| Literature DB >> 28927453 |
Ferenc Magyari1, Karolina Kósa2, Roland Berecz3, Anna Illés4, Zsófia Miltényi5, Zsófia Simon5, Árpád Illés5.
Abstract
BACKGROUND: Due to risk and response adapted treatment strategies, more than 80% of newly diagnosed classical Hodgkin lymphoma (HL) patients can be cured, and become long-term survivors. However, a high proportion of survivors suffer from treatment-related long-term side effects such as secondary malignancy, organ failure, persistent fatigue and psychological distress. The aim of this study was to evaluate psychological distress and its risk factors among our HL survivors.Entities:
Keywords: Employment; HRQoL; Hodgkin-lymphoma; Long-term side effects; Survivorship
Mesh:
Year: 2017 PMID: 28927453 PMCID: PMC5605984 DOI: 10.1186/s12955-017-0758-x
Source DB: PubMed Journal: Health Qual Life Outcomes ISSN: 1477-7525 Impact factor: 3.186
The treatment protocols based on the stage of disease
| Treatment | Number of patients | ||||
|---|---|---|---|---|---|
| Stage I. | Stage II. | Stage III. | Stage IV. | All | |
| ABVD/EBVD + RT | 3 | 52 | 9 | 8 | 72 (51.5%) |
| ABVD/EBVD – RT | 0 | 5 | 9 | 9 | 23 (16.5%) |
| COPP/ABVD + RT | 1 | 3 | 12 | 0 | 16 (11%) |
| COPP/ABVD – RT | 0 | 0 | 5 | 2 | 7 (5%) |
| CVPP + RT | 1 | 6 | 4 | 1 | 12 (9%) |
| CVPP – RT | 1 | 0 | 2 | 0 | 3 (2%) |
| Other | 1 | 2 | 4 | 0 | 7 (5%) |
A(E)BVD: adriamycin (epirubicin), bleomycin, vinblastine and dacarbazine; CV(O)PP: cyclophosphamide, vinblastine [vincristine], procarbazine and prednisolone; COPP/ABV: cyclophosphamide, vincristine, procarbazine, prednisolone/adriamycin, bleomycin and vinblastine; Other protocols include MOPP: mustargen, vincristine, procarbazin, prednisolone, OEPA: vincristine, etoposide, prednisone, and doxorubicin
Characteristics of survivors of working age and independent variables of employment by the results of multiple logistic regression analysis
| All patients ( | Inactive employment status (n = 47) | Active employment status (n = 93) | Univariate analysis | Multiple analysis | |||||
|---|---|---|---|---|---|---|---|---|---|
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| ODDS | 95% CI |
| ODDS | 95% CI | ||||
| Age at survey > = 40 yr. | 76 (54%) | 15 (32%) | 61 (66%) | <0.001 | 4.357 | 2.038–9.316 | |||
| vs. <40 yr. | 64 (46%) | 32 (68%) | 32 (34%) | ||||||
| Age at dg. > = 30 yr. | 80 (57%) |
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| vs. <30 yr. | 60 (43%) |
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| Elapsed time > =10 yr. | 66 (47%) | 24 (51%) | 42 (45%) | 0.436 | 1.325 | 0.652–2.689 | |||
| vs. <10 yr. | 74 (53%) | 23 (49%) | 51 (55%) | ||||||
| Male | 69 (49%) | 23 (49%) | 46 (49%) | 0.953 | 0.979 | 0.485–1.975 | |||
| vs. female | 71 (51%) | 24 (51%) | 47 (51%) | ||||||
| Residence: village | 32 (23%) | 12 (26%) | 20 (22%) | 0.592 | 1.252 | 0.507–2.062 | |||
| vs. city | 108 (77%) | 35 (74%) | 73 (78%) | ||||||
| Education level: | |||||||||
| elementary | 50 (36%) |
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| vs. college | 37 (27%) |
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| elementary | 0.568 | 1.336 | 0.494–3.609 | 0.235 | 1.967 | 0.644–6.007 | |||
| vs. high school | 52 (37%) | 8 (17%) | 29 (31%) | ||||||
| Single | 68 (50%) | 23 (52%) | 45 (49%) | 0.714 | 1.144 | 0.557–2.347 | |||
| vs. live together | 68 (50%) | 21 (48%) | 47 (51%) | ||||||
| Stage 3–4 | 73 (53%) | 24 (52%) | 41 (45%) | 0.399 | 1.357 | 0.668–2762 | |||
| vs. 1–2 | 65 (47%) | 22 (48%) | 51 (55%) | ||||||
| Bulk | 42 (32%) | 11 (27%) | 31 (34%) | 0.409 | 0.710 | 0.314–1.605 | |||
| vs. without bulk | 90 (68%) | 30 (73%) | 60 (66%) | ||||||
| B symptom | 61 (46%) | 20 (49%) | 41 (44%) | 0.691 | 1.161 | 0.555–2.433 | |||
| vs. no B symptom | 71 (54%) | 21 (51%) | 50 (56%) | ||||||
| ECOG 1–2 | 22 (17%) | 8 (20%) | 14 (16%) | 0.593 | 1.299 | 0.497–3.390 | |||
| vs. ECOG 0 | 108 (83%) | 33 (80%) | 75 (84%) | ||||||
| Comorbidity | 68 (49%) | 25 (53%) | 43 (44%) | 0.437 | 1.321 | 0.654–2.667 | |||
| vs. no comorbidity | 72 (51%) | 22 (47%) | 50 (56%) | ||||||
| Treatment: ABVD | 43 (31%) | 16 (34%) | 27 (30%) | 0.599 | 1.224 | 0.576–2.597 | |||
| vs. other | 95 (69%) | 31 (66%) | 64 (70%) | ||||||
| Irradiation | 103 (74%) | 35 (74%) | 68 (73%) | 0.864 | 1.072 | 0.482–2.387 | |||
| vs. no irradiation | 37 (26%) | 12 (26%) | 25 (27%) | ||||||
| Treatment response: PR | 72 (51%) | 4 (9%) | 5 (5%) | 0.484 | 1.637 | 0.418–6.409 | |||
| vs. SD | 68 (49%) | 43 (81%) | 88 (95%) | ||||||
| Treatment related side effect: yes | 72 (51%) |
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| vs. no | 68 (49%) |
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| Relapse | 21 (15%) | 7 (15%) | 14 (15%) | 0.980 | 0.983 | 0.369–2.641 | |||
| vs. no relapse | 119 (85%) | 40 (85%) | 79 (85%) | ||||||
Fig. 1Survivors’ employment status at completion of survey (organogram)
Fig. 2ORs and 95% CI of inactive vs. active employment status by clinical data in HL survivors of working age. The analysis was performed by binary logistic regression. Values under 1 are related to the active employment status, above 1 to inactive employment status
Quality of Life questionnaires for survivors
| All patients ( | Inactive(I) ( | Active(A) ( | P (I-A) | |
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| Mean ± SD | ||||
| HADS anxiety | 5.46 ± 3.54 |
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| HADS depression | 3.05 ± 3.19 |
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| PSS | 4.55 ± 2.80 |
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| SOC | 66.90 ± 11.26 |
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| DAS total | 49.35 ± 18.94 |
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| DAS perfection | 28.41 ± 12.61 |
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| DAS dependency | 20.94 ± 8.01 | 22.81 ± 8.35 | 20.07 ± 7.74 | 0.063 |
| Number of patients (%) | ||||
| HADS anxiety | ||||
| normal score: 0–7 |
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| borderline: 8–11 |
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| abnormal: 11–21 |
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| HADS depression | ||||
| normal score: 0–7 |
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| borderline: 8–10 |
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| abnormal: 11–21 |
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| GHQ | ||||
| normal score: 0–4 |
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| abnormal: ≥5 |
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HADS Hospital Anxiety and Depression scale, GHQ General Health Questionnaire, PSS Perceived Stress, Scale, SOC Sense of Coherence Scale, DAS Dysfunctional Attitude Scale
Predictors for treatment related long-term side effects
| Treatment related long- term side effects | No treatment related long-term side effects |
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|---|---|---|---|
| Gender | |||
| Male ( | 28 (41%) | 41 (59%) | 0.011 |
| Female ( | 44 (62%) | 27 (38%) | |
| Chemotherapy | |||
| A(E)BVD ( | 38 (40%) | 57 (60%) | <0.001 |
| Other than ABVD ( | 33 (77%) | 10 (23%) | |
A(E)BVD: adriamycin, (epirubicin), bleomycin, vinblastine and dacarbazine; Other than ABVD: CV(O)PP:cyclophosphamide, vinblastine [vincristine], procarbazine and prednisolone; COPP/ABV:cyclophosphamide, vincristine, procarbazine, prednisolone/adriamycin, bleomycin and vinblastine
Fig. 3Loss of work after lymphoma treatment by patient reports