The hybrid oncolytic peptide NTP-385 potently inhibits adherent cancer cells by targeting the nucleus

Hao Yin; Xi-Tong Chen; Qiao-Na Chi; Yan-Nan Ma; Xing-Yan Fu; Shan-Shan Du; Yun-Kun Qi; Ke-Wei Wang

doi:10.1038/s41401-022-00939-x

The hybrid oncolytic peptide NTP-385 potently inhibits adherent cancer cells by targeting the nucleus

Acta Pharmacol Sin. 2023 Jan;44(1):201-210. doi: 10.1038/s41401-022-00939-x. Epub 2022 Jul 6.

Authors

Hao Yin^{1

2}, Xi-Tong Chen³, Qiao-Na Chi⁴, Yan-Nan Ma³, Xing-Yan Fu³, Shan-Shan Du⁵, Yun-Kun Qi^{6

7}, Ke-Wei Wang^{8

9}

Affiliations

¹ Department of Pharmacology, School of Pharmacy, Qingdao University Medical College, Qingdao University, #1 Ningde Road, Qingdao, 266073, China.
² Institute of Innovative Drugs, Qingdao University, 38 Dengzhou Road, Qingdao, 266021, China.
³ Department of Medicinal Chemistry, School of Pharmacy, Qingdao University Medical College, Qingdao University, #1 Ningde Road, Qingdao, 266073, China.
⁴ College of Chemical Engineering, Qingdao University of Science and Technology, Qingdao, 266042, China.
⁵ College of Chemical Engineering, Qingdao University of Science and Technology, Qingdao, 266042, China. shanshandu@qust.edu.cn.
⁶ Institute of Innovative Drugs, Qingdao University, 38 Dengzhou Road, Qingdao, 266021, China. qiyunkun@qdu.edu.cn.
⁷ Department of Medicinal Chemistry, School of Pharmacy, Qingdao University Medical College, Qingdao University, #1 Ningde Road, Qingdao, 266073, China. qiyunkun@qdu.edu.cn.
⁸ Department of Pharmacology, School of Pharmacy, Qingdao University Medical College, Qingdao University, #1 Ningde Road, Qingdao, 266073, China. wangkw@qdu.edu.cn.
⁹ Institute of Innovative Drugs, Qingdao University, 38 Dengzhou Road, Qingdao, 266021, China. wangkw@qdu.edu.cn.

Abstract

The use of oncolytic peptides with activity against a wide range of cancer entities as a new and promising cancer therapeutic strategy has drawn increasing attention. The oncolytic peptide LTX-315 derived from bovine lactoferricin (LfcinB) was found to be highly effective against suspension cancer cells, but not adherent cancer cells. In this study, we tactically fused LTX-315 with rhodamine B through a hybridization strategy to design and synthesize a series of nucleus-targeting hybrid peptides and evaluated their activity against adherent cancer cells. Thus, four hybrid peptides, NTP-212, NTP-217, NTP-223 and NTP-385, were synthesized. These hybrid peptides enhanced the anticancer activity of LTX-315 in a panel of adherent cancer cell lines by 2.4- to 37.5-fold. In model mice bearing B16-F10 melanoma xenografts, injection of NTP-385 (0.5 mg per mouse for 3 consecutive days) induced almost complete regression of melanoma, prolonged the median survival time and increased the overall survival. Notably, the administered dose of NTP-385 was only half the effective dose of LTX-315. We further revealed that unlike LTX-315, which targets the mitochondria, NTP-385 disrupted the nuclear membrane and accumulated in the nucleus, resulting in the transfer of a substantial amount of reactive oxygen species (ROS) from the cytoplasm to the nucleus through the fragmented nuclear membrane. This ultimately led to DNA double-strand break (DSB)-mediated intrinsic apoptosis. In conclusion, this study demonstrates that hybrid peptides obtained from the fusion of LTX-315 and rhodamine B enhance anti-adherent cancer cell activity by targeting the nucleus and triggering DNA DSB-mediated intrinsic apoptosis. This study also provides an advantageous reference for nucleus-targeting peptide modification.

Keywords: DNA double-strand break; LTX-315; ROS; hybridization strategy; intrinsic apoptosis; melanoma; nucleus-targeting peptides; oncolytic peptides; rhodamine B.

MeSH terms

Animals
Apoptosis
Cell Line, Tumor
DNA
Humans
Melanoma*
Mice
Peptides* / pharmacology
Peptides* / therapeutic use

Substances

Peptides
DNA