Gene therapy for non-small cell lung cancer: A preliminary report of a phase I trial of adenoviral p53 gene replacement

J. A. Roth; S. G. Swisher; J. A. Merritt; D. D. Lawrence; B. L. Kemp; C. H. Carrasco; A. K. El-Naggar; F. V. Fossella; B. S. Glisson; W. K. Hong; F. R. Khurl; J. M. Kurie; J. C. Nesbitt; K. Pisters; J. B. Putnam; D. S. Schrump; D. M. Shin; G. L. Walsh

Gene therapy for non-small cell lung cancer: A preliminary report of a phase I trial of adenoviral p53 gene replacement

J. A. Roth, S. G. Swisher, J. A. Merritt, D. D. Lawrence, B. L. Kemp, C. H. Carrasco, A. K. El-Naggar, F. V. Fossella, B. S. Glisson, W. K. Hong, F. R. Khurl, J. M. Kurie, J. C. Nesbitt, K. Pisters, J. B. Putnam, D. S. Schrump, D. M. Shin, G. L. Walsh

Research output: Contribution to journal › Review article › peer-review

118 Scopus citations

Abstract

The identification of genetic lesions that lead a normal cell to become malignant presents us with the opportunity of targeting those lesions as a means of therapy. Given the key role played by the tumor suppressor gene p53 in cell cycle regulation and apoptosis, and the evidence linking p53 mutations with non-small cell lung cancer, attempts at p53 replacement are a logical approach to therapy in this disease. In a phase I study, administration of an adenoviral p53 vector (Adp53) to 21 patients with advanced non-small cell lung cancer produced little toxicity. Up to six intratumoral injections at monthly intervals were well-tolerated. Expression of the p53 transgene was evident, along with potentially useful clinical responses. Time to disease progression in the indicator lesion treated with Adp53 appears to be enhanced by higher doses of vector, concomitant cisplatin therapy, and evidence of apoptosis on tumor biopsy specimens. Phase II trials should now be undertaken to determine the response rate to Adp53.

Original language	English (US)
Pages (from-to)	33-37
Number of pages	5
Journal	Seminars in oncology
Volume	25
Issue number	3 SUPPL. 8
State	Published - 1998

ASJC Scopus subject areas

Hematology
Oncology

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Roth, J. A., Swisher, S. G., Merritt, J. A., Lawrence, D. D., Kemp, B. L., Carrasco, C. H., El-Naggar, A. K., Fossella, F. V., Glisson, B. S., Hong, W. K., Khurl, F. R., Kurie, J. M., Nesbitt, J. C., Pisters, K., Putnam, J. B., Schrump, D. S., Shin, D. M., & Walsh, G. L. (1998). Gene therapy for non-small cell lung cancer: A preliminary report of a phase I trial of adenoviral p53 gene replacement. Seminars in oncology, 25(3 SUPPL. 8), 33-37.

Roth, JA, Swisher, SG, Merritt, JA, Lawrence, DD, Kemp, BL, Carrasco, CH, El-Naggar, AK , Fossella, FV, Glisson, BS, Hong, WK, Khurl, FR, Kurie, JM, Nesbitt, JC, Pisters, K, Putnam, JB, Schrump, DS, Shin, DM & Walsh, GL 1998, 'Gene therapy for non-small cell lung cancer: A preliminary report of a phase I trial of adenoviral p53 gene replacement', Seminars in oncology, vol. 25, no. 3 SUPPL. 8, pp. 33-37.

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title = "Gene therapy for non-small cell lung cancer: A preliminary report of a phase I trial of adenoviral p53 gene replacement",

abstract = "The identification of genetic lesions that lead a normal cell to become malignant presents us with the opportunity of targeting those lesions as a means of therapy. Given the key role played by the tumor suppressor gene p53 in cell cycle regulation and apoptosis, and the evidence linking p53 mutations with non-small cell lung cancer, attempts at p53 replacement are a logical approach to therapy in this disease. In a phase I study, administration of an adenoviral p53 vector (Adp53) to 21 patients with advanced non-small cell lung cancer produced little toxicity. Up to six intratumoral injections at monthly intervals were well-tolerated. Expression of the p53 transgene was evident, along with potentially useful clinical responses. Time to disease progression in the indicator lesion treated with Adp53 appears to be enhanced by higher doses of vector, concomitant cisplatin therapy, and evidence of apoptosis on tumor biopsy specimens. Phase II trials should now be undertaken to determine the response rate to Adp53.",

author = "Roth, {J. A.} and Swisher, {S. G.} and Merritt, {J. A.} and Lawrence, {D. D.} and Kemp, {B. L.} and Carrasco, {C. H.} and El-Naggar, {A. K.} and Fossella, {F. V.} and Glisson, {B. S.} and Hong, {W. K.} and Khurl, {F. R.} and Kurie, {J. M.} and Nesbitt, {J. C.} and K. Pisters and Putnam, {J. B.} and Schrump, {D. S.} and Shin, {D. M.} and Walsh, {G. L.}",

year = "1998",

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AU - Roth, J. A.

AU - Swisher, S. G.

AU - Merritt, J. A.

AU - Lawrence, D. D.

AU - Kemp, B. L.

AU - Carrasco, C. H.

AU - El-Naggar, A. K.

AU - Fossella, F. V.

AU - Glisson, B. S.

AU - Hong, W. K.

AU - Khurl, F. R.

AU - Kurie, J. M.

AU - Nesbitt, J. C.

AU - Pisters, K.

AU - Putnam, J. B.

AU - Schrump, D. S.

AU - Shin, D. M.

AU - Walsh, G. L.

PY - 1998

Y1 - 1998

N2 - The identification of genetic lesions that lead a normal cell to become malignant presents us with the opportunity of targeting those lesions as a means of therapy. Given the key role played by the tumor suppressor gene p53 in cell cycle regulation and apoptosis, and the evidence linking p53 mutations with non-small cell lung cancer, attempts at p53 replacement are a logical approach to therapy in this disease. In a phase I study, administration of an adenoviral p53 vector (Adp53) to 21 patients with advanced non-small cell lung cancer produced little toxicity. Up to six intratumoral injections at monthly intervals were well-tolerated. Expression of the p53 transgene was evident, along with potentially useful clinical responses. Time to disease progression in the indicator lesion treated with Adp53 appears to be enhanced by higher doses of vector, concomitant cisplatin therapy, and evidence of apoptosis on tumor biopsy specimens. Phase II trials should now be undertaken to determine the response rate to Adp53.

AB - The identification of genetic lesions that lead a normal cell to become malignant presents us with the opportunity of targeting those lesions as a means of therapy. Given the key role played by the tumor suppressor gene p53 in cell cycle regulation and apoptosis, and the evidence linking p53 mutations with non-small cell lung cancer, attempts at p53 replacement are a logical approach to therapy in this disease. In a phase I study, administration of an adenoviral p53 vector (Adp53) to 21 patients with advanced non-small cell lung cancer produced little toxicity. Up to six intratumoral injections at monthly intervals were well-tolerated. Expression of the p53 transgene was evident, along with potentially useful clinical responses. Time to disease progression in the indicator lesion treated with Adp53 appears to be enhanced by higher doses of vector, concomitant cisplatin therapy, and evidence of apoptosis on tumor biopsy specimens. Phase II trials should now be undertaken to determine the response rate to Adp53.

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ER -

Gene therapy for non-small cell lung cancer: A preliminary report of a phase I trial of adenoviral p53 gene replacement

Abstract

ASJC Scopus subject areas

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