Genetically Modified DR5-Specific TRAIL Variant DR5-B Revealed Dual Antitumor and Protumoral Effect in Colon Cancer Xenografts and an Improved Pharmacokinetic Profile

Anne V Yagolovich; Artem A Artykov; Tatiana A Karmakova; Maria S Vorontsova; Andrey A Pankratov; Alexander A Andreev-Andrievsky; Dmitry A Dolgikh; Mikhail P Kirpichnikov; Marine E Gasparian

doi:10.1016/j.tranon.2020.100762

Genetically Modified DR5-Specific TRAIL Variant DR5-B Revealed Dual Antitumor and Protumoral Effect in Colon Cancer Xenografts and an Improved Pharmacokinetic Profile

Transl Oncol. 2020 Apr;13(4):100762. doi: 10.1016/j.tranon.2020.100762. Epub 2020 Mar 27.

Authors

Anne V Yagolovich¹, Artem A Artykov¹, Tatiana A Karmakova², Maria S Vorontsova², Andrey A Pankratov², Alexander A Andreev-Andrievsky³, Dmitry A Dolgikh¹, Mikhail P Kirpichnikov¹, Marine E Gasparian⁴

Affiliations

¹ Department of Bioengineering, Shemyakin-Ovchinnikov Institute of Bioorganic Chemistry of the Russian Academy of Sciences, Moscow, Russia; Faculty of Biology, Lomonosov Moscow State University, Moscow, Russia.
² Department of modifiers and protectors of antitumor therapy, National Medical Research Radiological Center of the Ministry of Health of the Russian Federation, Moscow, Russia.
³ Faculty of Biology, Lomonosov Moscow State University, Moscow, Russia.
⁴ Department of Bioengineering, Shemyakin-Ovchinnikov Institute of Bioorganic Chemistry of the Russian Academy of Sciences, Moscow, Russia. Electronic address: marine_gasparian@yahoo.com.

Abstract

Despite the weak clinical efficacy of TRAIL death receptor agonists, a search is under way for new agents that more efficiently activate apoptotic signaling. We previously created a TRAIL DR5-selective variant DR5-B without affinity for the DR4, DcR1, DcR2, and OPG receptors and increased proapoptotic activity in tumor cells. Here we showed that DR5-B significantly inhibited tumor growth in HCT116 and Caco-2 but not in HT-29 xenografts. The antitumor activity of DR5-B was 2.5 times higher in HCT116 xenografts compared to TRAIL. DR5-B at a dose of 2 or 10 mg/kg/d for 10 days inhibited tumor growth in HCT116 xenografts by 26% or 50% respectively, and increased animal survival. Unexpectedly, DR5-B at a higher dose (25 mg/kg/d) inhibited tumor growth only during the first 8 days of drug exposure, while at the end of the monitoring, no effect or even slight stimulation of tumor growth was observed. The pharmacokinetic parameters of DR5-B were comparable to those of TRAIL, except that the half-life was 3.5 times higher. Thus, enhancing TRAIL selectivity to DR5 may increase both antitumor and proliferative activities depending on the concentration and administration regimens.