Phase I Clinical and Pharmacological Study of Suppression of Human Antimouse Antibody Response to Monoclonal Antibody L6 by Deoxyspergualin

Kapil Dhingra; Herbert Fritsche; James L. Murray; Albert F. LoBuglio; M. B. Khazaeli; Susan Kelley; Mark A. Tepper; Dennis Grasela; Aman Buzdar; Vicente Valero; Daniel Booser; Hannah Whealin; Tedd J. Collins; Janice M. Pursley; Gabriel Hortobagyi

Phase I Clinical and Pharmacological Study of Suppression of Human Antimouse Antibody Response to Monoclonal Antibody L6 by Deoxyspergualin

Kapil Dhingra, Herbert Fritsche, James L. Murray, Albert F. LoBuglio, M. B. Khazaeli, Susan Kelley, Mark A. Tepper, Dennis Grasela, Aman Buzdar, Vicente Valero, Daniel Booser, Hannah Whealin, Tedd J. Collins, Janice M. Pursley, Gabriel Hortobagyi

Breast Medical Oncology

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

24 Scopus citations

Abstract

Development of human antimouse antibody (HAMA) is a major limiting factor in the application of murine mAb for clinical use. A novel immunomodulatory drug, deoxyspergualin (DSG), has shown potential to suppress antimouse antibody response in preclinical model systems. We conducted a Phase I trial to determine the effect of DSG on HAMA response to murine mAb L6 administered to patients with advanced cancers (in previous trials, this antibody elicited HAMA in two-thirds of the treated patients). L6 mAb was administered at a fixed dose of 200 mg/m2 on days 1-5. DSG was administered at doses of 50 mg/m2 [dose level (dl) 1] or 150 mg/m2 (dis H and TO) on days 1-7. Treatment courses were repeated every 6 weeks (dls I and II) or every 3 weeks (dl HI). HAMAs were quantitated by a commercially available ELISA assay (ImmuSTRIP; anti-isotypk antibodies) and a radiometric assay (anti-isotypic and anti-idiotypic antibodies). Pharmacokinetics of L6 and DSG was also studied in all consenting patients. Among 24 evaluable patients, 2 patients developed detectable HAMAs using the ELISA (one each at dls I and II) after a median follow-up of 122 days (P = 0.0001 as compared to historical controls). Even in the two patients who developed HAMA, the HAMA levels were quite low (160 and 181 ng/ml; historical experience, 70-38,744 ng/ml). The radiometric assay detected anti-L6 antibodies in 13 patients (4, 6, and 3 at dls I-IH, respectively) after a median of 82 days. The median highest anti-L6 antibody level was 129 ng/ml (range, 21-2150). The highest anti-L6 antibody level at dl IH was only 44 ng/ml. The results suggest suppression of anti-idiotypic response also. No clinical antitumor activity was observed, and no significant changes in T4/T8 subsets or immunoglobulins occurred (suggesting a lack of generalized immunosuppression). We conclude that DSG can suppress HAMA response to L6. A starting dose of 150 mg/m2/day is recommended for Phase H trials to confirm this observation.

Original language	English (US)
Pages (from-to)	3060-3067
Number of pages	8
Journal	Cancer Research
Volume	55
Issue number	14
State	Published - Jul 15 1995

ASJC Scopus subject areas

Oncology
Cancer Research

Cite this

Dhingra, K., Fritsche, H., Murray, J. L., LoBuglio, A. F., Khazaeli, M. B., Kelley, S., Tepper, M. A., Grasela, D., Buzdar, A., Valero, V., Booser, D., Whealin, H., Collins, T. J., Pursley, J. M., & Hortobagyi, G. (1995). Phase I Clinical and Pharmacological Study of Suppression of Human Antimouse Antibody Response to Monoclonal Antibody L6 by Deoxyspergualin. Cancer Research, 55(14), 3060-3067.

Dhingra, K, Fritsche, H, Murray, JL, LoBuglio, AF, Khazaeli, MB, Kelley, S, Tepper, MA, Grasela, D, Buzdar, A , Valero, V , Booser, D, Whealin, H, Collins, TJ, Pursley, JM & Hortobagyi, G 1995, 'Phase I Clinical and Pharmacological Study of Suppression of Human Antimouse Antibody Response to Monoclonal Antibody L6 by Deoxyspergualin', Cancer Research, vol. 55, no. 14, pp. 3060-3067.

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title = "Phase I Clinical and Pharmacological Study of Suppression of Human Antimouse Antibody Response to Monoclonal Antibody L6 by Deoxyspergualin",

abstract = "Development of human antimouse antibody (HAMA) is a major limiting factor in the application of murine mAb for clinical use. A novel immunomodulatory drug, deoxyspergualin (DSG), has shown potential to suppress antimouse antibody response in preclinical model systems. We conducted a Phase I trial to determine the effect of DSG on HAMA response to murine mAb L6 administered to patients with advanced cancers (in previous trials, this antibody elicited HAMA in two-thirds of the treated patients). L6 mAb was administered at a fixed dose of 200 mg/m2 on days 1-5. DSG was administered at doses of 50 mg/m2 [dose level (dl) 1] or 150 mg/m2 (dis H and TO) on days 1-7. Treatment courses were repeated every 6 weeks (dls I and II) or every 3 weeks (dl HI). HAMAs were quantitated by a commercially available ELISA assay (ImmuSTRIP; anti-isotypk antibodies) and a radiometric assay (anti-isotypic and anti-idiotypic antibodies). Pharmacokinetics of L6 and DSG was also studied in all consenting patients. Among 24 evaluable patients, 2 patients developed detectable HAMAs using the ELISA (one each at dls I and II) after a median follow-up of 122 days (P = 0.0001 as compared to historical controls). Even in the two patients who developed HAMA, the HAMA levels were quite low (160 and 181 ng/ml; historical experience, 70-38,744 ng/ml). The radiometric assay detected anti-L6 antibodies in 13 patients (4, 6, and 3 at dls I-IH, respectively) after a median of 82 days. The median highest anti-L6 antibody level was 129 ng/ml (range, 21-2150). The highest anti-L6 antibody level at dl IH was only 44 ng/ml. The results suggest suppression of anti-idiotypic response also. No clinical antitumor activity was observed, and no significant changes in T4/T8 subsets or immunoglobulins occurred (suggesting a lack of generalized immunosuppression). We conclude that DSG can suppress HAMA response to L6. A starting dose of 150 mg/m2/day is recommended for Phase H trials to confirm this observation.",

author = "Kapil Dhingra and Herbert Fritsche and Murray, {James L.} and LoBuglio, {Albert F.} and Khazaeli, {M. B.} and Susan Kelley and Tepper, {Mark A.} and Dennis Grasela and Aman Buzdar and Vicente Valero and Daniel Booser and Hannah Whealin and Collins, {Tedd J.} and Pursley, {Janice M.} and Gabriel Hortobagyi",

year = "1995",

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language = "English (US)",

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pages = "3060--3067",

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T1 - Phase I Clinical and Pharmacological Study of Suppression of Human Antimouse Antibody Response to Monoclonal Antibody L6 by Deoxyspergualin

AU - Dhingra, Kapil

AU - Fritsche, Herbert

AU - Murray, James L.

AU - LoBuglio, Albert F.

AU - Khazaeli, M. B.

AU - Kelley, Susan

AU - Tepper, Mark A.

AU - Grasela, Dennis

AU - Buzdar, Aman

AU - Valero, Vicente

AU - Booser, Daniel

AU - Whealin, Hannah

AU - Collins, Tedd J.

AU - Pursley, Janice M.

AU - Hortobagyi, Gabriel

PY - 1995/7/15

Y1 - 1995/7/15

N2 - Development of human antimouse antibody (HAMA) is a major limiting factor in the application of murine mAb for clinical use. A novel immunomodulatory drug, deoxyspergualin (DSG), has shown potential to suppress antimouse antibody response in preclinical model systems. We conducted a Phase I trial to determine the effect of DSG on HAMA response to murine mAb L6 administered to patients with advanced cancers (in previous trials, this antibody elicited HAMA in two-thirds of the treated patients). L6 mAb was administered at a fixed dose of 200 mg/m2 on days 1-5. DSG was administered at doses of 50 mg/m2 [dose level (dl) 1] or 150 mg/m2 (dis H and TO) on days 1-7. Treatment courses were repeated every 6 weeks (dls I and II) or every 3 weeks (dl HI). HAMAs were quantitated by a commercially available ELISA assay (ImmuSTRIP; anti-isotypk antibodies) and a radiometric assay (anti-isotypic and anti-idiotypic antibodies). Pharmacokinetics of L6 and DSG was also studied in all consenting patients. Among 24 evaluable patients, 2 patients developed detectable HAMAs using the ELISA (one each at dls I and II) after a median follow-up of 122 days (P = 0.0001 as compared to historical controls). Even in the two patients who developed HAMA, the HAMA levels were quite low (160 and 181 ng/ml; historical experience, 70-38,744 ng/ml). The radiometric assay detected anti-L6 antibodies in 13 patients (4, 6, and 3 at dls I-IH, respectively) after a median of 82 days. The median highest anti-L6 antibody level was 129 ng/ml (range, 21-2150). The highest anti-L6 antibody level at dl IH was only 44 ng/ml. The results suggest suppression of anti-idiotypic response also. No clinical antitumor activity was observed, and no significant changes in T4/T8 subsets or immunoglobulins occurred (suggesting a lack of generalized immunosuppression). We conclude that DSG can suppress HAMA response to L6. A starting dose of 150 mg/m2/day is recommended for Phase H trials to confirm this observation.

AB - Development of human antimouse antibody (HAMA) is a major limiting factor in the application of murine mAb for clinical use. A novel immunomodulatory drug, deoxyspergualin (DSG), has shown potential to suppress antimouse antibody response in preclinical model systems. We conducted a Phase I trial to determine the effect of DSG on HAMA response to murine mAb L6 administered to patients with advanced cancers (in previous trials, this antibody elicited HAMA in two-thirds of the treated patients). L6 mAb was administered at a fixed dose of 200 mg/m2 on days 1-5. DSG was administered at doses of 50 mg/m2 [dose level (dl) 1] or 150 mg/m2 (dis H and TO) on days 1-7. Treatment courses were repeated every 6 weeks (dls I and II) or every 3 weeks (dl HI). HAMAs were quantitated by a commercially available ELISA assay (ImmuSTRIP; anti-isotypk antibodies) and a radiometric assay (anti-isotypic and anti-idiotypic antibodies). Pharmacokinetics of L6 and DSG was also studied in all consenting patients. Among 24 evaluable patients, 2 patients developed detectable HAMAs using the ELISA (one each at dls I and II) after a median follow-up of 122 days (P = 0.0001 as compared to historical controls). Even in the two patients who developed HAMA, the HAMA levels were quite low (160 and 181 ng/ml; historical experience, 70-38,744 ng/ml). The radiometric assay detected anti-L6 antibodies in 13 patients (4, 6, and 3 at dls I-IH, respectively) after a median of 82 days. The median highest anti-L6 antibody level was 129 ng/ml (range, 21-2150). The highest anti-L6 antibody level at dl IH was only 44 ng/ml. The results suggest suppression of anti-idiotypic response also. No clinical antitumor activity was observed, and no significant changes in T4/T8 subsets or immunoglobulins occurred (suggesting a lack of generalized immunosuppression). We conclude that DSG can suppress HAMA response to L6. A starting dose of 150 mg/m2/day is recommended for Phase H trials to confirm this observation.

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Phase I Clinical and Pharmacological Study of Suppression of Human Antimouse Antibody Response to Monoclonal Antibody L6 by Deoxyspergualin

Abstract

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