Regulatable gene expression systems for gene therapy applications: Progress and future challenges

S. Goverdhana; M. Puntel; W. Xiong; J. M. Zirger; C. Barcia; J. F. Curtin; E. B. Soffer; S. Mondkar; G. D. King; J. Hu; S. A. Sciascia; M. Candolfi; D. S. Greengold; P. R. Lowenstein; M. G. Castro

doi:10.1016/j.ymthe.2005.03.022

Regulatable gene expression systems for gene therapy applications: Progress and future challenges

S. Goverdhana, M. Puntel, W. Xiong, J. M. Zirger, C. Barcia, J. F. Curtin, E. B. Soffer, S. Mondkar, G. D. King, J. Hu, S. A. Sciascia, M. Candolfi, D. S. Greengold, P. R. Lowenstein, M. G. Castro^*

^*Autor corresponent d’aquest treball

University of California at Los Angeles (UCLA)

Producció científica: Contribució a revista › Article de revisió › Recerca › Avaluat per experts

246 Cites (Scopus)

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Gene therapy aims to revert diseased phenotypes by the use of both viral and nonviral gene delivery systems. Substantial progress has been made in making gene transfer vehicles more efficient, less toxic, and nonimmunogenic and in allowing long-term transgene expression. One of the key issues in successfully implementing gene therapies in the clinical setting is to be able to regulate gene expression very tightly and consistently as and when it is needed. The regulation ought to be achievable using a compound that should be nontoxic, be able to penetrate into the desired target tissue or organ, and have a half-life of a few hours (as opposed to minutes or days) so that when withdrawn or added (depending on the regulatable system used) gene expression can be turned "on" or "off" quickly and effectively. Also, the genetic switches employed should ideally be nonimmunogenic in the host. The ability to switch transgenes on and off would be of paramount importance not only when the therapy is no longer needed, but also in the case of the development of adverse side effects to the therapy. Many regulatable systems are currently under development and some, i.e., the tetracycline-dependent transcriptional switch, have been used successfully for in vivo preclinical applications. Despite this, there are no examples of switches that have been employed in a human clinical trial. In this review, we aim to highlight the main regulatable systems currently under development, the gene transfer systems employed for their expression, and also the preclinical models in which they have been used successfully. We also discuss the substantial challenges that still remain before these regulatable switches can be employed in the clinical setting.

Idioma original	Anglès
Pàgines (de-a)	189-211
Nombre de pàgines	23
Revista	Molecular Therapy
Volum	12
Número	2
DOIs	https://doi.org/10.1016/j.ymthe.2005.03.022
Estat de la publicació	Publicada - d’ag. 2005

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10.1016/j.ymthe.2005.03.022

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Goverdhana, S., Puntel, M., Xiong, W., Zirger, J. M., Barcia, C., Curtin, J. F., Soffer, E. B., Mondkar, S., King, G. D., Hu, J., Sciascia, S. A., Candolfi, M., Greengold, D. S., Lowenstein, P. R., & Castro, M. G. (2005). Regulatable gene expression systems for gene therapy applications: Progress and future challenges. Molecular Therapy, 12(2), 189-211. https://doi.org/10.1016/j.ymthe.2005.03.022

@article{6d52540538c94a34a996086fecca3260,

title = "Regulatable gene expression systems for gene therapy applications: Progress and future challenges",

abstract = "Gene therapy aims to revert diseased phenotypes by the use of both viral and nonviral gene delivery systems. Substantial progress has been made in making gene transfer vehicles more efficient, less toxic, and nonimmunogenic and in allowing long-term transgene expression. One of the key issues in successfully implementing gene therapies in the clinical setting is to be able to regulate gene expression very tightly and consistently as and when it is needed. The regulation ought to be achievable using a compound that should be nontoxic, be able to penetrate into the desired target tissue or organ, and have a half-life of a few hours (as opposed to minutes or days) so that when withdrawn or added (depending on the regulatable system used) gene expression can be turned {"}on{"} or {"}off{"} quickly and effectively. Also, the genetic switches employed should ideally be nonimmunogenic in the host. The ability to switch transgenes on and off would be of paramount importance not only when the therapy is no longer needed, but also in the case of the development of adverse side effects to the therapy. Many regulatable systems are currently under development and some, i.e., the tetracycline-dependent transcriptional switch, have been used successfully for in vivo preclinical applications. Despite this, there are no examples of switches that have been employed in a human clinical trial. In this review, we aim to highlight the main regulatable systems currently under development, the gene transfer systems employed for their expression, and also the preclinical models in which they have been used successfully. We also discuss the substantial challenges that still remain before these regulatable switches can be employed in the clinical setting.",

author = "S. Goverdhana and M. Puntel and W. Xiong and Zirger, {J. M.} and C. Barcia and Curtin, {J. F.} and Soffer, {E. B.} and S. Mondkar and King, {G. D.} and J. Hu and Sciascia, {S. A.} and M. Candolfi and Greengold, {D. S.} and Lowenstein, {P. R.} and Castro, {M. G.}",

note = "Funding Information: Work described in this review is funded by the National Institute of Neurological Disorders & Stroke (NINDS), Grant 1 R01 NS44556.01; by NIDDK Grant 1 RO3 TW006273-01 to M.G.C.; by NINDS Grants 1 RO1 NS42893, U54 4 NS04-5309, and R21 NS47298 to P.R.L.; by The Linda Tallen & David Paul Kane Annual Fellowship to M.G.C. and P.R.L.; and by the Board of Governors at Cedars–Sinai Medical Center. We also thank the unparalleled support and academic leadership of Dr. Shlomo Melmed. We are grateful to Mr. Richard Katzman and Dr. David Meyer for their superb administrative support.",

year = "2005",

month = aug,

doi = "10.1016/j.ymthe.2005.03.022",

language = "English",

volume = "12",

pages = "189--211",

journal = "Molecular Therapy",

issn = "1525-0016",

number = "2",

}

Goverdhana, S, Puntel, M, Xiong, W, Zirger, JM, Barcia, C, Curtin, JF, Soffer, EB, Mondkar, S, King, GD, Hu, J, Sciascia, SA, Candolfi, M, Greengold, DS, Lowenstein, PR & Castro, MG 2005, 'Regulatable gene expression systems for gene therapy applications: Progress and future challenges', Molecular Therapy, vol. 12, núm. 2, pàg. 189-211. https://doi.org/10.1016/j.ymthe.2005.03.022

TY - JOUR

T1 - Regulatable gene expression systems for gene therapy applications

T2 - Progress and future challenges

AU - Goverdhana, S.

AU - Puntel, M.

AU - Xiong, W.

AU - Zirger, J. M.

AU - Barcia, C.

AU - Curtin, J. F.

AU - Soffer, E. B.

AU - Mondkar, S.

AU - King, G. D.

AU - Hu, J.

AU - Sciascia, S. A.

AU - Candolfi, M.

AU - Greengold, D. S.

AU - Lowenstein, P. R.

AU - Castro, M. G.

N1 - Funding Information: Work described in this review is funded by the National Institute of Neurological Disorders & Stroke (NINDS), Grant 1 R01 NS44556.01; by NIDDK Grant 1 RO3 TW006273-01 to M.G.C.; by NINDS Grants 1 RO1 NS42893, U54 4 NS04-5309, and R21 NS47298 to P.R.L.; by The Linda Tallen & David Paul Kane Annual Fellowship to M.G.C. and P.R.L.; and by the Board of Governors at Cedars–Sinai Medical Center. We also thank the unparalleled support and academic leadership of Dr. Shlomo Melmed. We are grateful to Mr. Richard Katzman and Dr. David Meyer for their superb administrative support.

PY - 2005/8

Y1 - 2005/8

N2 - Gene therapy aims to revert diseased phenotypes by the use of both viral and nonviral gene delivery systems. Substantial progress has been made in making gene transfer vehicles more efficient, less toxic, and nonimmunogenic and in allowing long-term transgene expression. One of the key issues in successfully implementing gene therapies in the clinical setting is to be able to regulate gene expression very tightly and consistently as and when it is needed. The regulation ought to be achievable using a compound that should be nontoxic, be able to penetrate into the desired target tissue or organ, and have a half-life of a few hours (as opposed to minutes or days) so that when withdrawn or added (depending on the regulatable system used) gene expression can be turned "on" or "off" quickly and effectively. Also, the genetic switches employed should ideally be nonimmunogenic in the host. The ability to switch transgenes on and off would be of paramount importance not only when the therapy is no longer needed, but also in the case of the development of adverse side effects to the therapy. Many regulatable systems are currently under development and some, i.e., the tetracycline-dependent transcriptional switch, have been used successfully for in vivo preclinical applications. Despite this, there are no examples of switches that have been employed in a human clinical trial. In this review, we aim to highlight the main regulatable systems currently under development, the gene transfer systems employed for their expression, and also the preclinical models in which they have been used successfully. We also discuss the substantial challenges that still remain before these regulatable switches can be employed in the clinical setting.

AB - Gene therapy aims to revert diseased phenotypes by the use of both viral and nonviral gene delivery systems. Substantial progress has been made in making gene transfer vehicles more efficient, less toxic, and nonimmunogenic and in allowing long-term transgene expression. One of the key issues in successfully implementing gene therapies in the clinical setting is to be able to regulate gene expression very tightly and consistently as and when it is needed. The regulation ought to be achievable using a compound that should be nontoxic, be able to penetrate into the desired target tissue or organ, and have a half-life of a few hours (as opposed to minutes or days) so that when withdrawn or added (depending on the regulatable system used) gene expression can be turned "on" or "off" quickly and effectively. Also, the genetic switches employed should ideally be nonimmunogenic in the host. The ability to switch transgenes on and off would be of paramount importance not only when the therapy is no longer needed, but also in the case of the development of adverse side effects to the therapy. Many regulatable systems are currently under development and some, i.e., the tetracycline-dependent transcriptional switch, have been used successfully for in vivo preclinical applications. Despite this, there are no examples of switches that have been employed in a human clinical trial. In this review, we aim to highlight the main regulatable systems currently under development, the gene transfer systems employed for their expression, and also the preclinical models in which they have been used successfully. We also discuss the substantial challenges that still remain before these regulatable switches can be employed in the clinical setting.

UR - http://www.scopus.com/inward/record.url?scp=22644442838&partnerID=8YFLogxK

U2 - 10.1016/j.ymthe.2005.03.022

DO - 10.1016/j.ymthe.2005.03.022

M3 - Review article

C2 - 15946903

AN - SCOPUS:22644442838

SN - 1525-0016

VL - 12

SP - 189

EP - 211

JO - Molecular Therapy

JF - Molecular Therapy

IS - 2

ER -

Regulatable gene expression systems for gene therapy applications: Progress and future challenges

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