A First-Time-In-Human Phase I Clinical Trial of Bispecific Antibody-Targeted, Paclitaxel-Packaged Bacterial Minicells | Zendy

Benjamin Solomon | Zendy; Jayesh Desai | Zendy; Mark Rosenthal | Zendy; Grant A. McArthur | Zendy; Scott Pattison | Zendy; Stacey L. Pattison | Zendy; Jennifer A. MacDiarmid | Zendy; Himanshu Brahmbhatt | Zendy; Andrew M. Scott | Zendy

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A First-Time-In-Human Phase I Clinical Trial of Bispecific Antibody-Targeted, Paclitaxel-Packaged Bacterial Minicells

Author(s) -

Benjamin Solomon,

Jayesh Desai,

Mark Rosenthal,

Grant A. McArthur,

Scott Pattison,

Stacey L. Pattison,

Jennifer A. MacDiarmid,

Himanshu Brahmbhatt,

Andrew M. Scott

Publication year - 2015

Publication title -

plos one

Language(s) - English

Resource type - Journals

SCImago Journal Rank - 0.99

H-Index - 332

ISSN - 1932-6203

DOI - 10.1371/journal.pone.0144559

Subject(s) - medicine , adverse effect , tolerability , dosing , antibody , immune system , cancer , pharmacology , clinical trial , immunology , gastroenterology , oncology

Background We have harnessed a novel biological system, the bacterial minicell, to deliver cancer therapeutics to cancer cells. Preclinical studies showed that epidermal growth factor receptor (EGFR)-targeted, paclitaxel-loaded minicells ( EGFR minicells Pac ) have antitumor effects in xenograft models. To examine the safety of the minicell delivery system, we initiated a first-time-in-human, open-label, phase I clinical study of EGFR minicells Pac in patients with advanced solid tumors. Methodology Patients received 5 weekly infusions followed by a treatment free week. Seven dose levels (1x10 8 , 1x10 9 , 3x10 9 , 1x10 10 , 1.5x10 10 , 2x10 10 , 5x10 10 ) were evaluated using a 3+3 dose-escalation design. Primary objectives were safety, tolerability and determination of the maximum tolerated dose. Secondary objectives were assessment of immune/inflammatory responses and antitumor activity. Principal Findings Twenty eight patients were enrolled, 22 patients completed at least one cycle of EGFR minicells Pac ; 6 patients did not complete a cycle due to rapidly progressive disease. A total of 236 doses was delivered over 42 cycles, with a maximum of 45 doses administered to a single patient. Most common treatment-related adverse events were rigors and pyrexia. No deaths resulted from treatment-related adverse events and the maximum tolerated dose was defined as 1x10 10 EGFR minicells Pac . Surprisingly, only a mild self-limiting elevation in the inflammatory cytokines IL-6, IL-8 and TNFα and anti-inflammatory IL-10 was observed. Anti-LPS antibody titers peaked by dose 3 and were maintained at that level despite repeat dosing with the bacterially derived minicells. Ten patients (45%; n = 22) achieved stable disease as their best response. Conclusions/Significance This is the first study in humans of a novel biological system that can provide targeted delivery of a range of chemotherapeutic drugs to solid tumor cells. Bispecific antibody-targeted minicells, packaged with the chemotherapeutic paclitaxel, were shown to be safe in patients with advanced solid tumors with modest clinical efficacy observed. Further study in Phase II trials is planned. Trial Registration Australian New Zealand Clinical Trials Registry ACTRN12609000672257

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