**2. Radiation therapy for endometrial cancer**

In Europe and the US, the postoperative therapy most commonly used for intermediate-risk patients with advanced endometrial cancer or early-stage cancer who are at risk of recurrence is mainly radiation therapy4). In Japan, on the other hand, chemotherapy is often chosen as a postoperative therapy, and radiation therapy is performed only for limited cases. Radiation therapy is indicated as an option for initial treatment only when surgery would be difficult to perform from a practical perspective, such as in advanced cases that are considered inoperable, and in cases where surgery is considered a high-risk procedure because of serious complications, obesity, or other reasons5). The following types of radiation therapy can be used for endometrial cancer following a hysterectomy. (1)Vaginal brachytherapy: A radioactive source for brachytherapy is inserted into the vagina and left there for two to three days. (2)External-beam radiation therapy (EBRT): Tumors are exposed to radiation from outside the body.

There are two kinds of EBRT: whole abdominal irradiation (WAI) and whole pelvic irradiation (WPI). WAI or WPI is usually carried out as postoperative radiation therapy and is sometimes accompanied by vaginal brachytherapy.

The effects of postoperative radiation therapy on intermediate-risk cases of early-stage endometrial cancer have been studied in comparison with groups observed over time in the absence of postoperative treatment in NRH6), PORTEC7), GOG-998). Although these reports are from different regions, they all showed the same results. Specifically, the effect in suppressing local recurrence was significantly better in the radiation therapy groups, but radiation did not significantly prolong progression-free survival (PFS) or overall survival (OS).

A study on the effects of postoperative (adjuvant) EBRT on outcome in patients with earlystage endometrial cancer was recently reported in The Lancet9). Out of 905 patients with early-stage cancer in seven countries that had been enrolled in the ASTEC and EN.5 studies, intermediate to high-risk patients who had undergone surgery for endometrial cancer were randomly assigned to an observation or an EBRT group. The risk of developing distant metastasis based on the PORTEC and GOG99 data, where a high risk was defined as "all papillary serous and clear cell subtypes, all other subtypes in IC (grade 3) and IIA (grade 3), and all patients with stage IIB", and intermediate risk was defined as "subtypes other than papillary serous and clear cell histology within stage IA and IB (grade 3) and stage IC and IIA (grades 1 and 2)." The results of an analysis revealed that, after 58 months of follow up, the hazard ratio (HR) for death was 1.05 (95% CI, 0.75 to 1.48; *P* = 0.77) in 68 out of 453 subjects in the group observed over time and in 67 out of 452 subjects in the EBRT group, indicating no difference in OS. There was also no significant difference in terms of recurrence-free survival (RFS), with a HR of 0.93 (95% CI, 0.66 to 1.31; *P* = 0.68). The incidence of distant recurrence was also the same (8% in the observation group and 9% in the EBRT group), but the HR of 0.46 (95% CI, 0.24 to 0.89; *P* = 0.02) for vaginal or pelvic initial recurrence indicated that local recurrence was suppressed in the EBRT group. However, since these numbers do not include cases of distant metastasis or simultaneous local recurrence/distant metastasis, which account for 65% of recurrences, the overall outcome was not considered to have improved. The development of acute toxicity was also higher in the EBRT group, with a rate of 43% compared to the rate of 27% in the group without radiation therapy.

A meta-analysis9) of 2011 cases comprising the PORTEC and GOG99 data was performed in addition to the above ASTEC and EN.5 data. The HR for OS was 1.04 (95% CI, 0.84 to 1.29; *P*  = 0.38), indicating no significant differences depending on whether or not adjuvant EBRT was performed. A sub-analysis divided the patients into what the authors termed intermediate risk and high risk also revealed no significant differences in OS between the ASTEC+EN.5 and the ASTEC+EN.5+PORTEC+GOG99 data.

Because adjuvant EBRT thus failed to improve survival and also resulted in adverse effects in early-stage endometrial cancer patients who had a risk of recurrence, the authors concluded that such treatment could not be recommended for patients with early-stage endometrial cancer.

## **3. Chemotherapy for advanced or recurrent endometrial cancer**

Although adjuvant EBRT can be expected to be effective to a certain extent for advanced or recurrent endometrial cancer, chemotherapy with anti-tumor agents is also being additionally performed in Europe and the US. After many changes in regimens, AP therapy

There are two kinds of EBRT: whole abdominal irradiation (WAI) and whole pelvic irradiation (WPI). WAI or WPI is usually carried out as postoperative radiation therapy and

The effects of postoperative radiation therapy on intermediate-risk cases of early-stage endometrial cancer have been studied in comparison with groups observed over time in the absence of postoperative treatment in NRH6), PORTEC7), GOG-998). Although these reports are from different regions, they all showed the same results. Specifically, the effect in suppressing local recurrence was significantly better in the radiation therapy groups, but radiation did not

A study on the effects of postoperative (adjuvant) EBRT on outcome in patients with earlystage endometrial cancer was recently reported in The Lancet9). Out of 905 patients with early-stage cancer in seven countries that had been enrolled in the ASTEC and EN.5 studies, intermediate to high-risk patients who had undergone surgery for endometrial cancer were randomly assigned to an observation or an EBRT group. The risk of developing distant metastasis based on the PORTEC and GOG99 data, where a high risk was defined as "all papillary serous and clear cell subtypes, all other subtypes in IC (grade 3) and IIA (grade 3), and all patients with stage IIB", and intermediate risk was defined as "subtypes other than papillary serous and clear cell histology within stage IA and IB (grade 3) and stage IC and IIA (grades 1 and 2)." The results of an analysis revealed that, after 58 months of follow up, the hazard ratio (HR) for death was 1.05 (95% CI, 0.75 to 1.48; *P* = 0.77) in 68 out of 453 subjects in the group observed over time and in 67 out of 452 subjects in the EBRT group, indicating no difference in OS. There was also no significant difference in terms of recurrence-free survival (RFS), with a HR of 0.93 (95% CI, 0.66 to 1.31; *P* = 0.68). The incidence of distant recurrence was also the same (8% in the observation group and 9% in the EBRT group), but the HR of 0.46 (95% CI, 0.24 to 0.89; *P* = 0.02) for vaginal or pelvic initial recurrence indicated that local recurrence was suppressed in the EBRT group. However, since these numbers do not include cases of distant metastasis or simultaneous local recurrence/distant metastasis, which account for 65% of recurrences, the overall outcome was not considered to have improved. The development of acute toxicity was also higher in the EBRT group, with a rate of 43% compared to the rate of 27% in the group

A meta-analysis9) of 2011 cases comprising the PORTEC and GOG99 data was performed in addition to the above ASTEC and EN.5 data. The HR for OS was 1.04 (95% CI, 0.84 to 1.29; *P*  = 0.38), indicating no significant differences depending on whether or not adjuvant EBRT was performed. A sub-analysis divided the patients into what the authors termed intermediate risk and high risk also revealed no significant differences in OS between the

Because adjuvant EBRT thus failed to improve survival and also resulted in adverse effects in early-stage endometrial cancer patients who had a risk of recurrence, the authors concluded that such treatment could not be recommended for patients with early-stage

Although adjuvant EBRT can be expected to be effective to a certain extent for advanced or recurrent endometrial cancer, chemotherapy with anti-tumor agents is also being additionally performed in Europe and the US. After many changes in regimens, AP therapy

ASTEC+EN.5 and the ASTEC+EN.5+PORTEC+GOG99 data.

**3. Chemotherapy for advanced or recurrent endometrial cancer** 

significantly prolong progression-free survival (PFS) or overall survival (OS).

is sometimes accompanied by vaginal brachytherapy.

without radiation therapy.

endometrial cancer.

(combining doxorubicin and cisplatin) is currently the standard therapy. The changes in regimens are summarized below.

From the 1970s to the 1980s, doxorubicin monotherapy was reported to result in a response rate of 20% to 42%10), and a good response rate of 45% to 60% was reported in a subsequent phase II study combining cisplatin with doxorubicin11). These two drugs therefore came to be positioned as key drugs in chemotherapy for endometrial cancer. In the 1990s, the Gynecologic Oncology Group (GOG) in the US and the European Organization for Research and Treatment of Cancer (EORTC) conducted phase III randomized comparative studies on "doxorubicin vs. doxorubicin + cisplatin (AP therapy)" in both the GOG10712) and EORTC5587213) trials, respectively, and the response rates of 25% vs. 42% in the GOG107 study and 43% vs. 17% in the EORTC55872 study demonstrated the efficacy of AP therapy. Although no significant differences in OS were found in the GOG-107 study, AP therapy was shown to be superior in the EORTC55872 study. On the other hand, CAP (cyclophosphamide + doxorubicin + cisplatin) therapy is also being used for endometrial cancer in Japan, where chemotherapy is more often performed as a postoperative therapy5). However, cyclophosphamide was not found to result in significant differences in the response rate in phase II studies of CAP therapy and AP therapy14), while the GOG48 study on "doxorubicin vs. doxorubicin + cyclophosphamide (AC therapy)" also revealed no significant differences in the response rate, response period, or OS, thus contradicting the usefulness of concomitant cyclophosphamide for endometrial cancer15);AP therapy has come to be acknowledged as the standard chemotherapy for endometrial cancer in Japan as well.

Radiation therapy and chemotherapy are thus the primary modalities of therapy that should be used after surgery for endometrial cancer. However, the following three questions still need to be answered:


#### **4. Radiation therapy vs. chemotherapy as adjuvant therapy for endometrial cancer**

Three randomized studies have compared radiation therapy and chemotherapy as adjuvant therapies for endometrial cancer (Table 1).

#### **4.1 GOG122**

The GOG12216), reported in the US in 2006, was a randomized study comparing WAI and AP therapy as first-line therapies for stage III and IV cases with residual tumors no greater than 2 cm after surgery. The HR for progression adjusted for stage was 0.71, favoring AP therapy (95% CI, 0.55 to 0.91; *P* < 0.01). At 60 months, 50% of the patients receiving AP were predicted to be alive and disease-free after adjustments for stage, compared with 38% of patients receiving WAI. The stage-adjusted death HR was 0.68 (95% CI, 0.52 to 0.89; *P* < 0.01), favoring AP therapy. Moreover, at 60 months and after adjustments for stage, 55% of the AP patients were predicted to be alive, compared with 42% of the WAI patients. The PFS and OS were both significantly higher in the AP arm, but greater acute toxicity was seen in the


a: significantly better

Table 1. Randomized trials comparing radiation therapy and chemotherapy as an adjuvant therapy for endometrial cancer.

AP arm. Treatment probably contributed to the deaths of 8 patients (4%) in the AP arm and 5 patients (2%) in the WAI arm, indicating that AP therapy was associated with a somewhat stronger toxicity. However, in view of the survival data, AP chemotherapy appeared to be better than radiation therapy as a first-line postoperative therapy for advanced endometrial cancer. This was the first trial to reveal the positive effects of chemotherapy over radiation therapy. A subgroup analysis revealed that significantly lower HRs regarding OS were recognized in patients younger than 60 years old, cases with microscopic residual tumors, cases with a pathological subtype of endometrioid adenocarcinoma, and stage III cases. After the results of this study were reported, chemotherapy tended to be more often incorporated into adjuvant therapy for endometrial cancer.

#### **4.2 Italian study**

170 Cancer of the Uterine Endometrium – Advances and Controversies

Table 1. Randomized trials comparing radiation therapy and chemotherapy as an adjuvant

a: significantly better

therapy for endometrial cancer.

Maggi R et al. 17) reported a multicenter randomized trial comparing five courses of adjuvant chemotherapy with CAP (cyclophosphamide, 600 mg/m2; doxorubicin, 45 mg/m2; and cisplatin, 50 mg/m2) and external radiation therapy (45 Gy) for mainly high-risk endometrial cancer patients, including stage IC grade 3, stage IIA to IIB grade 3 with more than 50% myometrial invasion (stage I/II: 36%), and also stage III disease. The pathological subtype was restricted to endometrioid type. Selective pelvic and paraaortic node sampling were performed; however, the percentage of patients undergoing a lymphadenectomy was not stated. More than 60% of the cases were stage III and had a high risk of recurrence. The 3-, 5-, and 7-year OS rates were 78%, 69% and 62% in the RT group and 76%, 66% and 62% in the CT group. The 3-, 5-, and 7-year PFS rates were 69%, 63%, and 56% and 68%, 63%, and 60%, respectively. This study revealed no significant differences in the OS or the PFS. Radiation therapy delayed local relapses, and CT delayed distant metastases.

#### **4.3 JGOG2033**

In 2008, the Japanese Gynecologic Oncology Group (JGOG) published a paper18) about a randomized phase III trial (JGOG2033) comparing adjuvant chemotherapy with cyclophosphamide (333 mg/m2), doxorubicin (40 mg/m2), and cisplatin (50 mg/m2) (CAP) administered every four weeks for three or more cycles with radiotherapy administered using pelvic EBRT (PRT) at 50 Gy in 385 patients with endometrioid adenocarcinoma and myometrial invasion deeper than 50%, myometrial invasion, most of whom had an intermediate -risk but a small proportion of whom had a high -risk of recurrence after the initial operation for endometrial cancer. No statistically significant differences in the PFS or OS were recognized between the patient groups treated with the two modalities. However, in the high intermediate-risk (HIR) group consisting of (1) patients with stage IC disease who were over 70 years of age and/or had G3 endometrioid adenocarcinoma and (2) patients with stage II or IIIA disease (positive cytology), the CAP treatment was associated with a significantly higher PFS rate (83.8% vs. 66.2%) as well as a higher OS rate (89.7% vs. 73.6%). Adjuvant chemotherapy was emphasized as being a useful alternative to radiotherapy for patients with intermediate-risk endometrial cancer.

In this study, a pelvic lymphadenectomy was performed in 96% of the cases and a paraaortic lymphadenectomy was performed in 29% of the cases; furthermore, the ratio of stage I or II cases was higher (75% vs. 35%) and the ratio of grade 3 tumors was lower (14% vs. 56%). Most of the cases in JGOG2033 study had an intermediate risk, while most of the cases in the Italian study17) had a high risk. Although both of these studies used the CAP regimen, the doses of cyclophosphamide and doxorubicin were lower and the number of chemotherapy cycles was fewer in the JGOG2033 study (Table 2). In fact, the incidence of


a: recurrent tumor

Table 2. Randomized trials comparing chemotherapy regimens as an adjuvant therapy for endometrial cancer.

Table 2. Randomized trials comparing chemotherapy regimens as an adjuvant therapy for

a: recurrent tumor

endometrial cancer.

G3/4 adverse effects was lower in the JGOG2033 study. The CAP regimen in the JGOG2033 study, therefore, represented a more modest therapy than that used in the Italian study. Nevertheless, the 5-year PFS rate and OS rate of the high-intermediate risk (HIR) subgroup of the JGOG2033 study were significantly improved by this modest CAP regimen. This means that the cases in the high-intermediate risk (HIR) subgroup of the JGOG2033 study may be good candidates for answering the question, "Which patients with endometrial cancer may benefit from adjuvant chemotherapy?" To answer this question definitively, further evidence is needed from randomized studies investigating the efficacy of adjuvant chemotherapy designed for patients with intermediate- or high-risk endometrial cancer. The modest adjuvant chemotherapy regimen of CAP was superior to pelvic radiotherapy in HIR patients, as defined above; however, this chemotherapy did not have a sufficient efficacy to improve the prognosis of patients with stage III advanced endometrial cancer.

The Italian study17) revealed no significant differences in the PFS or OS rates among highrisk patients even when a higher-dose CAP regimen was used. The dose of doxorubicin was 60 mg/m2 in the GOG122 study16), 45 mg/m2 in the Italian study, and 40 mg/m2 in the JGOG2033 study18).

#### **4.4 What is the best adjuvant chemotherapy for endometrial cancer?**

Then, what is the best adjuvant chemotherapy for endometrial cancer? First, let me look back to some studies for advanced or recurrent endometrial cancer.

The response rates to paclitaxel in phase II studies for advanced or recurrent endometrial cancer were reported to be 37.5%19) and 30.4%20) in 1996 and 2004, respectively, and the response rates to docetaxel in phase II studies for advanced or recurrent endometrial cancer were reported to be 33%21) and 31.3%22) in 2002 and 2005, respectively. These numbers are comparable to the response rates obtained with doxorubicin alone.

In the GOG163 phase III randomized study23) of AP vs. concomitant doxorubicin + paclitaxel (AT) + G-CSF reported in 2004 on the effects of combining a taxane with doxorubicin or cisplatin, the response rates of 40% vs. 43% revealed no significant differences when compared with the concomitant use of cisplatin, and the median OS was 12.6 months vs.13.6 months, with a HR of 1.00. Furthermore, AT therapy had more disadvantages, such as the need for G-CSF support, compared with AP therapy, and no advantage was found in switching from cisplatin to paclitaxel as the concomitant drug to be used with doxorubicin.

On the other hand, the GOG177 phase III randomized study24) of AP vs. concomitant paclitaxel + doxorubicin + cisplatin (TAP) + G-CSF reported in the same year (2004) showed that the results of TAP therapy were superior, based on response rates of 34% vs. 57%. The median PFS (8.3 months vs. 5.3 months) and the median OS (15.3 months vs. 12.3 months) were significantly improved in the TAP group. However, in the TAP arm, the incidence of neurotoxicity was significantly higher, and congestive heart failure or treatment-related deaths occurred. Compliance was therefore considered to be poor in view of the toxicity, and TAP therapy has not widely replaced AP as a standard therapy in clinical practice.

Based on the results of the GOG163 study, it seemed that the next steps should be to study the significance of replacing doxorubicin, which has been considered a key drug for a long time, with a taxane and to study which of the two platinum agents should be used. There was thus a need to first study whether or not a regimen combining two agents (taxane + platinum agent) would be better than AP. As there are two taxanes and two platinum agents, whether these regimens or AP therapy would be more effective was investigated in Japan.

Out of the various combinations of the two taxanes and two platinum agents, i.e., TC (paclitaxel + carboplatin), DP (docetaxel + cisplatin), DC (docetaxel + carboplatin), and TP (paclitaxel + cisplatin), the efficacy and safety of the TC, DP, and DC regimens were first compared in JGOG2041, a phase II randomized study25) (Table 2). TP therapy had already been eliminated, as the results of clinical trials for ovarian cancer revealed a strong neurotoxicity, and a shift from TP to TC therapy had occurred26-28). The results revealed the response rates of the three regimens to be in no way inferior to AP therapy, and the toxicity was also within an acceptable range25).

Based on the results of the JGOG2041 study, a phase III randomized study (JGOG2043) was conducted to compare AP therapy with chemotherapy combining platinum and taxanes in groups with a high risk for the recurrence of endometrial cancer. The results of the JGOG2041 study revealed the response rate of DC therapy (48%) to be somewhat lower, although not significantly, than that of TC therapy (60%) and DP therapy (52%), and TC and DP therapy were therefore selected for comparison with AP therapy in the JGOG2043 study. The groups with a high risk for the recurrence of endometrial cancer in the JGOG2043 study included advanced cases with residual tumors of no greater than 2 cm, and stage I and II cases with invasion to more than half of the myometrium and histological grade 2 or 3 (including serous or clear cell adenocarcinoma), thus allowing the effects on advanced cases and intermediate risk cases to be analyzed separately using sub-analyses. Enrollment in this study was closed at the end of 2010.

In the phase II study, the TC response rate was 60% and the compliance was high (90%). The response rate of TC is therefore being compared with that of TAP (which had the highest response rate in the GOG177 study but had problems in compliance) in patients with advanced or recurrent cancer. The results of the JGOG2041 study, in conjunction with the results of a comparison of the efficacies of TC, DP, and AP in the JGOG2043 study, should prove to be useful for research on the most effective and appropriate chemotherapy regimens. Randomized studies, such as GOG 209 (TAP vs. TC for advanced or recurrent disease) and JGOG 2043 (AP vs. TC vs. DP for adjuvant therapy) are now underway. The TC regimen is widely used both in practical treatment and in research trials for endometrial cancer, based on the promising efficacies reported by various phase II studies, although no evidence of a phase III trial level that certifies TC as a truly standard regimen for endometrial cancer has been obtained.

Chemotherapy has been the mainstream treatment in Japan, but postoperative therapy in Europe is now shifting from the formerly preferred radiation therapy alone to radiation therapy plus chemotherapy. In the US as well, the GOG194 study (closed) for WAI vs. WAI followed by paclitaxel + doxorubicin + cisplatin (TAP therapy) is being conducted to test the effects of combining chemotherapy with radiation therapy as a postoperative treatment regimen for intermediate-risk or high-risk cases.

#### **5. Comparison of radiation therapy alone and the combination of radiation therapy and chemotherapy**

Several randomized studies have compared radiation therapy alone and the combination of radiation therapy and chemotherapy as an adjuvant therapy for endometrial cancer (Table 3).

#### Adjuvant Chemotherapy for Endometrial Cancer 175

174 Cancer of the Uterine Endometrium – Advances and Controversies

Out of the various combinations of the two taxanes and two platinum agents, i.e., TC (paclitaxel + carboplatin), DP (docetaxel + cisplatin), DC (docetaxel + carboplatin), and TP (paclitaxel + cisplatin), the efficacy and safety of the TC, DP, and DC regimens were first compared in JGOG2041, a phase II randomized study25) (Table 2). TP therapy had already been eliminated, as the results of clinical trials for ovarian cancer revealed a strong neurotoxicity, and a shift from TP to TC therapy had occurred26-28). The results revealed the response rates of the three regimens to be in no way inferior to AP therapy, and the toxicity

Based on the results of the JGOG2041 study, a phase III randomized study (JGOG2043) was conducted to compare AP therapy with chemotherapy combining platinum and taxanes in groups with a high risk for the recurrence of endometrial cancer. The results of the JGOG2041 study revealed the response rate of DC therapy (48%) to be somewhat lower, although not significantly, than that of TC therapy (60%) and DP therapy (52%), and TC and DP therapy were therefore selected for comparison with AP therapy in the JGOG2043 study. The groups with a high risk for the recurrence of endometrial cancer in the JGOG2043 study included advanced cases with residual tumors of no greater than 2 cm, and stage I and II cases with invasion to more than half of the myometrium and histological grade 2 or 3 (including serous or clear cell adenocarcinoma), thus allowing the effects on advanced cases and intermediate risk cases to be analyzed separately using sub-analyses. Enrollment in this

In the phase II study, the TC response rate was 60% and the compliance was high (90%). The response rate of TC is therefore being compared with that of TAP (which had the highest response rate in the GOG177 study but had problems in compliance) in patients with advanced or recurrent cancer. The results of the JGOG2041 study, in conjunction with the results of a comparison of the efficacies of TC, DP, and AP in the JGOG2043 study, should prove to be useful for research on the most effective and appropriate chemotherapy regimens. Randomized studies, such as GOG 209 (TAP vs. TC for advanced or recurrent disease) and JGOG 2043 (AP vs. TC vs. DP for adjuvant therapy) are now underway. The TC regimen is widely used both in practical treatment and in research trials for endometrial cancer, based on the promising efficacies reported by various phase II studies, although no evidence of a phase III trial level that certifies TC as a truly standard regimen for

Chemotherapy has been the mainstream treatment in Japan, but postoperative therapy in Europe is now shifting from the formerly preferred radiation therapy alone to radiation therapy plus chemotherapy. In the US as well, the GOG194 study (closed) for WAI vs. WAI followed by paclitaxel + doxorubicin + cisplatin (TAP therapy) is being conducted to test the effects of combining chemotherapy with radiation therapy as a postoperative treatment

**5. Comparison of radiation therapy alone and the combination of radiation** 

Several randomized studies have compared radiation therapy alone and the combination of radiation therapy and chemotherapy as an adjuvant therapy for endometrial cancer

was also within an acceptable range25).

study was closed at the end of 2010.

endometrial cancer has been obtained.

**therapy and chemotherapy** 

(Table 3).

regimen for intermediate-risk or high-risk cases.



a: sampling of PLN or PAN was not required.

b: significantly better

c: 1) G2/3 with LVSI and outer-third myometrial invasion, 2) age of 50 years or greater in addition to any two factors listed above, or 3) age of 70 years or greater with any risk factor listed above.

Table 3. Randomized trials comparing radiation therapy with combination of radiation therapy and chemotherapy as an adjuvant therapy for endometrial cancer.

#### **5.1 GOG34**

176 Cancer of the Uterine Endometrium – Advances and Controversies

a: sampling of PLN or PAN was not required.

c: 1) G2/3 with LVSI and outer-third myometrial invasion, 2) age of 50 years or greater in addition to any two factors listed above, or 3) age of 70 years or greater with any risk factor listed above. Table 3. Randomized trials comparing radiation therapy with combination of radiation

therapy and chemotherapy as an adjuvant therapy for endometrial cancer.

b: significantly better

This study was the first randomized trial to compare radiation alone and radiation followed by chemotherapy29). The subjects were comprised of patients with clinical stage I or II (occult) disease in whom surgical-pathologic evaluation had revealed one or more risk factors for recurrence: a greater than 50% myometrial invasion, pelvic or aortic node metastasis, cervical involvement, or adnexal metastases. The patients received 50-Gy EBRT with or without paraaortic radiation and were then randomized into two arms: no further therapy or additional doxorubicin (45 – 60 mg/m2) every three weeks to a maximum cumulative dose of 500 mg/m2. No statistically significant difference in the OS or PFS was observed between the two arms. Unfortunately, because of protocol violations, the small sample size, and the number of patients lost to follow-up, this study was unable to determine what effect the use of doxorubicin as an adjuvant therapy had on recurrence, progression, and survival.

#### **5.2 Finnish study**

For the Finnish study30), surgically staged IA-B G3 cases or stage IC-IIIA G1-3 cases were enrolled and randomized to receive pelvic EBRT alone (28 Gy x 2 cycles) or a unique combination of alternating EBRT and chemotherapy, namely, a first cycle of CEP (cyclophosphamide 500 mg/m2; epirubicin, 60 mg/m2; and cisplatin, 50 mg/m2) followed by a first cycle of EBRT (28 Gy), a second cycle of CEP, a second cycle of EBRT (28 Gy), and finally a third cycle of CEP. However, this study failed to reveal an improvement in the OS or PFS by the addition of chemotherapy to radiation therapy. Moreover, adverse events such as severe bowel obstruction requiring surgery tended to occur more frequently in the combined treatment arm.

#### **5.3 GOG 184**

For the GOG184 study31), surgically staged III or IV cases were enrolled and treated with volume-directed irradiation of the pelvic/para-aortic lymph nodes. The patients were subsequently randomized to compare the recurrence-free survival (RFS) and toxicity between two chemotherapy regimens. Treatment was randomized between six cycles of cisplatin (50 mg/m2) and doxorubicin (45 mg/m2) with or without paclitaxel (160 mg/m2). The accrual of stage IV patients was completed in June, 2003. Approximately 80% of the subjects completed six cycles of chemotherapy. Three deaths resulted from bowel complications, and one death was caused by renal failure. Hematologic adverse events, sensory neuropathy, and myalgia, were more frequent and severe in the paclitaxel arm (*P* < 0.01). The percentage of patients alive and recurrence-free at 36 months was 62% for RT + AP vs. 64% for RT + TAP. The hazard of recurrence or death relative to the RT + AP arm and stratified according to stage was 0.90 (95% CI, 0.69 to 1.17; *P* = 0.21). However, in a subgroup analysis, RT + TAP was associated with a 50% reduction in the risk of recurrence or death among patients with gross residual disease (95% CI, 0.26 to 0.92). This study showed that the addition of paclitaxel to cisplatin and doxorubicin following surgery and radiation was not associated with a significant improvement in RFS but was associated with increased toxicity.

#### **5.4 NSGO 9501/ EORTC 55991 study and MaNGO ILIADE III study**

Hogberg et al. reported a paper32), presenting two randomized clinical trials (NSGO EC9501 /EORTC55991 and MaNGO ILIADEIII). The former study was reported at the ASCO 2007 meeting33). These two studies were undertaken to clarify whether the sequential combination of chemotherapy and radiotherapy improves the PFS in high-risk subjects with endometrial cancer. These studies had similar designs; however, some differences existed regarding the distribution of stages and the rates of pelvic or paraaortic lymphadenectomy. Most of the enrolled cases were stage I in the former study, while all the cases were stage II or III in the latter study; in addition, the rate of pelvic or paraaortic lymphadenectomy was higher in the ILIADEIII study. In total, patients (n = 540) with surgically resected endometrial cancer stage I – III and with no residual tumor or prognostic factors implying a high -risk were randomly allocated to an adjuvant radiotherapy group with or without sequential chemotherapy.

In the NSGO/EORTC study, patients with stage I, II, IIIA (positive peritoneal fluid cytology only), or IIIC (positive pelvic lymph nodes only) diseases were enrolled. The chemotherapy modalities included AP (doxorubicin, 50 mg/m2 + cisplatin, 50 mg/m2; 83%), EP (epirubicin, 75 mg/m2; 4%), TEC (paclitaxel, 175 mg/m2 + epirubicin, 60 mg/m2 + carboplatin, AUC 5; 3%), and TC (paclitaxel, 175 mg/m2, carboplatin, AUC 5 – 6; 10%). The radiation arm consisted of pelvic EBRT (44 Gy) with or without brachytherapy. The combined modality treatment was associated with a 36% reduction in the risk of relapse or death (HR, 0.64; 95% CI, 0.41 – 0.99; *P* = 0.04); two-sided tests were used. In the MaNGO ILIADEIII study, only the AP therapy was used as a chemotherapy regimen. The results from the MaNGO ILIADEIII study pointed in the same direction (HR, 0.61) as those of the NSGO/EORTC study, but were not significant. In both studies, adverse effects were more severe in the combined modality group.

In the combined analysis, the estimate of the risk for relapse or death was similar but with narrower confidence limits (HR, 0.63; 95% CI, 0.44 – 0.89; *P* = 0.009). Neither study showed significant differences in the OS. In the combined analysis, the OS approached statistical significance (HR, 0.69; 95% CI, 0.46 – 1.03; *P* = 0.07) and cancer-specific survival (CSS) was significant (HR, 0.55; 95% CI, 0.35 – 0.88; *P* = 0.01). Thus, the addition of adjuvant chemotherapy to radiation improved the PFS and CSS in surgically treated endometrial cancer patients with no residual tumor and a high-risk profile. Regarding the pathological subtypes, combined therapy offered a superior benefit to patients with endometrioid type and grade 1 or 2 diseases, but not to patients with serous or clear cell types and grade 3 diseases. Several remaining questions need to be further investigated in future trials.

#### **6. Ongoing trials comparing radiation therapy alone and radiation therapy plus chemotherapy**

At present, there are several ongoing studies comparing radiation therapy alone and radiation plus chemotherapy (Table 3). The RTOG-GOG9905 study finished accrual in 2004; however, its results have not yet been presented. Accrual for the PORTECIII and GOG249 trials is ongoing. These three trials are phase III randomized trials comparing a radiation alone group and a combined radiation and chemotherapy group. Two of them are examining concurrent chemoradiotherapy followed by four cycles of TC, and the third trial is examining brachytherapy followed by three cycles of TC.
