Liver as an ideal target for gene therapy: expression of CTLA4Ig by retroviral gene transfer.

Siu Tim Cheung; Tung Yu Tsui; Wei Lin Wang; Zhen Fan Yang; San Yu Wong; Ying Chi Ip; John Luk; Sheung Tat Fan

Liver as an ideal target for gene therapy: expression of CTLA4Ig by retroviral gene transfer.

Standard

Liver as an ideal target for gene therapy: expression of CTLA4Ig by retroviral gene transfer. / Cheung, Siu Tim; Tsui, Tung Yu; Wang, Wei Lin; Yang, Zhen Fan; Wong, San Yu; Ip, Ying Chi; Luk, John; Fan, Sheung Tat.

In: J GASTROEN HEPATOL, Vol. 17, No. 9, 9, 2002, p. 1008-1014.

Research output: SCORING: Contribution to journal › SCORING: Journal article › Research › peer-review

Harvard

Cheung, ST, Tsui, TY, Wang, WL, Yang, ZF, Wong, SY, Ip, YC, Luk, J & Fan, ST 2002, 'Liver as an ideal target for gene therapy: expression of CTLA4Ig by retroviral gene transfer.', J GASTROEN HEPATOL, vol. 17, no. 9, 9, pp. 1008-1014. <http://www.ncbi.nlm.nih.gov/pubmed/12167123?dopt=Citation>

APA

Cheung, S. T., Tsui, T. Y., Wang, W. L., Yang, Z. F., Wong, S. Y., Ip, Y. C., Luk, J., & Fan, S. T. (2002). Liver as an ideal target for gene therapy: expression of CTLA4Ig by retroviral gene transfer. J GASTROEN HEPATOL, 17(9), 1008-1014. [9]. http://www.ncbi.nlm.nih.gov/pubmed/12167123?dopt=Citation

Vancouver

Cheung ST, Tsui TY, Wang WL, Yang ZF, Wong SY, Ip YC et al. Liver as an ideal target for gene therapy: expression of CTLA4Ig by retroviral gene transfer. J GASTROEN HEPATOL. 2002;17(9):1008-1014. 9.

Bibtex

@article{a083eaafefcb476fac201ea44a56796e,

title = "Liver as an ideal target for gene therapy: expression of CTLA4Ig by retroviral gene transfer.",

abstract = "BACKGROUND AND AIMS: Liver has been a target organ for gene therapy as it plays a central role in metabolism and production of serum proteins. Many metabolic disorders result from a deficiency of liver-derived protein products. In transplantation settings, modulation of the immune responses caused by CTLA4Ig protein has been shown to be an attractive direction. In this study, we investigated the efficacy of hepatocyte transduction via introduction of the exogenous CTLA4Ig gene to the rat liver graft by retrovirus vector, and examined the presence of target serum protein after gene transfers. METHODS: We constructed a replication defective retroviral vector that contained the CTLA4Ig gene. The liver graft regeneration index was first examined by 5-bromo-2-deoxyuridine, Ki-67 and proliferating cell nuclear antigen antibodies to determine the optimal time of gene transduction. The liver graft was then perfused with the retroviral vector, and animals were killed at constant time points to examine for the presence of CTLA4 protein in the graft and peripheral blood. RESULTS: CTLA4 protein was detected on postoperative days 5, 9 and 14, with liver graft tissue transduction indexes of 7.2, 10.9 and 1.8, respectively. Blood protein levels were at 151.6, 26.5 and 21.4 rhog/mL, respectively. A transduction index reaching 22.1 was observed in the graft with the most rapid liver regeneration. CONCLUSIONS: We had established the gene delivery model in rat with auxiliary partial liver transplantation. Expression of the exogenous gene delivered by retrovirus was demonstrated in the liver with secretion of diffusible protein in the bloodstream. The present study provides important information for gene transfer using the liver to produce the target protein in situ and as serum protein. This will also be applicable to the treatment of other metabolic diseases.",

author = "Cheung, {Siu Tim} and Tsui, {Tung Yu} and Wang, {Wei Lin} and Yang, {Zhen Fan} and Wong, {San Yu} and Ip, {Ying Chi} and John Luk and Fan, {Sheung Tat}",

year = "2002",

language = "Deutsch",

volume = "17",

pages = "1008--1014",

journal = "J GASTROEN HEPATOL",

issn = "0815-9319",

publisher = "Wiley-Blackwell",

number = "9",

}

RIS

TY - JOUR

T1 - Liver as an ideal target for gene therapy: expression of CTLA4Ig by retroviral gene transfer.

AU - Cheung, Siu Tim

AU - Tsui, Tung Yu

AU - Wang, Wei Lin

AU - Yang, Zhen Fan

AU - Wong, San Yu

AU - Ip, Ying Chi

AU - Luk, John

AU - Fan, Sheung Tat

PY - 2002

Y1 - 2002

N2 - BACKGROUND AND AIMS: Liver has been a target organ for gene therapy as it plays a central role in metabolism and production of serum proteins. Many metabolic disorders result from a deficiency of liver-derived protein products. In transplantation settings, modulation of the immune responses caused by CTLA4Ig protein has been shown to be an attractive direction. In this study, we investigated the efficacy of hepatocyte transduction via introduction of the exogenous CTLA4Ig gene to the rat liver graft by retrovirus vector, and examined the presence of target serum protein after gene transfers. METHODS: We constructed a replication defective retroviral vector that contained the CTLA4Ig gene. The liver graft regeneration index was first examined by 5-bromo-2-deoxyuridine, Ki-67 and proliferating cell nuclear antigen antibodies to determine the optimal time of gene transduction. The liver graft was then perfused with the retroviral vector, and animals were killed at constant time points to examine for the presence of CTLA4 protein in the graft and peripheral blood. RESULTS: CTLA4 protein was detected on postoperative days 5, 9 and 14, with liver graft tissue transduction indexes of 7.2, 10.9 and 1.8, respectively. Blood protein levels were at 151.6, 26.5 and 21.4 rhog/mL, respectively. A transduction index reaching 22.1 was observed in the graft with the most rapid liver regeneration. CONCLUSIONS: We had established the gene delivery model in rat with auxiliary partial liver transplantation. Expression of the exogenous gene delivered by retrovirus was demonstrated in the liver with secretion of diffusible protein in the bloodstream. The present study provides important information for gene transfer using the liver to produce the target protein in situ and as serum protein. This will also be applicable to the treatment of other metabolic diseases.

AB - BACKGROUND AND AIMS: Liver has been a target organ for gene therapy as it plays a central role in metabolism and production of serum proteins. Many metabolic disorders result from a deficiency of liver-derived protein products. In transplantation settings, modulation of the immune responses caused by CTLA4Ig protein has been shown to be an attractive direction. In this study, we investigated the efficacy of hepatocyte transduction via introduction of the exogenous CTLA4Ig gene to the rat liver graft by retrovirus vector, and examined the presence of target serum protein after gene transfers. METHODS: We constructed a replication defective retroviral vector that contained the CTLA4Ig gene. The liver graft regeneration index was first examined by 5-bromo-2-deoxyuridine, Ki-67 and proliferating cell nuclear antigen antibodies to determine the optimal time of gene transduction. The liver graft was then perfused with the retroviral vector, and animals were killed at constant time points to examine for the presence of CTLA4 protein in the graft and peripheral blood. RESULTS: CTLA4 protein was detected on postoperative days 5, 9 and 14, with liver graft tissue transduction indexes of 7.2, 10.9 and 1.8, respectively. Blood protein levels were at 151.6, 26.5 and 21.4 rhog/mL, respectively. A transduction index reaching 22.1 was observed in the graft with the most rapid liver regeneration. CONCLUSIONS: We had established the gene delivery model in rat with auxiliary partial liver transplantation. Expression of the exogenous gene delivered by retrovirus was demonstrated in the liver with secretion of diffusible protein in the bloodstream. The present study provides important information for gene transfer using the liver to produce the target protein in situ and as serum protein. This will also be applicable to the treatment of other metabolic diseases.

M3 - SCORING: Zeitschriftenaufsatz

VL - 17

SP - 1008

EP - 1014

JO - J GASTROEN HEPATOL

JF - J GASTROEN HEPATOL

SN - 0815-9319

IS - 9

M1 - 9

ER -