| Literature DB >> 17299394 |
T Powles1, P M Savage, J Stebbing, D Short, A Young, M Bower, C Pappin, P Schmid, M J Seckl.
Abstract
The majority of women requiring chemotherapy for gestational trophoblastic disease (GTN) are cured with their initial chemotherapy treatment. However, a small percentage either become refractory to treatment, or relapse after the completion of treatment. This study investigates the characteristics and outcome of these patients. Patients were identified from the Charing Cross Hospital GTD database. The outcome of these patients with relapsed disease was compared to those with refractory disease. Between 1980 and 2004, 1708 patients were treated with chemotherapy for GTN. Sixty (3.5%) patents relapsed following completion of initial therapy. The overall 5-year survival for patients with relapsed GTN was 93% (95% CI 86-100%). The overall survival for patients with low-risk and high-risk disease at presentation, who subsequently relapsed was 100% (n=35), and 84% (n=25) (95% CI: 66-96%: P<0.05), respectively. Eleven patients were identified who failed to enter remission and had refractory disease. These patients had a worse outcome compared to patients with relapsed disease (5-year survival 43% (95% CI:12-73% P<0.01)). The outcome of patients with relapsed GTN is good. However, patients with primary chemo-refractory disease do poorly and novel therapies are required for this group of patients.Entities:
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Year: 2007 PMID: 17299394 PMCID: PMC2360082 DOI: 10.1038/sj.bjc.6603608
Source DB: PubMed Journal: Br J Cancer ISSN: 0007-0920 Impact factor: 7.640
Characteristics at initial presentation of disease for patients who developed relapsed GTN (n=60)
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| Number | 60 | 25 | 11 |
| Median prognostic score (WHO) at diagnosis | 7 (range 2–23) | 9 (range 8–23) | 16 (range 8–26) |
| Median prognostic score (FIGO) | 4 (range 1–12) | 7 (range 5–12) | 10 (range 6–18) |
| Antecedent pregnancy | Term 19 Abortion 7 Mole 34 | Term 17 Abortion 5 Mole 3 | Term 7 Abortion 1 Mole 3 |
| Median hCG before initial treatment | 21 000 (range 31–814 000) | 66 000 (range 350–814 000) | 380 000 (range 79 000–1 100 000) |
| Duration between causal pregnancy and initial treatment | 0.4 years (range 0.1–7.3 years) | 1.1 years (range 0.1–7.3 years) | 3.2 years (range 0.1–15) |
| Uterine size | 0–3 cm–15 3–5 cm–39 >5 cm–6 | 0–3 cm–7 3–5 cm–16 >5 cm–2 | 0–3 cm5 3–5 cm–4 >5 cm–2 |
| Site of metastasis | None 40
Lung only 16
Other sites | None 12
Lung only 9
Other sites | None 0
Lung only 7
Other sites |
| Initial treatment regimens | Methotrexate 35 EMA/CO 18 Platinum-based 7 | EMA/CO 17 Platinum-based 7 | EMA/CO 11 |
GTN=gestational trophoblastic neoplasia; WHO=World Health Organization.
With or without lung metastasis (includes liver (2), brain (1) and liver and brain(1).
Liver, 2; brain, 2.
Patients characteristics at time of relapse or refractory disease
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| Number | 60 | 11 |
| Median time to relapse or refractory disease (months) | 4 months (range 0.25–37 months) | 3 months (range 0.25–6.75) |
| Median hCG at relapse/refractory disease | 309 (range 25–105 000) | 1244 (range 14–255 000) |
| Rate of hCG rise (median doubling time in days) | 9 days (range 3–28) days) | NA |
| Median time between diagnosis of relapse and starting treatment (months) | 0.4 months (range 0–3) | NA |
| Symptoms/method of diagnosis of relapse | hCG Screening 47
PV bleeding 2
Amenorrhoea 7
Other | Screening 11 |
| Site of disease at relapse | hCG relapse12
Mass in uterus only 29
Lung 12
Lung and uterus 3
Pelvis 1 other and uterus 3 | NA |
HCG=human chorionic gonadotropin; NA=not available.
Respiratory symptoms, haemoptysis and re-entry to screening programme.
Includes liver (1), liver and brain(1), pelvis (2).
Time to relapse after chemotherapy
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| 0–3 months | 31 (51.6) | 51.6 |
| 3–6 months | 10 (16.6) | 68.2 |
| 6–12 months | 3 (5) | 73.2 |
| 12–24 months | 7 (11.7) | 84.9 |
| 1–5 years | 8 (13.5) | 98.4 |
| >5 years | 1 (1.6) | 100 |
Management and outcome of relapsed disease
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| Hysterectomy only | 2 |
| Hysterectomy and chemotherapy | EMA/CO 3 EP 1 |
| Chemotherapy only | EMA/CO 25 CO/EP 1 EP 1 EP/EMA 2 |
| 5-year survival | 100% |
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| Thoracotomy and chemotherapy | EP/EMA 2 POMB ACE 1 EMA/CO 1 |
| Hysterectomy and chemotherapy | EP/EMA 3 EMA/CO 1 Cis/taxol 1 |
| Chemotherapy only | EMA/CNS 1 EMA/CO 3 EP/EMA 10 Cisplatin vincristine 1 Cis/taxol 1 |
| 5-year survival | 84% (95% CI: 68–99%) |
EMA/CO – weekly combination chemotherapy, comprising of etoposide(dose), methotrexate, actinomycin alternating with cyclophosphamide and vincristine (Bower ).
POMBACE – cisplatin, vincristine, methotrexate, bleomycin alternating with actinomycin D, cyclophosphamide and etoposide (Newlands ).
EP/EMA – etoposide, cisplatin/etoposide, methotrexate and actinomycin D (Newlands ).
EMA/CNS – etoposide, methotrexate and actinomycin alternating weekly with vincristine and cyclophosphamide. The dose of methotrexate was increased to 1 g m−2.
Cis/taxol – cisplatin etoposide and paclitaxel (Osborne ) EP cisplatin etoposide (IV day 1–5).
Univariate analysis for patients with relapsed disease
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| Median age at relapse (years) | 32 | 29 | 0.26 | |
| Median hCG at presentation | 15 000 | 28 000 | 0.14 | |
| Median interval between causal pregnancy and first chemotherapy | 1.1 years | 0.5 years | 0.57 | |
| Maximum hCG at relapse (medium) | 350 | 121 | 0.41 | |
| HCG doubling time at relapse (days) | 15 | 7 | 0.01* | |
| Lung metastasis at presentation | No | 2 | 42 | 0.11 |
| Yes | 3 | 13 | ||
| Nonpulmonary metastasis at presentation | No | 3 | 52 | 0.05* |
| Yes | 2 | 3 | ||
| Treatment at initial presentation | High risk | 5 | 20 | 0.01* |
| Low risk | 0 | 35 | ||
| Interval between chemotherapy and relapse | 0–3 months | 4 | 30 | 0.19 |
| >3 months | 1 | 25 | ||
| Metastasis identified at relapse | No | 1 | 39 | 0.03* |
| Yes | 4 | 16 | ||
| Uterine mass identified at relapse | No | 3 | 24 | 0.65 |
| Yes | 2 | 31 | ||
| Nonpulmonary metastasis at relapse | No | 4 | 52 | 0.30 |
| Yes | 1 | 3 | ||
| Causal pregnancy | Mole | 0 | 29 | 0.02* |
| Term | 5 | 26 | ||