| Literature DB >> 28265583 |
Jiang Chen1, Guo Xiao-Zhong1, Xing-Shun Qi1.
Abstract
Specific immunotherapies, including vaccines with autologous tumor cells and tumor antigen-specific monoclonal antibodies, are important treatments for PC patients. To evaluate the clinical outcomes of PC-specific immunotherapy, we performed a systematic review and meta-analysis of the relevant published clinical trials. The effects of specific immunotherapy were compared with those of nonspecific immunotherapy and the meta-analysis was executed with results regarding the overall survival (OS), immune responses data, and serum cancer markers data. The pooled analysis was performed by using the random-effects model. We found that significantly improved OS was noted for PC patients utilizing specific immunotherapy and an improved immune response was also observed. In conclusion, specific immunotherapy was superior in prolonging the survival time and enhancing immunological responses in PC patients.Entities:
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Year: 2017 PMID: 28265583 PMCID: PMC5318641 DOI: 10.1155/2017/8282391
Source DB: PubMed Journal: J Immunol Res ISSN: 2314-7156 Impact factor: 4.818
Figure 1Flowchart of inclusion.
Clinical information from eligible trials used in the meta-analysis.
| Author, journal (year) [Ref] | Country | Age | Sex (M/F) | Number of pts. (case/control) | Study design | Enrollment period | Tumor stage | Specific immunotherapy arm | Control arm | Specific immunotherapy course | Length of follow-up |
|---|---|---|---|---|---|---|---|---|---|---|---|
| Asahara et al., J Transl Med (2013) [ | Japan | Median (range) 61.3 (33–80) years | 66/46 | 112 (31/81) | Retrospective case-control study | 2009.3–2010.2 | Unknown | KIF20A-66 HLA-A24-restricted peptide + chemotherapy | Chemotherapy | 1.0 or 3.0 mg/body peptide × 8 in a 56 days cycle + 1.0 or 3.0 mg/m2 gemcitabine per 2 weeks | Unknown |
| Bernhardt et al., Br J Cancer (2006) [ | Norway | Range: 40–72 years | 26/22 | 48 (26/22) | Phase I/II case-control study | 2000.9–2003.3 | Unknown | Telomerase peptide vaccine | Negative peptide | 3 injections in week 1 and 1 weekly injection in weeks 2, 3, 4, 6, and 10 | 10–575 days (survival days from start of treatment) |
| Brett et al., J Clin Oncol (2002) [ | UK | Median (range) 62.95 (44–79) years | 24/6 | 30 | Phase II self-control study | Unknown | II, III, IV | Anti-gastrin-17 antibody | Unknown | 3 doses of 100 | 16 weeks |
| Cai et al., Chinese Journal of Cancer Biotherapy (2013) [ | China | Median (range) 64 (30–75) years | 13/11 | 24 | Self-control study | 2011.7–2012.5 | III, IV | DC pulsed with antigens of PANC-1 cells + CIK | Unknown | 1 × 106 DC × 4 + 1 × 106 CIK × 3 | 4 weeks after first treatment to 16.7 months |
| Chawla et al., Mol Ther (2010) [ | USA | Median (range) 64 (50–83) years | 7/6 | 13 (7/6) | Phase I/II case-control study | 2007.10–2009.1 | Unknown | Positive Rexin-G vaccine | Negative vaccine | 1-2 × 1011 cfu Rexin-G × 12 | 0–12 months |
| Endo et al., J Hepatobiliary Pancreat Sci (2012) [ | Japan | Mean age 62 ± 8.1 years | 13/11 | 24 (9/15) | Phase I case-control study | 2003.11–2007.7 | IA, IIA, IIB, IV | DC + OK432 | OK432 | 1.0 × 108 DC + 0.1 mL OK432 | 0.7–6.1 years |
| Gjertsen et al., Int J Cancer (2001) [ | Norway | Range: 35–77 years | 19/18 | 37 (17/20) | Phase I/II case-control study | 1996.11–1998.11 | Unknown | K-ras peptide vaccination + GM-CSF | Negative peptide | 100 | 3–6 months after first injection to 2 years |
| Kameshima et al., Cancer Sci (2013) [ | Japan | Range 50–80 years | 3/3 | 6 | Self-control study | 2005.12–2010.11 | Unknown | Survivin-2B80-88 peptide + IFA + | Unknown | (1 mg/1 mL peptide + 1 mL IFA) × 4 + 3,000 IU | Unknown |
| Koido et al., Clin Cancer Res (2014) [ | Japan | Range 39–73 years | 7/4 | 11 | Phase I self-control study | 2011.8–2013.1 | IV | DC pulsed with multiple WT-1 peptides + chemotherapy | Unknown | 1 × 107 DC/WT-1 cells/dose × 5 + 1000 mg/m2 gemcitabine × 5 | 800 days after first injection |
| Kondo et al., Anticancer Res (2008) [ | Japan | Range 51–84 years | 14/6 | 20 | Self-control study | 2001–2006 | III, IV | DCs pulsed with MUC1 peptide + CTLs stimulated by MUC1-expressing cells | Unknown | (1.1 × 107 to 3.1 × 108 MUC1-DCs + 5.0 × 108 to 6.8 × 109) × 2 to 15 times | Unknown |
| Kubuschok et al., Hum Gene Ther (2012) [ | Germany | Range 48–66 years | 4/3 | 7 | Self-control study | 1997–2000 | II, III | muRas-LCL | Unknown | 5 × 106 muRas-LCL × 8 | 7–52 weeks |
| Le et al., J Immunother (2013) [ | USA | Median (range) 62 (44–77) years | 21/9 | 30 (15/15) | Phase Ib, randomized study | 2009.3–2010.12 | II, III, IV | Ipilimumab + GVAX | Ipilimumab | 10 mg/kg ipilimumab + 2.5 × 108 cells of GVAX | 0–30 months |
| Le et al., J Clin Oncol (2015) [ | USA | Median (range) 63 (45–87) years | 53/37 | 90 (61/29) | Multicenter, randomized, case-control phase II trial | 2011.9–2012-11 | Unknown | Cy/GVAX plus CRS-207 | Cy/GVAX | (200 mg/m2 cy + 2.5 × 108 cells GVAX) × 6 + 1 × 109 colony-forming units CRS-207 × 6 | 600 days after first treatment |
| Liu, Chin J Clinicians (2012) [ | China | Median (range) 61 (42–76) years | 27/23 | 50 (25/25) | Randomized, case-control study | 2010.6–2011.12 | I, II, III, IV | DC pulsed with tumor cells lysates + CIK + chemotherapy | Chemotherapy | 2 × 109 DC-CIK cells × 6 + 600 mg/m2 5-FU | Unknown |
| Liu et al., Nanjing yi ke da xue xue bao (2010) [ | China | Range 48–79 years | 17/13 | 30 (15/15) | Randomized, case-control study | Unknown | III, IV | DC pulsed with tumor cells lysates + CIK + chemotherapy | Chemotherapy | DC × 4 + 1 g/m2 chemotherapy × 18 | 7 days after therapy |
| Middleton et al., Lancet Oncol (2014) [ | UK | Range 55–69 years | 608/454 | 1062 (704/358) | Multicenter, open-label, phase III randomized control trial | 2007.3–2011.3 | Unknown | Telomerase peptide vaccine GV1001 + gemcitabine and capecitabine | Gemcitabine, capecitabine | 1000 mg/m2 gemcitabine × 6 + 830 mg/m2 capecitabine × 2 + GV1001 | Followed up for a median of 6.0 months |
| Nishida et al., J Immunother (2014) [ | Japan | Median (range) 60 (41–75) years | 17/15 | 32 | Phase I self-control study | 2008–2010 | Unknown | WT-1 peptides vaccine + gemcitabine | Unknown | 1000 mg/m2 gemcitabine × 6 + 0.3 to 3.0 mg WT-1 vaccine × 4 | 30 months |
| Picozzi et al., Eur J Cancer (2015) [ | USA | Range 39–80 years | 33/25 | 58 (29/29) | Phase Ib case-control study | 2102.6–2013.2 | Unknown | 90Y-clivatuzumab tetraxetan (anti-MUC5ac monoclonal antibody) + gemcitabine | 90Y-clivatuzumab tetraxetan | 6.5 mCi/m2 Y-clivatuzumab tetraxetan × 3 ± 200 mg/m2 gemcitabine × 4 | 12 months after first injection |
| Qiu et al., Int J Clin Oncol (2013) [ | China | Mean (range) age 60.1 ± 8.4 (44–90) years | 12/2 | 14 | Phase I self-control study | 2004.3–2009.2 | III, IV | DC pulsed with | Unknown | (2 × 109cells–10 × 109cells) (DCs + CIKs)/injection × 1–5 times | 24 months after first injection |
| Sultana et al., BMC Cancer (2009) [ | UK | Median (range) 60 (47–67) years | Unknown | 19 | Randomized phase II self-control trial | 2003.2–2005.7 | IVa, IVb | Anti-carcinoembryonic antigen I131KAb201 antibodies | Unknown | 50 mCi–75 mCi KAb 201 via either the intra-arterial or intravenous delivery route | 90 days posttreatment |
| Suzuki et al., J Immunother (2014) [ | Japan | Median (range) 62 (48–74) years | 4/5 | 9 | Nonrandomized, open-label, phase I self-control study | Unknown | III, IV | KIF20A-10-66 peptide + gemcitabine | Unknown | 0.5–3 mg/body KIF20A-10-66 peptide × 4 + 1000 mg/m2 gemcitabine × 3 | 94–366 days |
| Wen et al., Xiandai zhongxiyi jiehe zazhi (2013) [ | China | Range 49–78 years | 33/27 | 60 (30/30) | Randomized, case-control study | 2008.3–2011.3 | Unknown | DC pulsed with tumor cells lysates + CIK + chemotherapy | Chemotherapy | 2 × 109 DC-CIK cells × 6 + 600 mg/m2 5-FU | 2–26 months |
| Yanagimoto et al., Oncol Rep (2010) [ | Japan | Median (range) 64 (48–80) years | 13/8 | 21 | Nonrandomized, open-label, phase II self-control study | 2006.9–2008.3 | IVa, IVb | PPV + gemcitabine | Unknown | 3 mg/peptide were administered weekly + 1000 mg/m2 gemcitabine per week for 3 weeks | 3–24 months |
| Yutani et al., Oncol Rep (2013) [ | Japan | Median (range) 61 (44–78) years | 27/14 | 41 | Open-label phase II self-control study | 2008.11–2011.3 | IVa, IVb | PPV | Unknown | 4 peptides (3 mg/each peptide) administered once a week for 6 consecutive weeks | Over 800 days |
| Zhang, Zhongguo xian dai yi xue za zhi (2014) [ | China | Mean range 58.2 ± 5.2 (48–78) years | 33/27 | 60 (30/30) | Randomized, case-control study | 2010.1–2012.6 | I, II, III, IV | DC pulsed with tumor cells lysates + CIK + chemotherapy | Chemotherapy | 2 × 109 DC-CIK cells × 4 + 15 mg/kg 5-FU × 4 | Over 3 years |
DC, dendritic cell; CIK, cytokine-induced killer cell; GM-CSF, granulocyte-macrophage colony-stimulating factor; IFA, incomplete Freund's adjuvant; WT-1, Wilms' tumor-1; MUC1, Mucin 1; LCL; lymphoblastoid cell lines; GVAX, GM-CSF cell-based vaccines; α-Gal, alpha-galactosyl; PPV, personalized peptide vaccination; CRS-207, human mesothelin; ipilimumab, anti-CTLA-4 antibody.
Figure 2Forest plot of comparison: 3-month overall survival of 7 included studies.
Figure 3Forest plot of comparison: 6-month overall survival (12 studies).
Figure 4Forest plot of comparison: 1-year overall survival of 14 included studies.
Figure 5Forest plot of comparison: 1.5-year overall survival of 9 included studies.
Figure 6Forest plot of comparison: 2-year overall survival (6 studies).
Figure 7Forest plot of comparison: 3-year overall survival of 4 included studies.
Figure 8Forest plot of comparison: CTL-responses between before and after specific immunotherapy treatment groups (3 studies).
Figure 9Forest plot of comparison: antibody-responses between before and after specific immunotherapy treatment groups (3 studies).
Figure 10Forest plot of comparison: CD4+ lymphocyte subset percentages between specific immunotherapy group and the baseline observed before treatment group in 4 included studies.
Figure 11Forest plot of comparison: portion of CD4+/CD8+ between specific immunotherapy group and the baseline observed before treatment group (4 studies).
Figure 12Forest plot of comparison: CD4+CD25+ lymphocyte subset percentages between specific immunotherapy group and the baseline observed before treatment group (3 studies).
Figure 13Forest plot of comparison: CD8+ lymphocyte subset percentages between specific immunotherapy group and the baseline observed before treatment group in 4 included studies.
Figure 14Forest plot of comparison: CD56+ lymphocyte subset percentages between specific immunotherapy group and the baseline observed before treatment group in 6 included studies.
Figure 15Forest plot of comparison: IFN-γ levels between specific immunotherapy group and the baseline observed before treatment group (4 trials).
Figure 16Forest plot of comparison: IL4 levels between specific immunotherapy group and the baseline observed before treatment group (2 trials).
Figure 17Forest plot of comparison: CA19-9 levels between specific immunotherapy group and the baseline observed before treatment group (4 trials).
Figure 18Forest plot of comparison: CEA levels between specific immunotherapy group and the baseline observed before treatment group (2 trials).