Radiation Oncology/Uterine Sarcoma/Leiomyosarcoma
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Uterine Leiomyosarcoma
Overview
edit- LMS account for ~25% of uterine sarcomas, which account for ~4% of uterine malignancies
- Presentation typically with vaginal bleeding, pelvic mass, and pain
- PET/CT useful based on anecdotal evidence
- Staging: based on endometrial CA; cervical LMS is considered Stage II
- Outcome prediction
- Mayo clinic risk assessment index (age, size, stage, grade)
- Prognostic index developed for soft tissue sarcomas does not apply to LMS (PMID 10717626)
- Surgery main treatment modality
- TAH standard component
- Lymph node dissection has not improved survival, but provides prognostic information
- Oophorectomy may not be necessary in premenopausal women, if ovaries are grossly normal
- Outcomes:
- Stage I-II LMS may be cured (15-year OS 40-50%)
- Stage III-IV LMS have very poor prognosis (5-year OS 15-30%)
- Adjuvant RT is controversial; Mayo data suggest significantly improved LC, but no impact on DFS or OS. Phase III EORTC trial in Stage I-II showed no impact on loco-regional control, PFS or OS for leiomyosarcoma (but LRR benefit for carcinosarcoma)
- Adjuvant chemotherapy is also controversial; doxorubicin-based regimens appear the most active, but have not resulted in significant survival benefit
Localized LMS
edit- EORTC 55874 (1987-2000) -- observation vs. pelvic RT
- Randomized. 224 patients with high grade uterine sarcoma (leiomyosarcoma 46%, carcinosarcoma 41%, endometrial stromal sarcoma 13%), Stage I-II (LMS were all stage I using FIGO 2009 system), treated with TAH/BSO + washings (75%), nodal sampling optional (25%). Arm 1) observation vs. Arm 2) pelvic RT 50.4/28 Field: top border L4/L5, lower border lower margin of obturator foramina, posterior border S2/S3
- 2008 PMID 18378136 -- "Phase III randomised study to evaluate the role of adjuvant pelvic radiotherapy in the treatment of uterine sarcomas stages I and II: An European Organisation for Research and Treatment of Cancer Gynaecological Cancer Group Study (protocol 55874)." (Reed NS, Eur J Cancer. 2008 Mar 28 [Epub ahead of print])
- Outcome: LRR only observation 18% vs. RT 3%, LRR at any time 40% vs. 21% (SS); no impact on PFS or OS
- By subset: No benefit for LMS, improved local control for CS
- Conclusion: Pelvic RT improves local control but not PFS or OS for carcinosarcoma, there is no benefit in leiomyosarcoma
- Minnesota, 2005 (1972-1998) PMID 15923804 -- "On the apparent failure of adjuvant pelvic radiotherapy to improve survival for women with uterine sarcomas confined to the uterus." (Dusenbery KE, Am J Clin Oncol. 2005 Jun;28(3):295-300.)
- Retrospective. 49 patients with Stage I-II (20 LMS, 18 homologous mullerian, 11 heterologous mullerian)
- DFS: LMS 5-years 40%, 15-years 40%; Mullerian 5-years 65%, 15-years 61%. Failures mostly distant
- Toxicity: 3 SBO, 1 sigmoid colon obstruction
- Conclusion: adjuvant pelvic RT efficacious; frequent peritoneal failures suggest role for abdominal RT; better systemic therapy needed
- Gustave-Roussy, 2004 PMID 15571617 -- "Adjuvant chemotherapy with cisplatin, ifosfamide, and doxorubicin followed by radiotherapy in localized uterine sarcomas: results of a case-control study with radiotherapy alone." (Pautier P, Int J Gynecol Cancer. 2004 Nov-Dec;14(6):1112-7.)
- Case-control. 18 patients with chemo followed by RT vs. 16 patients RT alone vs. 2 patient no therapy
- Conclusion: Adjuvant chemo followed by RT is feasible; PIII trial ongoing in France
All stages
edit- SARCGYN trial; 2013 PMID 23139262 -- "A randomized clinical trial of adjuvant chemotherapy with doxorubicin, ifosfamide, and cisplatin followed by radiotherapy versus radiotherapy alone in patients with localized uterine sarcomas (SARCGYN study). A study of the French Sarcoma Group." (Pautier P, Ann Oncol. 2013 Apr;24(4):1099-104. doi: 10.1093/annonc/mds545. Epub 2012 Nov 8.)
- Randomized. 81 patients with LMS (48%), carcinosarcoma (23%), undifferentiated sarcoma (11%). Stage I (64%). Both arms surgery + pelvic RT. Randomized to observation vs chemotherapy with doxorubicin / ifosfamide / cisplatin x 4 cycles. Stopped early due to lack of recruitment. Median F/U 4.3 years
- Outcome: 3-year OS: chemo-RT 81% vs RT only 69% (NS); DFS 55% vs 41% (SS).
- Toxicity: Grade 3+ thrombopenia 76%, febrile neutropenia 22%, two toxic deaths
- Conclusion: chemotherapy increases disease-free survival
- Princess Margaret; 2013 (1998 - 2008) PMID 23705661 -- "Postoperative radiotherapy improves local control and survival in patients with uterine leiomyosarcoma." (Wong P, Radiat Oncol. 2013 May 24;8:128. doi: 10.1186/1748-717X-8-128.)
- Retrospective. 69 patients, primary uterine LMS with hysterectomy. Pelvic RT 45 Gy in 32 patients (46%). Median F/U 5 years
- Outcome: LR observation 39% vs RT 19% (SS); 3-year OS 69% vs 35% (SS) univariate, persisted on multivariate. Positive SM increased odds of LR (HR 5.6). Large tumor size and Stage II-IV associated with development of distant mets
- Conclusion: Postoperative pelvic RT reduces LR and improves OS of patients with uterine LMS
- Dijon, 2005 (France) (1966-2001) PMID 15837053 -- "The role of surgery and treatment trends in uterine sarcoma." (Benoit L, Eur J Surg Oncol. 2005 May;31(4):434-42.)
- Retrospective. 72 patients with uterine sarcomas (34 LMS, 25 mullerian, 12 ESS, 1 angiosarcoma). RT 55%. Chemo 37%
- 5-year OS: all 36%; Stage I 47%, Stage II 60%, Stage III/IV 15%
- Conclusion: surgery main treatment. Adjuvant therapies do not decrease DM or increase OS
- MGH, 2004 (1990-1999) PMID 14766261 -- "The treatment of uterine leiomyosarcoma. Results from a 10-year experience (1990-1999) at the Massachusetts General Hospital." (Dinh TA, Gynecol Oncol. 2004 Feb;92(2):648-52.)
- Retrospective. 27 patients. Most treated with multimodality therapy (surgery, chemotherapy, and/or RT)
- Sugery: if no visible disease post-op, better OS (SS)
- Adjuvant therapy: after optimal cytoreduction, no decrease in rate of recurrence
- Adjuvant chemo: minimally effective, with 80% progression of disease
- Conclusion: Deadly disease. Aggressive surgical cytoreduction should be the goal
- Mayo, 2003 (1976-1999) PMID 12798712 -- "Retrospective review of 208 patients with leiomyosarcoma of the uterus: prognostic indicators, surgical management, and adjuvant therapy." (Giuntoli RL 2nd, Gynecol Oncol. 2003 Jun;89(3):460-9.)
- Retrospective. 208 patients with LMS. Median F/U 7.7 years
- Worse prognosis: high grade, advanced stage, oophorectomy worse DSS
- Pelvic RT: no impact on DSS (p=0.06) in multivariate analysis. Significantly decreased LR when further evaluated as 31 case-controls (70% Stage I)
- Ovarian resection no impact on survival
- Risk-assessment index developed:
- Age (>51): 1 point; Tumor size (>5cm): 1 point; Stage (II-IV): 1 point; Grade (2-4): 2 points
- Low risk = 0-1 points (n=22, no deaths, median survival >25 years), intermediate risk = 2-3 points (n=53, median survival 6.5 years), high risk = 4-5 points (n=81, median survival 2.1 years)
- Vienna, 1999 PMID 10419731 -- "Leiomyosarcoma of the uterus: a clinicopathologic multicenter study of 71 cases." (Mayerhofer K, Gynecol Oncol. 1999 Aug;74(2):196-201.)
- Retrospective. 71 patients. Median F/U 9 years
- Predictors: age (<50 better), tumor stage, LVI, mitotic count in Stage I
- Norwegian Radium Hospital, 1993 (1976-1985) PMID 11578330 -- "Leiomyosarcoma (LMS) and endometrial stromal sarcoma (ESS) of the uterus. A survey of patients treated in the Norwegian Radium Hospital 1976-1985." (Nordal RN, Int J Gynecol Cancer. 1993 Mar;3(2):110-115.)
- Retrospective. 127 patients with LMS or endometrial stromal sarcoma, 14 reclassified
- 5-year OS: LMS 39%, ESS 67%
- Prognosis: grade (Grade I-II similar prognosis as endometrial carcinoma, Grade III-IV 5-year OS 33%)
- Adjuvant chemo: no clear benefit
Advanced LMS
edit- No good chemotherapy regimens available; minimal impact on survival
- Doxorubicin-based combinations appear the most active, and are typically used as first line
- Minnesota experience with RT not particularly successful
- Search continues ...
- GOG, 2005 PMID 15721421 -- "Phase II evaluation of liposomal doxorubicin (Doxil) in recurrent or advanced leiomyosarcoma of the uterus: a Gynecologic Oncology Group study." (Sutton G, Gynecol Oncol. 2005 Mar;96(3):749-52.)
- Phase II. 35 patients. Liposomal doxorubicin 50mg/m2 IV.
- Conclusion: no benefit over standard doxorubicin
- GOG, 2005 PMID 16051328 -- "Phase II trial of dacarbazine, mitomycin, doxorubicin, and cisplatin with sargramostim in uterine leiomyosarcoma: a Gynecologic Oncology Group study." (Long HJ, Gynecol Oncol. 2005 Nov;99(2):339-42.)
- Phase II. 18 patients. DMAP + sargramostim.
- Conclusion: too complex and toxic. Study closed early
- Minnesota, 2004(1978-1997) PMID 15262141 -- "Limitations of adjuvant radiotherapy for uterine sarcomas spread beyond the uterus." (Dusenbery KE, Gynecol Oncol. 2004 Jul;94(1):191-6.)
- Retrospective. 19 women with advanced uterine sarcomas who received adjuvant RT. 7 adjuvant chemo.
- Survival: 1-year 67%, 5-year 33%; failures mostly distant
- Conclusion: prognosis if spread beyond uterus is poor
- GOG, 2003 PMID 12694653 -- "Evaluation of paclitaxel in previously treated leiomyosarcoma of the uterus: a gynecologic oncology group study." (Gallup DG, Gynecol Oncol. 2003 Apr;89(1):48-51.)
- Phase II. 48 patients. Paclitaxel 175 mg/m2 IV
- Conclusion: modest activity, minimal toxicity
- GOG, 2002 PMID 12051882 -- "Phase II study of mitomycin, doxorubicin, and cisplatin in the treatment of advanced uterine leiomyosarcoma: a Gynecologic Oncology Group study." (Edmonson JH, Gynecol Oncol. 2002 Jun;85(3):507-10.)
- Phase II. 35 patients, treated with MAP 1-6 cycles
- Conclusion: MAP is not remarkably active; significant (10/35) pulmonary toxicity
- GOG, 1999 PMID 10479491 -- "Phase II trial of paclitaxel in leiomyosarcoma of the uterus: a gynecologic oncology group study." (Sutton G, Gynecol Oncol. 1999 Sep;74(3):346-9.)
- Phase II. 34 women. Paclitaxel 175 mg/m2 IV. RT in 23%
- Conclusion: Limited activity; consider higher dose
- GOG, 1996 PMID 8751554 -- "Ifosfamide and doxorubicin in the treatment of advanced leiomyosarcomas of the uterus: a Gynecologic Oncology Group study." (Sutton G, Gynecol Oncol. 1996 Aug;62(2):226-9.)
- Phase II. 34 women. Ifosfamide + doxorubicin
- Conclusion: Toxic, with moderate activity