The effects of mesenchymal stem cells injected via different routes on modified IL-12-mediated antitumor activity

S. H. Seo; K. S. Kim; S. H. Park; Y. S. Suh; S. J. Kim; S. S. Jeun; Y. C. Sung

doi:10.1038/gt.2010.170

The effects of mesenchymal stem cells injected via different routes on modified IL-12-mediated antitumor activity

S. H. Seo
, K. S. Kim
, S. H. Park
, Y. S. Suh
, S. J. Kim
, S. S. Jeun
, Y. C. Sung

Department of Neurosurgery

Pohang University of Science and Technology
Genexine, Inc.

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

142 Scopus citations

Abstract

Owing to its tumor tropism and prolonged transgene expression, mesenchymal stem cell (MSC) has been considered as an ideal delivery vehicle for cancer gene therapies or therapeutic vaccines. In this study, we demonstrated that intratumoral (i.t.) injection of MSCs expressing modified interleukin-12 (MSCs/IL-12M) exhibited stronger tumor-specific T-cell responses and antitumor effects as well as more sustained expressions of IL-12 and interferon (IFN)-γ in both sera and tumor sites than did IL-12M-expressing adenovirus (rAd/IL-12M) in mice bearing both solid and metastatic tumors. Subcutaneous (s.c.) injection of MSCs/IL-12M at contralateral site of tumor exhibited similar levels of serum IL-12 and IFN-γ as i.t. injection, but much weaker antitumor effects in both B16F10 melanoma and TC-1 cervical cancer models than i.t. injection. Although intravenous (i.v.) injection elicited earlier peak serum levels of cytokines, it induced weaker tumor-specific T-cell responses and antitumor effects than i.t. injection, indicating that serum cytokine levels are not surrogate indicators of antitumor effects. Taken together, these results indicated that MSC is more efficient than adenovirus as a cytokine gene delivery vehicle and that i.t. injection of MSCs/IL-12M is the best approach to induce strong tumor-specific T-cell responses that correlate with anti-metastatic effects as well as inhibition of solid tumor growth, although MSCs themselves have an ability to migrate into the tumor site. In addition, MSCs/IL-12M embedded in Matrigel (MSCs/IL-12M/Matrigel) exhibited significant antitumor effects even in immunodeficient mice such as SCID and BNX mice lacking T, B and natural killer (NK) cells, but not in IFN-γ knockout mice. Our findings provide an optimal approach for designing an efficient clinical protocol of MSC-based cytokine gene therapy to induce strong tumor-specific T-cell responses and therapeutic anticancer efficacy.

Original language	English
Pages (from-to)	488-495
Number of pages	8
Journal	Gene Therapy
Volume	18
Issue number	5
DOIs	https://doi.org/10.1038/gt.2010.170
State	Published - May 2011

Bibliographical note

Funding Information:
We would like to thank Sang-Chun Lee, Kwan-Seok Lee and Bok-Chae Cho for their devoted animal care, Hong-Hwa Jun for technical assistance, and Dr Chang-Yul Kang for providing the clone 2.43. The Korean Healthcare Technology Research and Development Project, Ministry for Health, Welfare and Family Affairs, Republic of Korea, grant no. A091205-0911-0000300.

UN SDGs

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

SDG 3 Good Health and Well-being

Keywords

Matrigel
injection route
interleukin-12
mesenchymal stem cell
metastasis

Access to Document

10.1038/gt.2010.170

Cite this

@article{7e24619f330e4484af83739643f3e7c8,

title = "The effects of mesenchymal stem cells injected via different routes on modified IL-12-mediated antitumor activity",

abstract = "Owing to its tumor tropism and prolonged transgene expression, mesenchymal stem cell (MSC) has been considered as an ideal delivery vehicle for cancer gene therapies or therapeutic vaccines. In this study, we demonstrated that intratumoral (i.t.) injection of MSCs expressing modified interleukin-12 (MSCs/IL-12M) exhibited stronger tumor-specific T-cell responses and antitumor effects as well as more sustained expressions of IL-12 and interferon (IFN)-γ in both sera and tumor sites than did IL-12M-expressing adenovirus (rAd/IL-12M) in mice bearing both solid and metastatic tumors. Subcutaneous (s.c.) injection of MSCs/IL-12M at contralateral site of tumor exhibited similar levels of serum IL-12 and IFN-γ as i.t. injection, but much weaker antitumor effects in both B16F10 melanoma and TC-1 cervical cancer models than i.t. injection. Although intravenous (i.v.) injection elicited earlier peak serum levels of cytokines, it induced weaker tumor-specific T-cell responses and antitumor effects than i.t. injection, indicating that serum cytokine levels are not surrogate indicators of antitumor effects. Taken together, these results indicated that MSC is more efficient than adenovirus as a cytokine gene delivery vehicle and that i.t. injection of MSCs/IL-12M is the best approach to induce strong tumor-specific T-cell responses that correlate with anti-metastatic effects as well as inhibition of solid tumor growth, although MSCs themselves have an ability to migrate into the tumor site. In addition, MSCs/IL-12M embedded in Matrigel (MSCs/IL-12M/Matrigel) exhibited significant antitumor effects even in immunodeficient mice such as SCID and BNX mice lacking T, B and natural killer (NK) cells, but not in IFN-γ knockout mice. Our findings provide an optimal approach for designing an efficient clinical protocol of MSC-based cytokine gene therapy to induce strong tumor-specific T-cell responses and therapeutic anticancer efficacy.",

keywords = "Matrigel, injection route, interleukin-12, mesenchymal stem cell, metastasis",

author = "Seo, \{S. H.\} and Kim, \{K. S.\} and Park, \{S. H.\} and Suh, \{Y. S.\} and Kim, \{S. J.\} and Jeun, \{S. S.\} and Sung, \{Y. C.\}",

note = "Funding Information: We would like to thank Sang-Chun Lee, Kwan-Seok Lee and Bok-Chae Cho for their devoted animal care, Hong-Hwa Jun for technical assistance, and Dr Chang-Yul Kang for providing the clone 2.43. The Korean Healthcare Technology Research and Development Project, Ministry for Health, Welfare and Family Affairs, Republic of Korea, grant no. A091205-0911-0000300.",

year = "2011",

month = may,

doi = "10.1038/gt.2010.170",

language = "English",

volume = "18",

pages = "488--495",

journal = "Gene Therapy",

issn = "0969-7128",

publisher = "Springer Nature",

number = "5",

}

TY - JOUR

T1 - The effects of mesenchymal stem cells injected via different routes on modified IL-12-mediated antitumor activity

AU - Seo, S. H.

AU - Kim, K. S.

AU - Park, S. H.

AU - Suh, Y. S.

AU - Kim, S. J.

AU - Jeun, S. S.

AU - Sung, Y. C.

N1 - Funding Information: We would like to thank Sang-Chun Lee, Kwan-Seok Lee and Bok-Chae Cho for their devoted animal care, Hong-Hwa Jun for technical assistance, and Dr Chang-Yul Kang for providing the clone 2.43. The Korean Healthcare Technology Research and Development Project, Ministry for Health, Welfare and Family Affairs, Republic of Korea, grant no. A091205-0911-0000300.

PY - 2011/5

Y1 - 2011/5

N2 - Owing to its tumor tropism and prolonged transgene expression, mesenchymal stem cell (MSC) has been considered as an ideal delivery vehicle for cancer gene therapies or therapeutic vaccines. In this study, we demonstrated that intratumoral (i.t.) injection of MSCs expressing modified interleukin-12 (MSCs/IL-12M) exhibited stronger tumor-specific T-cell responses and antitumor effects as well as more sustained expressions of IL-12 and interferon (IFN)-γ in both sera and tumor sites than did IL-12M-expressing adenovirus (rAd/IL-12M) in mice bearing both solid and metastatic tumors. Subcutaneous (s.c.) injection of MSCs/IL-12M at contralateral site of tumor exhibited similar levels of serum IL-12 and IFN-γ as i.t. injection, but much weaker antitumor effects in both B16F10 melanoma and TC-1 cervical cancer models than i.t. injection. Although intravenous (i.v.) injection elicited earlier peak serum levels of cytokines, it induced weaker tumor-specific T-cell responses and antitumor effects than i.t. injection, indicating that serum cytokine levels are not surrogate indicators of antitumor effects. Taken together, these results indicated that MSC is more efficient than adenovirus as a cytokine gene delivery vehicle and that i.t. injection of MSCs/IL-12M is the best approach to induce strong tumor-specific T-cell responses that correlate with anti-metastatic effects as well as inhibition of solid tumor growth, although MSCs themselves have an ability to migrate into the tumor site. In addition, MSCs/IL-12M embedded in Matrigel (MSCs/IL-12M/Matrigel) exhibited significant antitumor effects even in immunodeficient mice such as SCID and BNX mice lacking T, B and natural killer (NK) cells, but not in IFN-γ knockout mice. Our findings provide an optimal approach for designing an efficient clinical protocol of MSC-based cytokine gene therapy to induce strong tumor-specific T-cell responses and therapeutic anticancer efficacy.

AB - Owing to its tumor tropism and prolonged transgene expression, mesenchymal stem cell (MSC) has been considered as an ideal delivery vehicle for cancer gene therapies or therapeutic vaccines. In this study, we demonstrated that intratumoral (i.t.) injection of MSCs expressing modified interleukin-12 (MSCs/IL-12M) exhibited stronger tumor-specific T-cell responses and antitumor effects as well as more sustained expressions of IL-12 and interferon (IFN)-γ in both sera and tumor sites than did IL-12M-expressing adenovirus (rAd/IL-12M) in mice bearing both solid and metastatic tumors. Subcutaneous (s.c.) injection of MSCs/IL-12M at contralateral site of tumor exhibited similar levels of serum IL-12 and IFN-γ as i.t. injection, but much weaker antitumor effects in both B16F10 melanoma and TC-1 cervical cancer models than i.t. injection. Although intravenous (i.v.) injection elicited earlier peak serum levels of cytokines, it induced weaker tumor-specific T-cell responses and antitumor effects than i.t. injection, indicating that serum cytokine levels are not surrogate indicators of antitumor effects. Taken together, these results indicated that MSC is more efficient than adenovirus as a cytokine gene delivery vehicle and that i.t. injection of MSCs/IL-12M is the best approach to induce strong tumor-specific T-cell responses that correlate with anti-metastatic effects as well as inhibition of solid tumor growth, although MSCs themselves have an ability to migrate into the tumor site. In addition, MSCs/IL-12M embedded in Matrigel (MSCs/IL-12M/Matrigel) exhibited significant antitumor effects even in immunodeficient mice such as SCID and BNX mice lacking T, B and natural killer (NK) cells, but not in IFN-γ knockout mice. Our findings provide an optimal approach for designing an efficient clinical protocol of MSC-based cytokine gene therapy to induce strong tumor-specific T-cell responses and therapeutic anticancer efficacy.

KW - Matrigel

KW - injection route

KW - interleukin-12

KW - mesenchymal stem cell

KW - metastasis

UR - https://www.scopus.com/pages/publications/79955943420

U2 - 10.1038/gt.2010.170

DO - 10.1038/gt.2010.170

M3 - Article

C2 - 21228885

AN - SCOPUS:79955943420

SN - 0969-7128

VL - 18

SP - 488

EP - 495

JO - Gene Therapy

JF - Gene Therapy

IS - 5

ER -

The effects of mesenchymal stem cells injected via different routes on modified IL-12-mediated antitumor activity

Abstract

Bibliographical note

UN SDGs

Keywords

Access to Document

Other files and links

Fingerprint

Cite this