Near-infrared-traceable DNA nano-hydrolase: specific eradication of telomeric G-overhang in vivo

Author:

Sun Yuhuan12,Zhao Chuanqi1,Cui Tingting12,Qin Hongshuang1,Niu Jingsheng12,Ren Jinsong12,Qu Xiaogang12ORCID

Affiliation:

1. Laboratory of Chemical Biology and State Key Laboratory of Rare Earth Resource Utilization, Changchun Institute of Applied Chemistry, Chinese Academy of Sciences, Changchun, Jilin 130022, China

2. School of Applied Chemistry and Engineering, University of Science and Technology of China, Hefei, Anhui 230026, China

Abstract

Abstract Telomeric DNA, whose length homeostasis is closely correlated with immortality of cancer cells, is regarded as a molecular clock for cellular lifespan. Regarding the capacity in forming G-quadruplex, G-rich 3′-overhang (G-overhang) has been considered as an attractive anticancer target. However, it is still challenging to precisely target telomeric G-overhang with current ligands because of the polymorphism of G-quadruplexes in cells. Herein, we construct a telomeric G-overhang-specific near-infrared-traceable DNA nano-hydrolase, which is composed of four parts: (i) dexamethasone for targeting cell nuclei; (ii) complementary DNA for hybridizing with G-overhang; (iii) multinuclear Ce(IV) complexes for hydrolyzing G-overhang; and (iv) upconversion nanoparticles for real-time tracking. The multivalent targeted DNA nano-hydrolase can be traced to precisely digest telomeric G-overhang, which contributes to telomeric DNA shortening and thereby causes cell aging and apoptosis. The anticancer treatment is further proved by in vivo studies. In this way, this design provides a telomeric G-overhang-specific eradication strategy based on a non-G-quadruplex targeting manner.

Funder

National Natural Science Foundation of China

Chinese Academy of Sciences

Publisher

Oxford University Press (OUP)

Subject

Genetics

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