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Dive into the research topics where Bennett C. Laguzza is active.

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Featured researches published by Bennett C. Laguzza.


Cancer Immunology, Immunotherapy | 1989

In vivo efficacy of monoclonal antibody-drug conjugates of three different subisotypes which bind the human tumor-associated antigen defined by the KS1/4 monoclonal antibody.

James J. Starling; Ronald S. Maciak; N. Ann Hinson; Cynthia L. Nichols; Stephen L. Briggs; Bennett C. Laguzza

SummaryA panel of three hybridomas has been isolated each of which secretes a single species of monoclonal antibody (MoAb) directed against the KS1/4 tumor-associated antigen originally described by Varki et al. (Cancer Res 44:681, 1984). These MoAbs were designated L1-(IgG2b), L2-(IgG1), and L4-(IgG2a) KS. Binding specificity, immunoprecipitation, and competitive binding analyses indicated that these MoAbs each recognize the same epitope of the KS1/4 antigen. The immunoprecipitation studies indicated that the MoAbs recognized a major antigenic component of 42 kDa and a minor component of 35 kDa. The L-KS antibodies were evaluated as MoAb-drug conjugates against a variety of human tumor targets grown in vivo as nude mouse xenografts. The MoAb-drug conjugates were constructed using protein-A-purified MoAbs conjugated to 4-desacetyl-vinblastine-3-carboxhydrazide. Efficacy was determined using various dosing protocols on 2–14 day established tumors of lung, pharynx, colon, and skin origin. Control experiments included the use of dual-flank antigen-positive and negative tumors, free MoAbs, free drug, and mixtures of MoAbs and drug. These studies indicated that significant tumor growth supression and actual tumor regression could be achieved by the MoAb — vinca conjugates and that this activity was antigen-mediated. The drug conjugates were more efficacious than free drug or free MoAbs administered either singly or in combination with each other.


Journal of Medicinal Chemistry | 1989

New antitumor monoclonal antibody-vinca conjugates LY203725 and related compounds: design, preparation, and representative in vivo activity.

Bennett C. Laguzza; Cynthia L. Nichols; Stephen L. Briggs; George Joseph Cullinan; David A. Johnson; James J. Starling; A. Leroy Baker; Thomas F. Bumol; Jose R. F. Corvalan


Archive | 1989

Cytotoxic drug conjugates

David A. Johnson; Bennett C. Laguzza; William Leonard Scott


Archive | 1988

Cytotoxic antibody conjugates of hydrazide derivatized methotrexate analogs via simple organic linkers

David A. Johnson; Bennett C. Laguzza; William Leonard Scott


Cancer Research | 1991

In Vivo Antitumor Activity of a Monoclonal Antibody-Vinca Alkaloid Immunoconjugate Directed against a Solid Tumor Membrane Antigen Characterized by Heterogeneous Expression and Noninternalization of Antibody-Antigen Complexes

James J. Starling; Ronald S. Maciak; Law Kl; Hinson Na; Stephen L. Briggs; Bennett C. Laguzza; David A. Johnson


Archive | 1987

Hydrazone immunoglobulin conjugates

Bennett C. Laguzza; Cynthia L. Nichols


Archive | 1991

Cytotoxic antibody conjugates of hydrazide derivatized vinca analogs via simple organic linkers

George Joseph Cullinan; Bennett C. Laguzza; William Leonard Scott


Cancer Research | 1987

Antitumor Xenograft Activity with a Conjugate of a Vinca Derivative and the Squamous Carcinoma-reactive Monoclonal Antibody PF1/D

David A. Johnson; Bennett C. Laguzza


Archive | 1988

Intermediates for antibody-vinca drug conjugates

George Joseph Cullinan; Bennett C. Laguzza; William Leonard Scott


Cancer Research | 1990

Antitumor Activity of L/1C2-4-Desacetylvinblastine-3-carboxhydrazide Immunoconjugate in Xenografts

David A. Johnson; A. Leroy Baker; Bennett C. Laguzza; Daniel V. Fix; Magda C. Gutowski

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