Table 1.
Anti-CAIX monoclonal antibodies-based preclinical studies reporting antitumor responses.
| Author | Antibody Type | Tumor Type | Dosage | Response |
|---|---|---|---|---|
| Surfus et al. (1996) [17] | cG250 | RCC and breast carcinoma cell lines | cG250: 0.5 µg/mL, IL2: 100 U/mL |
ADCC with PBMCs (effector to target rate 100:1) after 4 h RCC—SK-RC-13: cG250 48%; cG250 + IL2 50%; SK-RC-30: cG250 25%; cG250 + IL2 65%; Breast cancer—BT-20: cG250 38%; cG250 + IL2 28% |
| Liu et al. (2002) [18] | cG250 | RCC and chronic myelogenous leukemia | cG250: 1 µg/mL, IL2 10 IU/mL; IFNγ, IFN-2a, IFN-2b 1000 IU/mL |
ADCC with PBMC (effector to target rate 25:1) after 2 days RCC—SK-RC-52: cG250 + IL2 42%; cG250 + IFN-𝛾 33%; cG250 + IFN-𝛼-2a or cG250 + IFN-α-2b 25%; SK-RC-09: cG250 + IL2 28%; cG250 + IFN-𝛾; cG250 + IFN-𝛼-2a, and cG250 + IFN-α-2b < 10%; Leukemia—K562: cG250 + IL2 60%; cG250 + IFN-𝛾 30%; cG250 + IFN-𝛼-2a or cG250 + INF-α-2b 43% |
| Brouwers et al. (2004) [19] | 131I-cG250, 90Y-SCN-Bz- DTPA-cG250, 177Lu-SCN-Bz-DTPA-cG250, or 186Re-MAG3 cG250 | RCC | 30 µg 131I-cG250, 30 µg 90Y-SCN-Bz-DTPA-cG250, 60 µg 177Lu-SCN-Bz-DTPA-cG250, or 35 µg 186Re-MAG3-cG250; Variable doses of radioisotopes |
Best median survival (SK-RC-52 cells) 177Lu-SCN-Bz-DTPA cG250: 294 days; 90Y-SCN-Bz-DTPA cG250: 241 days; 186Re-MAG3-cG250: 211 days; 131I-cG250: 164 days; Control groups < 150 days |
| Bauer et al. (2009) [20] | cG250-TNF and cG250 | RCC | 100 µg of cG250 or cG250-TNF 300 ng every 3 days |
In vivo tumor size after 78 days (SK-RC-52 cells) cG250-TNF + IFNγ: 60% decrease; cG250-TNF: 50% decrease; cG250 + IFNγ: no difference in tumor size compared to negative control |
| Zatovicova et al. (2010) [21] | VII/20 | Colorectal carcinoma | 100 μg twice a week | In vivo tumor weight/volume reduction (HT-29 cells) 60%/73% treatment initiated after 10 days of tumor implantation; 88%/93% treatment initiated in the same day of tumor implantation |
| Oosterwijk-Wakka et al. (2011) [22] | 125I-cG250 + sorafenib, sunitinib, or vandetanib | RCC |
125I-cG250 185 kBq/5 μg 35 mg/kg of sunitinib, 50 mg/kg of sorafenib, 50 mg/kg of vandetanib |
In vivo tumor volume (NU-12 cells) decrease for continuous treatment (14 days) Vandetanib: 57%, sunitinib: 49%, and sorafenib: 37%, all compared to 125I-cG250 alone |
| Petrul et al. (2012) [23] | BAY 79-4620 | Colorectal cancer, gastric carcinoma, and NSCLC-PDX | Variable | In vivo tumor regression (3 doses of every 4 days) Colorectal cancer (dose 10 mg/kg): HT-29: 100%, Colo205: 85%; Gastric carcinoma (dose 60 mg/kg): NCI-N87: 87%, MKN-45: 90%, SNU-16: 75%; NSCLC-PDX: complete regression in 2/5, partial regression in 3/5 |
| Muselaers et al. (2014) [15] | 111In-DOTA-mG250 and 177Lu-DOTA-mG250 | RCC | 13 MBq 177Lu-DOTA-mG250, 13 MBq nonspecific 177Lu-DOTA-MOPC21, 20 MBq 111In-DOTA-mG250 |
Median survival (SK-RC-52 cells) 177Lu-DOTA-mG250: 139 days; 177Lu-DOTA-MOPC21: 49 days; 111In-DOTA-mG250: 53 days; Control: 49–53 days |
| Zatovicova et al. (2014) [16] | mG250 | Colorectal carcinoma | 100 µg/dose | In vivo tumor weight/volume reduction (HT-29 cells) Treatment initiated after 10 days of tumor implantation: 55%/73%; Treatment initiated at the same day of tumor implantation: 90%/93% |
| Chang et al. (2015) [24] | In vitro: G10, G36, G37, G39, and G119; In vivo: only G37 and G119 were tested |
RCC | ADCC in vitro: 5 µg/mL, In vivo: 10 mg/kg |
ADCC in SK-RC-09 cells: 25:1 effector to target cells: 25% for G36 and G119; 15–20% for G10, G37, and G39; 50:1 effector to target cells: 45% for G10, G36, G37, and G119; 30% for G39 In vivo tumor weight (Day 29)/volume (Day 28) reduction (SK-RC-59 CAIX+ cells): 85%/75% for G37, G119, mG37, and mG119 |
| Oosterwijk-Wakka et al. (2015) [25] | 111In-cG250 and Sunitinib | RCC | 0.4 MBq/5 µg 111In-cG250 three days after administration of 40–50 mg/kg of sunitinib for 13 days |
In vivo tumor growth reduction 20 days after the beginning of the treatment with sunitinib NU-12: 60%; SK-RC-52: not statistically significant compared to control |
| Yamaguchi et al. (2015) [26] | chKM4927 and chKM4927_N297D | RCC | 10 mg/kg i.p. twice a week for three weeks | In vivo tumor volume (VMRC-RCW cells) reduction after 32 days chKM4927 and chKM4927_N297D: 60% compared to negative control |
| Lin et al. (2017) [27] | Anti-CAIX functionalized liposomes with TPL | Lung cancer cells | 0.15 mg/kg once every 3–4 days for 8 times via pulmonary delivery |
Median survival time (A549 cells) CAIX-TPL-Lips: 90 days (statistically significant compared to saline control); Nontargeted TPL-lips: 71 days (not statistically significant compared to saline control); Control group: 45 days |
| De Luca et al. (2019) [28] | IL2-Anti-CAIX(XE114)-TNFmut and IL2-Anti-CAIX(F8)-TNFmut |
Colon Carcinoma | 30 µg i.v. four times every 24 h | Tumor volume reduction (CT26-CAIX cells) after 18 days IL2-F8-TNFmut: 58%; mIL2-F8-mTNFmut: 72%; IL2-XE114-TNFmut: 63%; mIL2-XE114-mTNFmut: 50% |
ADCC: antibody-dependent cell cytotoxicity, Bz: benzyl, DOTA: 1,4,7,10-tetraazacyclododecane-tetraacetic acid, DTPA: diethylenetriaminepentaacetic acid, I: iodine, IL2: interleukin-2, In: indium, IFN: interferon, Lu: lutetium, MAG3: mercaptoacetyltriglycine, MOPC21: unspecific control antibody, NSCLC-PDX: non-small cell lung cancer patient-derived xenograft, PBMCs: peripheral blood mononuclear cells, RCC: renal cell cancer, Re: rhenium, TNF: tumor necrosis factor, TNFmut: low potency mutated tumor necrosis factor, TPL: triptolide, Y: yttrium.