TURKISH JOURNAL OF ONCOLOGY 2011 , Vol 26 , Num 1
Long-term results of adjuvant radiotherapy in stage I endometrial cancer
Didem ÇOLPAN ÖKSÜZ, Arzu ERGEN, Gülyüz ATKOVAR, İsmet ŞAHİNLER
Department of Radiation Oncology, Istanbul University Cerrahpasa Faculty of Medicine, Istanbul

Summary

OBJECTIVES
We aimed to analyze the treatment results and the acute and late side effects in patients with stage I endometrial carcinoma receiving adjuvant radiotherapy.

METHODS
Two hundred sixty-three patients with stage I endometrial adenocarcinoma, who were treated with postoperative radiotherapy between 1978 and 1998, were analyzed retrospectively. According to the 1988-FIGO staging system, the disease was stage IA in 19, stage IB in 128, and stage IC in 116 patients. One hundred and ninety-seven patients were treated with external and intracavitary irradiation, 45 patients with external radiotherapy and 21 patients with vaginal brachytherapy.

RESULTS
The 10-year local control, disease-free and actuarial survival rates were 96%, 93% and 95%, respectively. Fifty-five patients had late side effects. The late side effects were significantly higher in patients with acute toxicity and patients who were treated with external radiotherapy, followed by brachytherapy.

CONCLUSION
The decision of adjuvant therapy and choice of different treatment modalities in terms of a reduced risk of recurrence need to be weighed carefully against the treatment-related morbidity.

Introduction

Endometrial carcinoma is the most common gynecological cancer. About 80% of endometrial cancers are diagnosed at FIGO stage I (International Federation of Gynecology and Obstetrics) and have a favorable prognosis, with an overall survival of up to 90%.[1,2] Surgery consisting of total abdominal hysterectomy and bilateral salpingooophorectomy is the main treatment. However, optimal adjuvant treatment of stage I endometrial carcinoma is currently in dispute despite published results from randomized trials.[3-8] Several postoperative treatment options such as surveillance, external radiotherapy and/or vaginal vault brachytherapy are currently promoted. Even, adjuvant chemotherapy is a current area of active investigation.[9-13]

During external pelvic radiation treatment of endometrial carcinoma, other pelvic organs receive a significant radiation dose, resulting in both acute side effects and late complications.[6,14] Although severe consequences are rare, patients may have treatment-related symptoms associated with bladder, bowel or genitalia sufficient to have a significant effect on quality of life over a 10-year period. [14-16] In addition, there is increasing recognition of the effect of persistent low-grade problems in women. As vagina is the most frequent site of recurrence, vaginal brachytherapy alone can be used with less treatment-related toxicity.[17]

The aim of this retrospective study was to assess the results of postoperative radiotherapy, patterns of failure and late complications in patients with stage I endometrial carcinoma who were treated before 1999.

Methods

Patient characteristics
Between 1978 and 1998, 263 patients with pathological stage I endometrial carcinoma who were treated with postoperative radiotherapy in our department, were retrospectively analyzed. Patients with only adenocarcinoma histology were taken to analyze. We haven’t included patients treated after 1998; because we have changed our treatment protocol and our stage I A-IB, grade 1-2 endometrial cancer patients were included in a multicenter phase III randomized trial.[18]

Patients were evaluated with physical and pelvic examination, routine blood counts, blood chemistry profile including renal and hepatic function tests and chest X-ray. After the year 1989, most patients underwent abdominopelvic computerized tomography and/or pelvic magnetic resonance imaging. Patients were staged according to the FIGO 1988 pathologic staging. The patients who were treated before 1988, they were restaged according to FIGO 1988 staging. The patients’ age ranged from 31 to 83 years, with a median of 57 years. The patient characteristics are summarized in Table 1.

Table 1: Patient characteristics

Treatment
A simple hysterectomy was performed in 229 patients and 34 patients underwent radical hysterectomy. Peritoneal cytology was examined in 47 (17.9%) patients. All patients were evaluated according to indication of adjuvant radiotherapy. One hundred and ninety-seven (74.9%) patients were treated with external pelvic radiotherapy followed by vaginal brachytherapy and 45 patients (17.1%) were treated with only external pelvic irradiation. Remaining 21 (8%) patients treated with vaginal cuff irradiation alone. Patients treated with both external and intracavitary radiotherapy, were initially treated with external pelvic irradiation.

In external pelvic radiotherapy, standard pelvic fields were used. The field borders extend from the L4-L5 interspace to the obturator foramen. Laterally, the fields extend 1.5 to 2.0 cm from the widest plane of the true pelvis. The radiotherapy technique consisted of an anterior and posterior pair in 195 (74.1%) patients, a four-field box technique (anteroposterior, posteroanterior, and two lateral fields) in 47 (17.9%) patients. During external irradiation, midline shielding was not used. The radiation dose was specified at the patient’s midplane or at the isocentre of the fields. The total pelvic dose was median 50.4 Gy (45-54 Gy) with a daily dose of 1.8-2 Gy. In external pelvic irradiation, Co60 teletherapy device or 18 MV photons of linear accelerator were used.

Low-dose-rate radium source was used in intracavitary applications until the 1981; high-dose rate accelerated Curietron Co60 afterloading system has been used from that date on. Vaginal cuff HDR irradiation was performed in 215 (98.6%) patients. Each implant was performed at one week intervals. The vaginal cuff irradiation was performed with Fletcher-Suit HDR colpostats or vaginal cylinder. Patients treated with HDR brachytherapy each received three fractions of 8 Gy and the dose specified at 0.5 cm from the surface of the applicator.

Follow-up
During radiotherapy treatment, all patients were routinely reviewed once a week and patients underwent weekly blood tests. After the treatment, patients were seen monthly to assess acute reactions. Then, all patients were followed regularly with physical and pelvic examination every 3 months for 2 years, every 6 months between 3 and 5 years, and yearly thereafter. Chest X-rays, routine blood chemistry profiles were repeated in every 6 months. In the suspicious of the recurrence and/or metastases, other radiological examinations were required. Vaginal smears or biopsy samples were taken on indication. Loco-regional recurrences were confirmed by a biopsy sample. Acute and late toxic effects of radiotherapy were scored according to the Radiation Therapy Oncology Group/European Organization for Research and Treatment of Cancer (RTOG/EORTC) acute and late morbidity criteria.

Prognostic factors and statistical methods
Pelvic and local control, disease free survival and actuarial survival rates were calculated using the Kaplan-Meier method. Differences between curves were compared by the long rank test. Survival was measured from the operation date. Variables were compared using student-t, Mann-Whitney- U or chi-square test according to the variable properties. Univarite and multivariate analysis of prognostic factors were performed using log-rank and Cox regression models, respectively. All reported p-values are based on two-sided tests with p<0.005 taken to be significant.

Results

Survival and patterns of relapse
The median follow-up of all patients was 99 months (range: 12-311 months). Thirteen (%4.9) patients died of cancer, 22 patients (8.4%) died from intercurrent disease. Cardiovascular diseases were the most common cause of intercurrent death. In 3 patients, a metachronous breast cancer was the cause of death. The 5-year local control, diseasefree and actuarial survival rates were 97%, 94% and 95%, respectively. The 10-year local control, disease-free and actuarial survival rates were 96%, 93% and 95%, respectively.

Of 263 patients, 17 (6.5%) had a relapse, and their clinical, pathologic, and treatment characteristics are shown in Table 2. Nine (3.4%) patients had failure in vaginal cuff following treatment. The median time to local progression was 20 months (range: 6-72 months). Among the 9 patients, 5 patients also developed distant metastasis and died of progressive disease. Four patients had a isolated vaginal cuff recurrence and 2 of them had not received brachytherapy. Two patients with isolated vaginal relapse died due to intercurrent disease (cardiac, traffic accident). The other two patients were treated with chemotherapy and salvage surgery respectively and still alive at last follow-up. There was no isolated pelvic lymph node recurrence.

Table 2: Clinicopathologic features of 17 patients with treatment failure

Distant metastasis was noted in 13 (4.9%) patients after median 21 months (range: 9-35 months). Among 13 patients, 9 of them had stage IC disease. The most common sites of distant relapse were the lung in 8 patients, omentum in 7 patients. All patients with omentum metastasis had received pelvic external radiotherapy and 5 of them had stage IC, 4 of them had grade 3 disease. All patients with metastases died with disease.

Univariate analysis
Prognostic factors that might influence local control, disease free survival and actuarial survival were subjected to univariate analysis. These factors included age (≥60 years vs. <60 years), grade, stage, myometrial invasion, treatment type, time to radiotherapy after surgery, external treatment time, duration between external and intracavitary irradiation. However, no factor significantly influences 10-year pelvic and local control, disease-free and actuarial survival rates.

Acute and late side effects
Among the 263 patients, acute radiation side effects were documented in 116 (44.1%) patients. The majority of patients developed acute grade 1 skin reactions (22%) and grade 1 gastrointestinal tract side effects (20.9%). Grade 3 gastrointestinal toxicity was detected in 2 patients and grade 3 skin reactions was seen in 3 (1.1%) patients and all of them treated with external radiotherapy with Co60 machine. Acute complications are shown in Table 3.

Table 3: Incidence of acute side effects

Fifty-five (20.9%) patients had late side effects. The median time to the development of late complications was 22 month (6-84 months). The most common late side effect was in the gastrointestinal tract (Table 4). There was one case of grade 3 radiation gastrointestinal tract toxicity. Grade 3 skin fibrosis developed in two patients, and both of them had received 54 Gy radiotherapy to the pelvic region with anterior-posterior fields. There was no significant relation between age, radiotherapy technique, type of surgery and the risk of late side effects. However, as seen in Table 5, patients who were treated with external pelvic irradiation followed by vaginal brachytherapy had higher rates of late complications than patients being treated with external pelvic radiotherapy or vaginal brachytherapy alone (p=0.004) (Fig. 1). The other prognostic factor predisposing for the risk of late complications was the occurrence of acute radiotherapy side effects. The 5-year late complication rate was lower in patients without acute radiotherapy toxicity, in contrast to in patients with acute radiotherapy toxicity (p=0.0001) (Table 5).

Table 4: Incidence of late side effects

Fig 1: Complication rate among different adjuvant treatment groups (p=0.004).
ERT: External pelvic radiotherapy; VBT: Vaginal brachytherapy.

Table 5: Association of patient and treatment variables with risk of late toxicity for patients treated with RT

Discussion

Surgery is the mainstay of the treatment of stage I endometrial carcinoma, consisting of a total abdominal hysterectomy with bilateral salpingooophorectomy and peritoneal washings. Nevertheless, extent and impact of pelvic and para-aortic lymphadenectomy or sampling is widely debated. Although determination of patients with nodal involvement has significant prognostic and therapeutic implications; most authors support evaluation of lymph nodes for patients with moderate and high-risk primary features, which are deep myometrial invasion, cervical or isthmus involvement, high-grade lesions, and capillary-space invasion. [19-21] Recently, a large randomized controlled trial, A Study in the Treatment of Endometrial Cancer (ASTEC), showed that systematic lymphadenectomy does not improve overall survival or disease specific survival.[22] Our study included patients who had complete surgical staging and those who did not. In this study, type of surgery did not significantly influence the rate of recurrence. Also, peritoneal cytology was examined in only 17.9% of our patients as peritoneal washing sampling has not been standard in these years. However, peritoneal cytology positivity or negativity no longer alter the staging in the 2008 FIGO and 2010 AJCC staging systems.

Numerous studies have demonstrated that age, depth of myometrial invasion, histology subtypes, histologic grade, cervical involvement, lymphovascular space involvement, nodal involvement can predict recurrence and survival in patients with endometrial cancer.[3,4,19,20,23-25] Although there are national and international variations in the definition of intermediate and high risk, based on these histopathological findings patients are classified into 3 risk groups (low, intermediate, or high) and adjuvant therapy can be modified on the basis of the estimated risk for recurrence. In our study, no factor significantly influences pelvic and local control, disease-free and actuarial survival rates. This might be due to most of (75%) our patients received pelvic radiotherapy followed by vaginal brachytherapy.

There have been controversies concerning the indications and types of adjuvant radiation therapy for stage I endometrial cancer. Recently, randomized studies (NHR, PORTEC 1 & 2, GOG 99, MRC, NCIC) regarding adjuvant radiotherapy for early-stage endometrial cancers were performed. [3-8,18] GOG 99 and PORTEC-1 trials compared pelvic external radiotherapy with no additional treatment after surgery. In these series, the locoregional recurrence rate was significantly lower in the pelvic irradiation group versus no adjuvant therapy group. Also, it has been shown that most locoregional recurrences were detected in the vaginal vault in the group receiving no additional treatment.[3,5] Medical Research Council (MRC) and the National Cancer Institute of Canada (NCIC) trial, 905 women with intermediate-risk or highrisk features were randomly assigned to immediate external radiotherapy or no radiotherapy until clinically indicated.[6] Brachytherapy was given to 50% of patients regardless of the EBRT allocation. However, the significant reduction in local recurrence would not justify its use as that may be reduced by brachytherapy. This pattern and the more favorable toxicity profile of vaginal brachytherapy suggest that brachytherapy alone may be a reasonable approach. For these reasons, many authors advocate radiation with vaginal brachytherapy alone. The randomized prospective study by Aalders et al.[4] compared vaginal brachytherapy to combination vaginal brachytherapy and external radiation therapy. This study showed the efficacy of pelvic external beam radiation therapy for patients who have >50% myometrial invasion or grade 3 cancers. However, the major criticism of the study is that the analysis was on patients who were surgically unstaged, and the study had a much higher incidence of stage I grade 3 cancers (34.4%) compared to that noted in most other surgical series (7% to 18%).[5,20,26] Beside this, GOG 99 trial showed us that nearly one-third of the pelvic failures in the surgery alone arm were in the lateral pelvis, and thus would not have been prevented with vaginal brachytherapy alone.[5] However, open-label, noninferiority, randomized PORTEC-2 trial showed that vaginal brachytherapy is as effective as pelvic external beam radiotherapy, with fewer adverse effects in patients with endometrial carcinoma of high-intermediate risk.[7,17] Although, none of these above randomized studies showed a significant improvement in survival, adjuvant therapy spares these patients the psychological stress of recurrence and the morbidity of intensive treatment of relapse. Nevertheless, there is no evidence to support benefit from any form of adjuvant radiotherapy in low-risk patients.[18,20]

Clinical stage I disease has recently emerged in the form of a meta-analysis of five randomised trials of adjuvant radiotherapy.[27] The results indicate that there is no survival advantage for adjuvant radiotherapy in low risk and intermediate risk disease. Adjuvant radiotherapy is associated with side effects and worse overall survival in this group. As most pelvic recurrences can be cured with radiotherapy in radiation naive patients, the benefit of adjuvant radiotherapy in this group of women is outweighed by the risks.[28] In contrast, the metaanalysis showed a 10% survival advantage for adjuvant radiotherapy in high risk disease (IC grade 3).

The 5-year local control, disease-free and actuarial survival rates of 97%, 93% and 95%, respectively, for the stage I patients of our study are comparable with the results of previous reports. It has been confirmed that 68% to 100% of recurrences occur within the first 3 years of diagnosis.[29] In our series, 94% of locoregional or distant relapses were seen in first 3 years. Radiation therapy, either external alone or combined with vaginal brachytherapy, seems to lower the incidence of local recurrence, but allows the distant disease to manifest itself first especially in high-risk patients.[29] Although we were very successful in maintaining locoregional control, there was a 3% isolated and 4.9% overall distant failure rate. This is consistent with the literature where the risk of distant failure ranges from 4-12%[4,30-33] and the risk of isolated distant failure is 4-6%.[31] Peritoneal relapse within 5 years of simple hysterectomy occurred in 7 women and 5 of them had stage IC disease. So, recently randomized studies[9,13] for adjuvant systemic chemotherapies have therefore been developed in high risk patients since extrapelvic recurrence cannot be prevented by pelvic radiation, as reported by Creutzberg et al.[14] and other investigators.[4-6,30,34]

Since stage I endometrial cancer have an excellent outcome, many women with endometrial adenocarcinoma live for many years with the consequences of treatment related toxicity.[14,15,35,36] In the literature, late grade 1-2 radiation toxicity rate of 8-23% was reported after vaginal brachytherapy and 25-45% after pelvic radiotherapy followed by vaginal cuff irradiation.[32,36,37] It has been shown that the rate of gastrointestinal side effects was more severe and more frequent in the pelvic irradiation group after pelvic lymphadenectomy or lymph node sampling in both the PORTEC study[3,14] and the GOG study.[5] Similar to the literature, our complication rates are dose dependent and are higher for the combination of pelvic radiotherapy and vaginal brachytherapy than for pelvic radiotherapy or vaginal brachytherapy alone. [17,30,32,35,38,39] Although commonly used in the past, nowadays the combined use of both pelvic radiotherapy and vaginal brachytherapy has been used very rare cases since it simply increases the risk of toxicity, without improving pelvic control in stage I endometrial carcinoma.[39,40]

Postoperative brachytherapy alone is recommended to reduce the risk of vaginal cuff recurrence with less toxicty in women with intermediate-risk disease in both retrospective and randomized studies.[7,17,21,26,38,41-44] Chadha et al.[41] reported success with vaginal brachytherapy alone and no grade 3 or 4 toxicity was detected. Fanning[21] designed a prospective evaluation of intermediate risk endometrial cancer treated with full lymphadenectomy and brachytherapy without pelvic radiotherapy. In this study, progression-free survival was 97% at a median follow-up of 4.4 years and with 6% major complication rate. Orr et al.[26] reported a 4% recurrence rate with minimal morbidity.

Treatment related factors that are related to the risk of complications are treatment volume, daily fractionation, radiotherapy technique.[15,20,37,39] We could not find significant relation between age, radiotherapy technique and equipment, type of surgery and the risk of late side effects. Furthermore, Creutzberg et al.[14] and Weiss et al.[45] found that; patients with acute side effects had a higher risk of late complications than patients without acute side effects. This observation was confirmed in our study: the presence of acute treatment-related symptoms was the important significant risk factor for late complications.

In conclusion, the benefit of adjuvant therapy in terms of a reduced risk of recurrence needs to be weighted carefully against the treatment related morbidity when deciding on treatment protocols for stage I endometrial carcinoma. Individual patient, the tumor characteristics should be considered. If administered, the least aggressive and modern radiotherapy approaches (conformal, intensity modulated radiotherapy-IMRT) should be used to reduce the rate of both acute and late side effects.

References

1) Kucera H, Vavra N, Weghaupt K. Benefit of external irradiation in pathologic stage I endometrial carcinoma: a prospective clinical trial of 605 patients who received postoperative vaginal irradiation and additional pelvic irradiation in the presence of unfavorable prognostic factors. Gynecol Oncol 1990;38(1):99-104.

2) Greenlee RT, Hill-Harmon MB, Murray T, Thun M. Cancer statistics, 2001. CA Cancer J Clin 2001;51(1):15-36.

3) Creutzberg CL, van Putten WL, Koper PC, Lybeert ML, Jobsen JJ, Wárlám-Rodenhuis CC, et al. Surgery and postoperative radiotherapy versus surgery alone for patients with stage-1 endometrial carcinoma: multicentre randomised trial. PORTEC Study Group. Post Operative Radiation Therapy in Endometrial Carcinoma. Lancet 2000;355(9213):1404-11.

4) Aalders J, Abeler V, Kolstad P, Onsrud M. Postoperative external irradiation and prognostic parameters in stage I endometrial carcinoma: clinical and histopathologic study of 540 patients. Obstet Gynecol 1980;56(4):419-27.

5) Keys HM, Roberts JA, Brunetto VL, Zaino RJ, Spirtos NM, Bloss JD, et al. A phase III trial of surgery with or without adjunctive external pelvic radiation therapy in intermediate risk endometrial adenocarcinoma: a Gynecologic Oncology Group study. Gynecol Oncol 2004;92(3):744-51.

6) ASTEC/EN.5 Study Group, Blake P, Swart AM, Orton J, Kitchener H, Whelan T, et al. Adjuvant external beam radiotherapy in the treatment of endometrial cancer (MRC ASTEC and NCIC CTG EN.5 randomised trials): pooled trial results, systematic review, and meta- analysis. Lancet 2009;373(9658):137-46.

7) Nout RA, Smit VT, Putter H, Jürgenliemk-Schulz IM, Jobsen JJ, Lutgens LC, et al. Vaginal brachytherapy versus pelvic external beam radiotherapy for patients with endometrial cancer of high-intermediate risk (PORTEC-2): an open-label, non-inferiority, randomised trial. Lancet 2010;375(9717):816-23.

8) Scholten AN, van Putten WL, Beerman H, Smit VT, Koper PC, Lybeert ML, et al. Postoperative radiotherapy for Stage 1 endometrial carcinoma: long-term outcome of the randomized PORTEC trial with central pathology review. Int J Radiat Oncol Biol Phys 2005;63(3):834-8.

9) Morrow CP, Bundy BN, Homesley HD, Creasman WT, Hornback NB, Kurman R, et al. Doxorubicin as an adjuvant following surgery and radiation therapy in patients with high-risk endometrial carcinoma, stage I and occult stage II: a Gynecologic Oncology Group Study. Gynecol Oncol 1990;36(2):166-71.

10) Maggi R, Lissoni A, Spina F, Melpignano M, Zola P, Favalli G, et al. Adjuvant chemotherapy vs radiotherapy in high-risk endometrial carcinoma: results of a randomised trial. Br J Cancer 2006;95(3):266-271.

11) Susumu N, Sagae S, Udagawa Y, Niwa K, Kuramoto H, Satoh S, Kudo R. Randomized phase III trial of pelvic radiotherapy versus cisplatin-based combined chemotherapy in patients with intermediate- and high-risk endometrial cancer: a Japanese Gynecologic Oncology Group study. Gynecol Oncol 2008;108 (1):226-233.

12) Greven K, Winter K, Underhill K, Fontenesci J, Cooper J, Burke T. Final analysis of RTOG 9708: adjuvant postoperative irradiation combined with cisplatin/paclitaxel chemotherapy following surgery for patients with high-risk endometrial cancer. Gynecol Oncol 2006;103(1):155-9.

13) National Cancer Institute. PORTEC 3. Available from: http://www.cancer.gov/search/ViewClinicalTrials.aspx ?cdrid=521447&protocolsearchid=4206096&version= healthprofessional (2006).

14) Creutzberg CL, van Putten WL, Koper PC, Lybeert ML, Jobsen JJ, Wárlám-Rodenhuis CC, et al. The morbidity of treatment for patients with Stage I endometrial cancer: results from a randomized trial. Int J Radiat Oncol Biol Phys 2001;51(5):1246-55.

15) Corn BW, Lanciano RM, Greven KM, Noumoff J, Schultz D, Hanks GE, et al. Impact of improved irradiation technique, age, and lymph node sampling on the severe complication rate of surgically staged endometrial cancer patients: a multivariate analysis. J Clin Oncol 1994;12(3):510-5.

16) Andreyev J. Gastrointestinal symptoms after pelvic radiotherapy: a new understanding to improve management of symptomatic patients. Lancet Oncol 2007;8(11):1007-17.

17) Nout RA, Putter H, Jürgenliemk-Schulz IM, Jobsen JJ, Lutgens LC, van der Steen-Banasik EM, et al. Quality of life after pelvic radiotherapy or vaginal brachytherapy for endometrial cancer: first results of the randomized PORTEC-2 trial. J Clin Oncol 2009;27(21):3547-56.

18) Sorbe B, Nordström B, Mäenpää J, Kuhelj J, Kuhelj D, Okkan S, et al. Intravaginal brachytherapy in FIGO stage I low-risk endometrial cancer: a controlled randomized study. Int J Gynecol Cancer 2009;19(5):873-8.

19) Creasman WT, Morrow CP, Bundy BN, Homesley HD, Graham JE, Heller PB. Surgical pathologic spread patterns of endometrial cancer. A Gynecologic Oncology Group Study. Cancer 1987;60(8 Suppl):2035-41.

20) Morrow CP, Bundy BN, Kurman RJ, Creasman WT, Heller P, Homesley HD, et al. Relationship between surgical-pathological risk factors and outcome in clinical stage I and II carcinoma of the endometrium: a Gynecologic Oncology Group study. Gynecol Oncol 1991;40(1):55-65.

21) Fanning J. Long-term survival of intermediate risk endometrial cancer (stage IG3, IC, II) treated with full lymphadenectomy and brachytherapy without teletherapy. Gynecol Oncol 2001;82(2):371-4.

22) ASTEC study group, Kitchener H, Swart AM, Qian Q, Amos C, Parmar MK. Efficacy of systematic pelvic lymphadenectomy in endometrial cancer (MRC ASTEC trial): a randomised study. Lancet 2009;373(9658):125-36.

23) Greven KM, Corn BW, Case D, Purser P, Lanciano RM. Which prognostic factors influence the outcome of patients with surgically staged endometrial cancer treated with adjuvant radiation? Int J Radiat Oncol Biol Phys 1997;39(2):413-8.

24) DiSaia PJ, Creasman WT, Boronow RC, Blessing JA. Risk factors and recurrent patterns in Stage I endometrial cancer. Am J Obstet Gynecol 1985;151(8):1009-15.

25) Tornos C, Silva EG, el-Naggar A, Burke TW. Aggressive stage I grade 1 endometrial carcinoma. Cancer 1992;70(4):790-8.

26) Orr JW Jr, Holimon JL, Orr PF. Stage I corpus cancer: is teletherapy necessary? Am J Obstet Gynecol 1997;176(4):777-89.

27) Johnson N, Cornes P. Survival and recurrent disease after postoperative radiotherapy for early endometrial cancer: systematic review and meta-analysis. BJOG 2007;114(11):1313-20.

28) Creutzberg CL, van Putten WL, Koper PC, Lybeert ML, Jobsen JJ, Wárlám-Rodenhuis CC, et al. Survival after relapse in patients with endometrial cancer: results from a randomized trial. Gynecol Oncol 2003;89(2):201-9.

29) Fung-Kee-Fung M, Dodge J, Elit L, Lukka H, Chambers A, Oliver T, et al. Follow-up after primary therapy for endometrial cancer: a systematic review. Gynecol Oncol 2006;101(3):520-9.

30) Carey MS, O’Connell GJ, Johanson CR, Goodyear MD, Murphy KJ, Daya DM, et al. Good outcome associated with a standardized treatment protocol using selective postoperative radiation in patients with clinical stage I adenocarcinoma of the endometrium. Gynecol Oncol 1995;57(2):138-44.

31) Rush S, Gal D, Potters L, Bosworth J, Lovecchio J. Pelvic control following external beam irradiation for surgical stage I endometrial adenocarcinoma. Int J Radiat Oncol Biol Phys 1995;33(4):851-4.

32) Irwin C, Levin W, Fyles A, Pintilie M, Manchul L, Kirkbride P. The role of adjuvant radiotherapy in carcinoma of the endometrium-results in 550 patients with pathologic stage I disease. Gynecol Oncol 1998;70(2):247-54.

33) Podczaski E, Kaminski P, Gurski K, MacNeill C, Stryker JA, Singapuri K, et al. Detection and patterns of treatment failure in 300 consecutive cases of “early” endometrial cancer after primary surgery. Gynecol Oncol 1992;47(3):323-7.

34) Elliott P, Green D, Coates A, Krieger M, Russell P, Coppleson M, et al. The efficacy of postoperative vaginal irradiation in preventing vaginal recurrence in endometrial cancer. Int J Gynecol Cancer 1994;4(2):84-93.

35) Greven KM, Lanciano RM, Herbert SH, Hogan PE. Analysis of complications in patients with endometrial carcinoma receiving adjuvant irradiation. Int J Radiat Oncol Biol Phys 1991;21(4):919-23.

36) MacLeod C, Fowler A, Duval P, D’Costa I, dalrymple C, Elliot P, et al. Adjuvant high-dose rate brachytherapy with or without external beam radiotherapy posthysterectomy for endometrial Cancer. Int J Gynecol Cancer 1999;9(3):247-55.

37) Jereczek-Fossa B, Jassem J, Nowak R, and Badzio A. Late complications after postoperative radiotherapy in endometrial cancer: Analysis of 317 consecutive cases with application of linear-quadratic model. Int J Radiat Oncol Biol Phys 1998;41(2):329-38.

38) Alektiar KM, Venkatraman E, Chi DS, Barakat RR. Intravaginal brachytherapy alone for intermediaterisk endometrial cancer. Int J Radiat Oncol Biol Phys 2005;62(1):111-7.

39) Randall ME, Wilder J, Greven K, Raben M. Role of intracavitary cuff boost after adjuvant external irradiation in early endometrial carcinoma. Int J Radiat Oncol Biol Phys 1990;19(1):49-54.

40) Weiss MF, Connell PP, Waggoner S, Rotmensch J, Mundt AJ. External pelvic radiation therapy in stage IC endometrial carcinoma. Obstet Gynecol 1999;93(4):599-602.

41) Chadha M, Nanavati P, Liu P, Fanning J, Jacobs A. Patterns of failure in endometrial carcinoma stage IB grade 3 and IC patients treated with vaginal cuff brachytherapy alone. Gynecol Oncol 1999;75(1):103-7.

42) Roper B, Astner ST, Heydemann-Obradovic A, Thamm R, Jacob V, Hölzel D,et al. Ten-year data on 138 patients with endometrial carcinoma and postoperative vaginal brachytherapy alone: no need for external-beam radiotherapy in low and intermediate risk patients. Gynecol Oncol 2007;107(3):541-8.

43) Anderson JM, Stae B, Hallum AV, Rogoff E, Childers J. High dose rate postoperative vaginal cuff irradiation alone for stage IB and IC endometrial cancer. Int J Radiat Oncol Biol Phys 2000;46(2):417-25.

44) Lin LL, Mutch DG, Rader JS, Powell MA, Grigsby PW. External radiotherapy versus vaginal brachytherapy for patients with intermediate risk endometrial cancer. Gynecol Oncol 2007;106(1):215-20.

45) Weiss E, Hirnle P, Arnold-Bofinger H, Hess CF, Bamberg M. Therapeutic outcome and relation of acute and late side effects in the adjuvant radiotherapy of endometrial carcinoma stage I and II. Radiother Oncol 1999;53(1):37-44.