndromes (No) . |
---|---|---|---|
PP: Pain Patients; TP: Total Patients, No: number, MM: Multiple Myeloma, ALL: Acute Lymphoblastyc Leukemia, NHL; Non Hodgkin’s Lymphomas; BC: Blastic Crisis, HD: Hodgkin’s Disease, CLL: Chronic Lymphocytic Leukemia, Acute Myeloblastyc Leukemia, MDS: Myelodysplastyc Syndromes, CMPD: Chronic Myeloproliferative Disorders. | |||
MM | 35/39 | 90 | 38 |
ALL | 31/39 | 79 | 40 |
NHL | 77/128 | 60 | 89 |
BC | 29/56 | 52 | 34 |
HD | 5/11 | 45 | 5 |
CLL | 10/24 | 42 | 11 |
AML | 28/69 | 41 | 34 |
MDS | 20/63 | 32 | 22 |
CMPD | 5/33 | 18 | 8 |
Others | 3/7 | 43 | 3 |
Total | 243/469 | 52 | 284 |
Malignancy . | PP/TP (No) . | Incidence of pain (%) . | Pain Syndromes (No) . |
---|---|---|---|
PP: Pain Patients; TP: Total Patients, No: number, MM: Multiple Myeloma, ALL: Acute Lymphoblastyc Leukemia, NHL; Non Hodgkin’s Lymphomas; BC: Blastic Crisis, HD: Hodgkin’s Disease, CLL: Chronic Lymphocytic Leukemia, Acute Myeloblastyc Leukemia, MDS: Myelodysplastyc Syndromes, CMPD: Chronic Myeloproliferative Disorders. | |||
MM | 35/39 | 90 | 38 |
ALL | 31/39 | 79 | 40 |
NHL | 77/128 | 60 | 89 |
BC | 29/56 | 52 | 34 |
HD | 5/11 | 45 | 5 |
CLL | 10/24 | 42 | 11 |
AML | 28/69 | 41 | 34 |
MDS | 20/63 | 32 | 22 |
CMPD | 5/33 | 18 | 8 |
Others | 3/7 | 43 | 3 |
Total | 243/469 | 52 | 284 |
Disclosure: No relevant conflicts of interest to declare.
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