Review
Copyright ©The Author(s) 2015.
World J Gastroenterol. Feb 28, 2015; 21(8): 2294-2302
Published online Feb 28, 2015. doi: 10.3748/wjg.v21.i8.2294
Table 1 Results of different treatment modalities in localized squamous cell anal cancer
ProtocolCRCFSOSDFS
ART54%[29]32% lower colostomy-free rate than C[28]14% higher death rate than C[27]12.9% higher death and relapse rates at 5 yr than C[27]
BRT + 5-FUNA71%[29]No significant difference from C51%[29]
CRT + 5-FU + Mitomycin80%[29]89.6% at 26 wk[34]59%[28]78.3% at 5 yr[32,33]67.8%[29,30]to 73%[29]
DRT + 5-FU + Cisplatin90.5% at 26 wk[34]NA70.7% at 5 yr[31,32]57.8%[31,32]
NA: Not availiable; RT: Radiation therapy; 5-FU: 5-Fluorouracil; CR: Complete response; CFS: Colostomy-free survival; OS: Overall survival; DFS: Disease free survival.
Table 2 Studies evaluating recent treatment options in locally advanced anal cancer
StudyPatients, nProtocolRROSDFSCFS
Induction chemotherapy in LAACNilsson et al[36], 2005Population-based series308 invasive SCAC- Arm A: Neoadjuvant platinum CT followed by RT aloneCR: 92%63%NANA
142 locally advanced-Arm B: RT with or without BleomycinCR: 76% P < 0.0144% P < 0.05
Meropol et al[37], 20081 Phase II45Induction: 2 28-d cycles (FU + cisplatin) followed by 2 28-d cycles (FU + mitomycin) with concurrent split-course radiationCR: 82%68% at 4 yr61% at 4 yr50%
Peiffert et al[38], 20122 Phase III RCT283-Arm A: 2 ICT cycles (5-FU + cisplatin) then RCT and standard dose boost (SD: 15 Gy)NANANA69.6%
-Arm B: 2 ICT, RCT and high dose boost (HD: 20-25 Gy)82.4%
-Arm C: RCT and SD boost77.1%
-Arm D: RCT and HD boost72.7%
Combination of MMC and cisplatin in LAACCrehange et al[39], 2007 Phase II211st sequence:RT 36 Gy over 4 wkCR: 90.5%NANANA
2nd sequence: 23.4 Gy over 2.5 wk, gap 16 d
MMC and CDDP
Matzinger et al[40], 20093 Phase II80RT: 36Gy + 2 wk gap + 23.4 Gy
-Arm A: MMC + Cisplatin + RTRR: 91.9%NANANA
-Arm B: MMC + 5-FU + RTRR: 79.5%
Targeted therapy in LAACOlivatto et al[48], 2013 Phase I21Cetuximab + RT + 5-FU + cisplatinpCR: 95%NANANA
Deutsch et al[49], 2013 Phase II16Cetuximab + RT + 5-FU + cisplatinCR: 55%PR: 45%92% at 1 yrNA67% at 1 yr
Cisplatin in LAACEng et al[50], 20134 Retrospective single institution analysis197 (41% stage II, 46% stage III, 24% N2-N3)Weekly (20 mg/m2) or daily (4 mg/m2) cisplatin with 5-FU and RTCR: 94%86% at 5 yr81% at 5 yr88% at 5 yr
1After induction, 8 CR and 21 PR. A third cycle of FU and cisplatin with radiation boost was given to patients with persistent primary site disease or bulky N2 or N3 disease at presentation;
2Considering the 2 × 2 factorial analysis, the 5-year CFS was 76.5% vs 75% in groups A and B vs C and D, respectively (ICT effect; P = 0.37), and 73.7% vs 77.8% in groups A and C vs B and D, respectively (RT-dose effect; P = 0.067);
3In the first arm, 9 patients discontinued treatment, with 9 grade 3 hematologic effects. In the second arm, 2 discontinued treatment, and no grade 3 hematologic effects were reported;
4The local recurrence rate was 11% after the median follow-up of 8.6 yr, and 8% of the patients developed distal metastases. LAAC: Locally advanced anal cancer; MMC: Mitomycin C; RR: Response rate; NA: Not availiable; RT: Radiation therapy; 5-FU: 5-Fluorouracil; CR: Complete response; CFS: Colostomy-free survival; OS: Overall survival; DFS: Disease free survival; RT: Radiation therapy.
Table 3 Recent case reports and case series evaluating treatment in metastatic anal cancer
StudynCharacteristics of patientsRegimenResponseSurvival
Jhawer et al[71], 200620Phase IIMMC, adriamycin, cisplatin followed by bleomycin-CCNU upon progression of disease60% PR0% CR15 mo
Golub et al[67], 20113P1P2P3Previously treated with 5-FU and cisplatinPaclitaxel 175 mg/m2 on D1Ifosfamide 1 g/m2 D1 to D4Cisplatin 75 mg/m2 on D1Every 3 wkCR in 3 patientsResponse duration6 mo2.5 yr4 moSurvival since recurrence14 mo30 mo17 mo (patient still alive)
Abbas et al[69], 20117Prior progression on cisplatin and 5-FUWeekly paclitaxel1 CR, 3PR,1 SD12-14 mo1
Kim et al[70], 20138Advanced recurrentDocetaxel 75 mg/m2 day 1, CDDP 75 mg/m2 day 1 and 5-FU at 750 mg/m(2)/day for 5 d every 3 wkCR: 50%OS 62.5% at 12 mo
Khawandanah et al[68], 20141Skin and perianal metastasis(1) Paclitaxel, ifosfamide, cisplatin (4 cycles) followed by(2) Mitomycin, cetuximab (2 cycles)(1) Minimal residual disease(2) Mixed response(1) Progression 5 mo after the end of therapy(2) OS 24 mo; 16 mo after paclitaxel was started
Barmettler et al[45], 20121Liver metastasis, KRAS wild type and EGFR 2 +FOLFIRI + cetuximabPartial response after 6 cycles21 mo
Bamba et al[46], 20121Lung metastasis3 FOLFOX→3 courses of FOLFOX + panitumumab→5 courses of FOLFIRI + panitumumabMarked reduction of primary tumor, disappearance of lung metastasis.The patient underwent low anterior resection.No recurrence after 5 mo
Lukan et al[47], 2009Case report7First or subsequent treatment lineCetuximab alone or with irinotecan first or subsequent line. KRAS mutated in 2/7PR 3MR 1PD 2 (Mutated kras)SD 1NA
Nitori et al[72], 2011158-yr-old femaleOral S-1 (120 mg/body; day 1-21) + low dose cisplatin (10 mg/body; day 1-5, 8-12) + RT for 2 cycles then rest for 4 wkCR of the primary lesion and PR for the metastatic lesions16 mo
1Duration of clinical benefit in SD and PR after the initiation of Paclitaxel: 4-6 mo. PD: Progressive disease; PR: Partial response; MR: Minor response; SD: Stable disease; NA: Not availiable.