Noncovalent Stabilization of Vesicular Polyion Complexes with Chemically Modified/Single-Stranded Oligonucleotides and PEG-b-guanidinylated Polypeptides for Intracavity Encapsulation of Effector Enzymes Aimed at Cooperative Gene Knockdown

Beob Soo Kim; Mitsuru Naito; Hiroyuki Chaya; Mao Hori; Kotaro Hayashi; Hyun Su Min; Yu Yi; Hyun Jin Kim; Tetsuya Nagata; Yasutaka Anraku; Akihiro Kishimura; Kazunori Kataoka; Kanjiro Miyata

doi:10.1021/acs.biomac.0c01192

Noncovalent Stabilization of Vesicular Polyion Complexes with Chemically Modified/Single-Stranded Oligonucleotides and PEG-b-guanidinylated Polypeptides for Intracavity Encapsulation of Effector Enzymes Aimed at Cooperative Gene Knockdown

Beob Soo Kim, Mitsuru Naito, Hiroyuki Chaya, Mao Hori, Kotaro Hayashi, Hyun Su Min, Yu Yi, Hyun Jin Kim, Tetsuya Nagata, Yasutaka Anraku, Akihiro Kishimura, Kazunori Kataoka, Kanjiro Miyata

Applied Chemistry

Research output: Contribution to journal › Article › peer-review

15 Citations (Scopus)

Abstract

For the simultaneous delivery of antisense oligonucleotides and their effector enzymes into cells, nanosized vesicular polyion complexes (PICs) were fabricated from oppositely charged polyion pairs of oligonucleotides and poly(ethylene glycol) (PEG)-b-polypeptides. First, the polyion component structures were carefully designed to facilitate a multimolecular (or secondary) association of unit PICs for noncovalent (or chemical cross-linking-free) stabilization of vesicular PICs. Chemically modified, single-stranded oligonucleotides (SSOs) dramatically stabilized the multimolecular associates under physiological conditions, compared to control SSOs without chemical modifications and duplex oligonucleotides. In addition, a high degree of guanidino groups in the polypeptide segment was also crucial for the high stability of multimolecular associates. Dynamic light scattering and transmission electron microscopy revealed the stabilized multimolecular associates to have a 100 nm sized vesicular architecture with a narrow size distribution. The loading number of SSOs per nanovesicle was determined to be â2500 using fluorescence correlation spectroscopic analyses with fluorescently labeled SSOs. Furthermore, the nanovesicle stably encapsulated ribonuclease H (RNase H) as an effector enzyme at â10 per nanovesicle through simple vortex-mixing with preformed nanovesicles. Ultimately, the RNase H-encapsulated nanovesicle efficiently delivered SSOs with RNase H into cultured cancer cells, thereby eliciting the significantly higher gene knockdown compared with empty nanovesicles (without RNase H) or a mixture of nanovesicles with RNase H without encapsulation. These results demonstrate the great potential of noncovalently stabilized nanovesicles for the codelivery of two varying bio-macromolecule payloads for ensuring their cooperative biological activity.

Original language	English
Pages (from-to)	4365-4376
Number of pages	12
Journal	Biomacromolecules
Volume	21
Issue number	10
DOIs	https://doi.org/10.1021/acs.biomac.0c01192
Publication status	Published - Oct 12 2020

All Science Journal Classification (ASJC) codes

Bioengineering
Biomaterials
Polymers and Plastics
Materials Chemistry

UN SDGs

This output contributes to the following UN Sustainable Development Goals (SDGs)

Access to Document

10.1021/acs.biomac.0c01192

Fingerprint

Dive into the research topics of 'Noncovalent Stabilization of Vesicular Polyion Complexes with Chemically Modified/Single-Stranded Oligonucleotides and PEG-b-guanidinylated Polypeptides for Intracavity Encapsulation of Effector Enzymes Aimed at Cooperative Gene Knockdown'. Together they form a unique fingerprint.

Cite this

Kim, B. S., Naito, M., Chaya, H., Hori, M., Hayashi, K., Min, H. S., Yi, Y., Kim, H. J., Nagata, T., Anraku, Y., Kishimura, A., Kataoka, K., & Miyata, K. (2020). Noncovalent Stabilization of Vesicular Polyion Complexes with Chemically Modified/Single-Stranded Oligonucleotides and PEG-b-guanidinylated Polypeptides for Intracavity Encapsulation of Effector Enzymes Aimed at Cooperative Gene Knockdown. Biomacromolecules, 21(10), 4365-4376. https://doi.org/10.1021/acs.biomac.0c01192

Noncovalent Stabilization of Vesicular Polyion Complexes with Chemically Modified/Single-Stranded Oligonucleotides and PEG-b-guanidinylated Polypeptides for Intracavity Encapsulation of Effector Enzymes Aimed at Cooperative Gene Knockdown. / Kim, Beob Soo; Naito, Mitsuru; Chaya, Hiroyuki et al.
In: Biomacromolecules, Vol. 21, No. 10, 12.10.2020, p. 4365-4376.

Research output: Contribution to journal › Article › peer-review

Kim, BS, Naito, M, Chaya, H, Hori, M, Hayashi, K, Min, HS, Yi, Y, Kim, HJ, Nagata, T, Anraku, Y, Kishimura, A, Kataoka, K & Miyata, K 2020, 'Noncovalent Stabilization of Vesicular Polyion Complexes with Chemically Modified/Single-Stranded Oligonucleotides and PEG-b-guanidinylated Polypeptides for Intracavity Encapsulation of Effector Enzymes Aimed at Cooperative Gene Knockdown', Biomacromolecules, vol. 21, no. 10, pp. 4365-4376. https://doi.org/10.1021/acs.biomac.0c01192

Kim BS, Naito M, Chaya H, Hori M, Hayashi K, Min HS et al. Noncovalent Stabilization of Vesicular Polyion Complexes with Chemically Modified/Single-Stranded Oligonucleotides and PEG-b-guanidinylated Polypeptides for Intracavity Encapsulation of Effector Enzymes Aimed at Cooperative Gene Knockdown. Biomacromolecules. 2020 Oct 12;21(10):4365-4376. doi: 10.1021/acs.biomac.0c01192

@article{08fe873f91a94e63a08d429c529dfbb0,

title = "Noncovalent Stabilization of Vesicular Polyion Complexes with Chemically Modified/Single-Stranded Oligonucleotides and PEG-b-guanidinylated Polypeptides for Intracavity Encapsulation of Effector Enzymes Aimed at Cooperative Gene Knockdown",

abstract = "For the simultaneous delivery of antisense oligonucleotides and their effector enzymes into cells, nanosized vesicular polyion complexes (PICs) were fabricated from oppositely charged polyion pairs of oligonucleotides and poly(ethylene glycol) (PEG)-b-polypeptides. First, the polyion component structures were carefully designed to facilitate a multimolecular (or secondary) association of unit PICs for noncovalent (or chemical cross-linking-free) stabilization of vesicular PICs. Chemically modified, single-stranded oligonucleotides (SSOs) dramatically stabilized the multimolecular associates under physiological conditions, compared to control SSOs without chemical modifications and duplex oligonucleotides. In addition, a high degree of guanidino groups in the polypeptide segment was also crucial for the high stability of multimolecular associates. Dynamic light scattering and transmission electron microscopy revealed the stabilized multimolecular associates to have a 100 nm sized vesicular architecture with a narrow size distribution. The loading number of SSOs per nanovesicle was determined to be {\^a}2500 using fluorescence correlation spectroscopic analyses with fluorescently labeled SSOs. Furthermore, the nanovesicle stably encapsulated ribonuclease H (RNase H) as an effector enzyme at {\^a}10 per nanovesicle through simple vortex-mixing with preformed nanovesicles. Ultimately, the RNase H-encapsulated nanovesicle efficiently delivered SSOs with RNase H into cultured cancer cells, thereby eliciting the significantly higher gene knockdown compared with empty nanovesicles (without RNase H) or a mixture of nanovesicles with RNase H without encapsulation. These results demonstrate the great potential of noncovalently stabilized nanovesicles for the codelivery of two varying bio-macromolecule payloads for ensuring their cooperative biological activity.",

author = "Kim, {Beob Soo} and Mitsuru Naito and Hiroyuki Chaya and Mao Hori and Kotaro Hayashi and Min, {Hyun Su} and Yu Yi and Kim, {Hyun Jin} and Tetsuya Nagata and Yasutaka Anraku and Akihiro Kishimura and Kazunori Kataoka and Kanjiro Miyata",

note = "Funding Information: This research was financially supported by the Center of Innovation (COI) Program (Grant Number: JPMJCE1305) from the Japan Science and Technology Agency (JST), Basic Science and Platform Technology Program for Innovative Biological Medicine (IBIOMED) from Japan Agency for Medical Research and Development (AMED), Grants-in-Aid for Scientific Research of MEXT of Japan (JSPS KAKENHI Grant Numbers 18 K19900 and 20H00658 for K.M. and 18H03534 for A.K.), and a grant JSPS Core-to-Core Program (Grant Number JPJSCCS20170007). We are grateful to Dr. S. Fukuda and Mr. H. Hoshi, The University of Tokyo, and the Research Hub for Advanced Nano Characterization at The University of Tokyo for their valuable support in TEM observations. Publisher Copyright: Copyright {\textcopyright} 2020 American Chemical Society.",

year = "2020",

month = oct,

day = "12",

doi = "10.1021/acs.biomac.0c01192",

language = "English",

volume = "21",

pages = "4365--4376",

journal = "Biomacromolecules",

issn = "1525-7797",

publisher = "American Chemical Society",

number = "10",

}

TY - JOUR

T1 - Noncovalent Stabilization of Vesicular Polyion Complexes with Chemically Modified/Single-Stranded Oligonucleotides and PEG-b-guanidinylated Polypeptides for Intracavity Encapsulation of Effector Enzymes Aimed at Cooperative Gene Knockdown

AU - Kim, Beob Soo

AU - Naito, Mitsuru

AU - Chaya, Hiroyuki

AU - Hori, Mao

AU - Hayashi, Kotaro

AU - Min, Hyun Su

AU - Yi, Yu

AU - Kim, Hyun Jin

AU - Nagata, Tetsuya

AU - Anraku, Yasutaka

AU - Kishimura, Akihiro

AU - Kataoka, Kazunori

AU - Miyata, Kanjiro

N1 - Funding Information: This research was financially supported by the Center of Innovation (COI) Program (Grant Number: JPMJCE1305) from the Japan Science and Technology Agency (JST), Basic Science and Platform Technology Program for Innovative Biological Medicine (IBIOMED) from Japan Agency for Medical Research and Development (AMED), Grants-in-Aid for Scientific Research of MEXT of Japan (JSPS KAKENHI Grant Numbers 18 K19900 and 20H00658 for K.M. and 18H03534 for A.K.), and a grant JSPS Core-to-Core Program (Grant Number JPJSCCS20170007). We are grateful to Dr. S. Fukuda and Mr. H. Hoshi, The University of Tokyo, and the Research Hub for Advanced Nano Characterization at The University of Tokyo for their valuable support in TEM observations. Publisher Copyright: Copyright © 2020 American Chemical Society.

PY - 2020/10/12

Y1 - 2020/10/12

N2 - For the simultaneous delivery of antisense oligonucleotides and their effector enzymes into cells, nanosized vesicular polyion complexes (PICs) were fabricated from oppositely charged polyion pairs of oligonucleotides and poly(ethylene glycol) (PEG)-b-polypeptides. First, the polyion component structures were carefully designed to facilitate a multimolecular (or secondary) association of unit PICs for noncovalent (or chemical cross-linking-free) stabilization of vesicular PICs. Chemically modified, single-stranded oligonucleotides (SSOs) dramatically stabilized the multimolecular associates under physiological conditions, compared to control SSOs without chemical modifications and duplex oligonucleotides. In addition, a high degree of guanidino groups in the polypeptide segment was also crucial for the high stability of multimolecular associates. Dynamic light scattering and transmission electron microscopy revealed the stabilized multimolecular associates to have a 100 nm sized vesicular architecture with a narrow size distribution. The loading number of SSOs per nanovesicle was determined to be â2500 using fluorescence correlation spectroscopic analyses with fluorescently labeled SSOs. Furthermore, the nanovesicle stably encapsulated ribonuclease H (RNase H) as an effector enzyme at â10 per nanovesicle through simple vortex-mixing with preformed nanovesicles. Ultimately, the RNase H-encapsulated nanovesicle efficiently delivered SSOs with RNase H into cultured cancer cells, thereby eliciting the significantly higher gene knockdown compared with empty nanovesicles (without RNase H) or a mixture of nanovesicles with RNase H without encapsulation. These results demonstrate the great potential of noncovalently stabilized nanovesicles for the codelivery of two varying bio-macromolecule payloads for ensuring their cooperative biological activity.

AB - For the simultaneous delivery of antisense oligonucleotides and their effector enzymes into cells, nanosized vesicular polyion complexes (PICs) were fabricated from oppositely charged polyion pairs of oligonucleotides and poly(ethylene glycol) (PEG)-b-polypeptides. First, the polyion component structures were carefully designed to facilitate a multimolecular (or secondary) association of unit PICs for noncovalent (or chemical cross-linking-free) stabilization of vesicular PICs. Chemically modified, single-stranded oligonucleotides (SSOs) dramatically stabilized the multimolecular associates under physiological conditions, compared to control SSOs without chemical modifications and duplex oligonucleotides. In addition, a high degree of guanidino groups in the polypeptide segment was also crucial for the high stability of multimolecular associates. Dynamic light scattering and transmission electron microscopy revealed the stabilized multimolecular associates to have a 100 nm sized vesicular architecture with a narrow size distribution. The loading number of SSOs per nanovesicle was determined to be â2500 using fluorescence correlation spectroscopic analyses with fluorescently labeled SSOs. Furthermore, the nanovesicle stably encapsulated ribonuclease H (RNase H) as an effector enzyme at â10 per nanovesicle through simple vortex-mixing with preformed nanovesicles. Ultimately, the RNase H-encapsulated nanovesicle efficiently delivered SSOs with RNase H into cultured cancer cells, thereby eliciting the significantly higher gene knockdown compared with empty nanovesicles (without RNase H) or a mixture of nanovesicles with RNase H without encapsulation. These results demonstrate the great potential of noncovalently stabilized nanovesicles for the codelivery of two varying bio-macromolecule payloads for ensuring their cooperative biological activity.

UR - http://www.scopus.com/inward/record.url?scp=85092803023&partnerID=8YFLogxK

UR - http://www.scopus.com/inward/citedby.url?scp=85092803023&partnerID=8YFLogxK

U2 - 10.1021/acs.biomac.0c01192

DO - 10.1021/acs.biomac.0c01192

M3 - Article

C2 - 32924444

AN - SCOPUS:85092803023

SN - 1525-7797

VL - 21

SP - 4365

EP - 4376

JO - Biomacromolecules

JF - Biomacromolecules

IS - 10

ER -

Noncovalent Stabilization of Vesicular Polyion Complexes with Chemically Modified/Single-Stranded Oligonucleotides and PEG-b-guanidinylated Polypeptides for Intracavity Encapsulation of Effector Enzymes Aimed at Cooperative Gene Knockdown

Abstract

All Science Journal Classification (ASJC) codes

UN SDGs

Access to Document

Other files and links

Fingerprint

Cite this