Clinical and biological effects of an agonist anti-CD40 antibody: a cancer research UK phase I study

Peter Johnson; Ruth Challis; Ferdousi Chowdhury; Yifang Gao; Melanie Harvey; Tom Geldart; Paul Kerr; Claude Chan; Anna Smith; Neil Steven; Ceri Edwards; Margaret Ashton-Key; Elisabeth Hodges; Alison Tutt; Christian Ottensmeier; Martin Glennie; Anthony Williams

doi:10.1158/1078-0432.CCR-14-2355

Clinical and biological effects of an agonist anti-CD40 antibody: a cancer research UK phase I study

Peter Johnson^*, Ruth Challis, Ferdousi Chowdhury, Yifang Gao, Melanie Harvey, Tom Geldart, Paul Kerr, Claude Chan, Anna Smith, Neil Steven, Ceri Edwards, Margaret Ashton-Key, Elisabeth Hodges, Alison Tutt, Christian Ottensmeier, Martin Glennie, Anthony Williams

^*Corresponding author for this work

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

43 Citations (Scopus)

Abstract

Purpose: This phase I study aimed to establish the biologic effects and MTD of the agonistic IgG1 chimeric anti-CD40 antibody ChiLob7/4 in patients (pts) with a range of CD40-expressing solid tumors and diffuse large B-cell lymphoma, resistant to conventional therapy. Potential mechanisms of action for agonistic anti-CD40 include direct cytotoxic effects on tumor cells and conditioning of antigen-presenting cells. Experimental Design: ChiLob7/4 was given by IV infusion weekly for 4 doses at a range from 0.5 to 240 mg/dose. Validated ELISAs were used to quantify ChiLob7/4 in serum and test for anti-chimeric MAb (HACA) responses. Pharmacodynamic assessments included quantitation of T-cell, natural killer-cell, and B-cell numbers and activation in blood by flow cytometry and a panel of cytokines in plasma by Luminex technology. Planned dose escalation was in cohorts of 3 patients until MTD or biologic effect, de fi ned as reduction of peripheral blood CD19⁺ B cells to 10% or less of baseline. Results: Twenty-nine courses of treatment were given to 28 subjects. The MTD was 200 mg x 4, with dose-limiting toxicity of liver transaminase elevations at 240 mg. At 200 mg (range between 2.1 mg/kg and 3.3 mg/kg based on patient body weight), the trough level pretreatment was above 25 μg/mL. Grade 1-2 infusion reactions were seen above the dose of 16 mg, but could be prevented with single-dose corticosteroid premedication. HACA responses were seen after doses between 1.6 mg and 50 mg, but not above this. There were dose-dependent falls in blood B-cell numbers accompanied by reduced expression of CD21, and transient reductions in NK cell numbers with increased CD54 expression from 50 mg upward. MIP-1β and IL12 plasma concentrations rose after doses above 16 mg. Fifteen of 29 treatments were accompanied by disease stabilization for a median 6 months, the longest for 37 months. Conclusions: ChiLob7/4 can activate B and NK cells at doses that can be administered safely, and should be tested in combination with other antibodies and chemotherapy agents.

Original language	English
Pages (from-to)	1321-1328
Number of pages	8
Journal	Clinical Cancer Research
Volume	21
Issue number	6
Early online date	14 Jan 2015
DOIs	https://doi.org/10.1158/1078-0432.CCR-14-2355
Publication status	Published - 15 Mar 2015

ASJC Scopus subject areas

Cancer Research
Oncology

UN SDGs

This output contributes to the following UN Sustainable Development Goals (SDGs)

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10.1158/1078-0432.CCR-14-2355

Cite this

Johnson, P., Challis, R., Chowdhury, F., Gao, Y., Harvey, M., Geldart, T., Kerr, P., Chan, C., Smith, A., Steven, N., Edwards, C., Ashton-Key, M., Hodges, E., Tutt, A., Ottensmeier, C., Glennie, M., & Williams, A. (2015). Clinical and biological effects of an agonist anti-CD40 antibody: a cancer research UK phase I study. Clinical Cancer Research, 21(6), 1321-1328. https://doi.org/10.1158/1078-0432.CCR-14-2355

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title = "Clinical and biological effects of an agonist anti-CD40 antibody: a cancer research UK phase I study",

abstract = "Purpose: This phase I study aimed to establish the biologic effects and MTD of the agonistic IgG1 chimeric anti-CD40 antibody ChiLob7/4 in patients (pts) with a range of CD40-expressing solid tumors and diffuse large B-cell lymphoma, resistant to conventional therapy. Potential mechanisms of action for agonistic anti-CD40 include direct cytotoxic effects on tumor cells and conditioning of antigen-presenting cells. Experimental Design: ChiLob7/4 was given by IV infusion weekly for 4 doses at a range from 0.5 to 240 mg/dose. Validated ELISAs were used to quantify ChiLob7/4 in serum and test for anti-chimeric MAb (HACA) responses. Pharmacodynamic assessments included quantitation of T-cell, natural killer-cell, and B-cell numbers and activation in blood by flow cytometry and a panel of cytokines in plasma by Luminex technology. Planned dose escalation was in cohorts of 3 patients until MTD or biologic effect, de fi ned as reduction of peripheral blood CD19+ B cells to 10% or less of baseline. Results: Twenty-nine courses of treatment were given to 28 subjects. The MTD was 200 mg x 4, with dose-limiting toxicity of liver transaminase elevations at 240 mg. At 200 mg (range between 2.1 mg/kg and 3.3 mg/kg based on patient body weight), the trough level pretreatment was above 25 μg/mL. Grade 1-2 infusion reactions were seen above the dose of 16 mg, but could be prevented with single-dose corticosteroid premedication. HACA responses were seen after doses between 1.6 mg and 50 mg, but not above this. There were dose-dependent falls in blood B-cell numbers accompanied by reduced expression of CD21, and transient reductions in NK cell numbers with increased CD54 expression from 50 mg upward. MIP-1β and IL12 plasma concentrations rose after doses above 16 mg. Fifteen of 29 treatments were accompanied by disease stabilization for a median 6 months, the longest for 37 months. Conclusions: ChiLob7/4 can activate B and NK cells at doses that can be administered safely, and should be tested in combination with other antibodies and chemotherapy agents.",

author = "Peter Johnson and Ruth Challis and Ferdousi Chowdhury and Yifang Gao and Melanie Harvey and Tom Geldart and Paul Kerr and Claude Chan and Anna Smith and Neil Steven and Ceri Edwards and Margaret Ashton-Key and Elisabeth Hodges and Alison Tutt and Christian Ottensmeier and Martin Glennie and Anthony Williams",

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Johnson, P, Challis, R, Chowdhury, F, Gao, Y, Harvey, M, Geldart, T, Kerr, P, Chan, C, Smith, A, Steven, N, Edwards, C, Ashton-Key, M, Hodges, E, Tutt, A, Ottensmeier, C, Glennie, M & Williams, A 2015, 'Clinical and biological effects of an agonist anti-CD40 antibody: a cancer research UK phase I study', Clinical Cancer Research, vol. 21, no. 6, pp. 1321-1328. https://doi.org/10.1158/1078-0432.CCR-14-2355

TY - JOUR

T1 - Clinical and biological effects of an agonist anti-CD40 antibody: a cancer research UK phase I study

AU - Johnson, Peter

AU - Challis, Ruth

AU - Chowdhury, Ferdousi

AU - Gao, Yifang

AU - Harvey, Melanie

AU - Geldart, Tom

AU - Kerr, Paul

AU - Chan, Claude

AU - Smith, Anna

AU - Steven, Neil

AU - Edwards, Ceri

AU - Ashton-Key, Margaret

AU - Hodges, Elisabeth

AU - Tutt, Alison

AU - Ottensmeier, Christian

AU - Glennie, Martin

AU - Williams, Anthony

PY - 2015/3/15

Y1 - 2015/3/15

N2 - Purpose: This phase I study aimed to establish the biologic effects and MTD of the agonistic IgG1 chimeric anti-CD40 antibody ChiLob7/4 in patients (pts) with a range of CD40-expressing solid tumors and diffuse large B-cell lymphoma, resistant to conventional therapy. Potential mechanisms of action for agonistic anti-CD40 include direct cytotoxic effects on tumor cells and conditioning of antigen-presenting cells. Experimental Design: ChiLob7/4 was given by IV infusion weekly for 4 doses at a range from 0.5 to 240 mg/dose. Validated ELISAs were used to quantify ChiLob7/4 in serum and test for anti-chimeric MAb (HACA) responses. Pharmacodynamic assessments included quantitation of T-cell, natural killer-cell, and B-cell numbers and activation in blood by flow cytometry and a panel of cytokines in plasma by Luminex technology. Planned dose escalation was in cohorts of 3 patients until MTD or biologic effect, de fi ned as reduction of peripheral blood CD19+ B cells to 10% or less of baseline. Results: Twenty-nine courses of treatment were given to 28 subjects. The MTD was 200 mg x 4, with dose-limiting toxicity of liver transaminase elevations at 240 mg. At 200 mg (range between 2.1 mg/kg and 3.3 mg/kg based on patient body weight), the trough level pretreatment was above 25 μg/mL. Grade 1-2 infusion reactions were seen above the dose of 16 mg, but could be prevented with single-dose corticosteroid premedication. HACA responses were seen after doses between 1.6 mg and 50 mg, but not above this. There were dose-dependent falls in blood B-cell numbers accompanied by reduced expression of CD21, and transient reductions in NK cell numbers with increased CD54 expression from 50 mg upward. MIP-1β and IL12 plasma concentrations rose after doses above 16 mg. Fifteen of 29 treatments were accompanied by disease stabilization for a median 6 months, the longest for 37 months. Conclusions: ChiLob7/4 can activate B and NK cells at doses that can be administered safely, and should be tested in combination with other antibodies and chemotherapy agents.

AB - Purpose: This phase I study aimed to establish the biologic effects and MTD of the agonistic IgG1 chimeric anti-CD40 antibody ChiLob7/4 in patients (pts) with a range of CD40-expressing solid tumors and diffuse large B-cell lymphoma, resistant to conventional therapy. Potential mechanisms of action for agonistic anti-CD40 include direct cytotoxic effects on tumor cells and conditioning of antigen-presenting cells. Experimental Design: ChiLob7/4 was given by IV infusion weekly for 4 doses at a range from 0.5 to 240 mg/dose. Validated ELISAs were used to quantify ChiLob7/4 in serum and test for anti-chimeric MAb (HACA) responses. Pharmacodynamic assessments included quantitation of T-cell, natural killer-cell, and B-cell numbers and activation in blood by flow cytometry and a panel of cytokines in plasma by Luminex technology. Planned dose escalation was in cohorts of 3 patients until MTD or biologic effect, de fi ned as reduction of peripheral blood CD19+ B cells to 10% or less of baseline. Results: Twenty-nine courses of treatment were given to 28 subjects. The MTD was 200 mg x 4, with dose-limiting toxicity of liver transaminase elevations at 240 mg. At 200 mg (range between 2.1 mg/kg and 3.3 mg/kg based on patient body weight), the trough level pretreatment was above 25 μg/mL. Grade 1-2 infusion reactions were seen above the dose of 16 mg, but could be prevented with single-dose corticosteroid premedication. HACA responses were seen after doses between 1.6 mg and 50 mg, but not above this. There were dose-dependent falls in blood B-cell numbers accompanied by reduced expression of CD21, and transient reductions in NK cell numbers with increased CD54 expression from 50 mg upward. MIP-1β and IL12 plasma concentrations rose after doses above 16 mg. Fifteen of 29 treatments were accompanied by disease stabilization for a median 6 months, the longest for 37 months. Conclusions: ChiLob7/4 can activate B and NK cells at doses that can be administered safely, and should be tested in combination with other antibodies and chemotherapy agents.

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U2 - 10.1158/1078-0432.CCR-14-2355

DO - 10.1158/1078-0432.CCR-14-2355

M3 - Article

AN - SCOPUS:84927615313

SN - 1078-0432

VL - 21

SP - 1321

EP - 1328

JO - Clinical Cancer Research

JF - Clinical Cancer Research

IS - 6

ER -

Clinical and biological effects of an agonist anti-CD40 antibody: a cancer research UK phase I study

Abstract

ASJC Scopus subject areas

UN SDGs

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