Author: Leverson, Joel D. ; Holms, James ; Henriques, Tracy A. ; Haasch, Deanna ; Judd, Andrew S. ; Jenkins, Gary J. ; Tao, Zhi-Fu ; Mitra, Diya ; Li, Yingchun ; Song, Xiaohong ; Haight, Anthony R. ; Kalvass, John C. ; Vaidya, Kedar S. ; Kunzer, Aaron ; Nelson, Lorne ; Peterson, Richard ; Izeradjene, Kamel ; Souers, Andrew J. ; Nimmer, Paul ; Phillips, Andrew ; Buck, Wayne R. ; Frey, Robin ; Shen, Xiaoqiang ; Bawa, Bhupinder ; Wang, Jin ; Phillips, Darren C. ; Zhang, Haichao ; Wang, Xilu ; Judge, Russell A. ; Ralston, Sherry L. ; Xiao, Yu ; Durbin, Kenneth R. ; Mitten, Michael J. ; Boghaert, Erwin R. ; Blomme, Eric A. ; Catron, Nathaniel ; Doherty, George ; Enright, Brian ; Martin, Ruth L. ; Bruncko, Milan ; Palma, Joann ; Mittelstadt, Scott ; Zhang, Xinxin ; Haman, Sandra ; Rosenberg, Saul H.

Overexpression of the antiapoptotic protein B-cell lymphoma-extra large (BCL-X L ) is associated with drug resistance and disease progression in numerous cancers. The compelling nature of this protein as a therapeutic target prompted efforts to develop selective small-molecule BCL-X L inhibitors. Although efficacious in preclinical models, we report herein that selective BCL-X L inhibitors cause severe mechanism-based cardiovascular toxicity in higher preclinical species. To overcome this liability, antibody-drug conjugates were constructed using altered BCL-X L –targeting warheads, unique linker technologies, and therapeutic antibodies. The epidermal growth factor receptor–targeting antibody-drug conjugate AM1-15 inhibited growth of tumor xenografts and did not cause cardiovascular toxicity nor dose-limiting thrombocytopenia in monkeys. While an unprecedented BCL-X L –mediated toxicity was uncovered in monkey kidneys upon repeat dosing of AM1-15, this toxicity was mitigated via further drug-linker modification to afford AM1-AAA (AM1-25). The AAA drug-linker has since been incorporated into mirzotamab clezutoclax, the first selective BCL-X L –targeting agent to enter human clinical trials.

01 Aug 2003·Antimicrobial agents and chemotherapyQ2 · MEDICINE

In Vitro Activities of Novel Oxapenems, Alone and in Combination with Ceftazidime, against Gram-Positive and Gram-Negative Organisms

Q2 · MEDICINE

Article

Author: Simpson, Iain N. ; Jamieson, Conor E. ; Lambert, Peter A.

ABSTRACT:

Four novel oxapenem compounds (i.e., AM-112, AM-113, AM-114, and AM-115) were investigated for their β-lactamase inhibitory activity against a panel of isolated class A, C, and D enzymes, which included expanded-spectrum β-lactamase enzymes (ESBLs). The oxapenems were potent β-lactamase inhibitors. Activity varied within the group, with AM-113 and AM-114 proving to be the most active compounds. The 50% inhibitory concentrations for these agents were up to 100,000-fold lower than that of clavulanic acid against class C and D enzymes. As a group, the oxapenems were more potent than clavulanic acid against enzymes from all classes. The ability of these compounds to protect ceftazidime from hydrolysis by β-lactamase-producing strains was evaluated by MIC tests that combined ceftazidime and each oxapenem in a 1:1 or 2:1 ratio. The oxapenems markedly reduced the MICs for ceftazidime against class C hyperproducing strains and strains producing TEM- and SHV-derived ESBLs. There was little difference between the activity of 1:1 and 2:1 combinations of ceftazidime and oxapenem. The oxapenems failed to enhance the activity of ceftazidime against derepressed AmpC-producing Pseudomonas aeruginosa strains.

01 Jan 2003·The Journal of antibioticsQ4 · MEDICINE

Synthesis and Biological Activity of AM-112 and Related Oxapenem Analogues

Q4 · MEDICINE

Article

Author: Birgit Sprinkart ; Hans R. Pfaendler ; Gudrun Hagen ; Iain N. Simpson ; Christopher J. Urch ; Ralf Albrecht

Thirty five oxapenem analogues substituted with a range of tertiary groups at C-2 have been synthesised and evaluated as broad-spectrum beta-lactamase inhibitors. All analogues enhanced the activity of ceftazidime against bacterial isolates producing Class A and Class C beta-lactamases. Compounds with cyclic substituents at C-1' (attached to C-6) were associated with enhanced antibacterial activity against Staphylococcus aureus. (R) Stereochemistry at C-1' led to synergistic activity against beta-lactamase negative enterococci. (S) Stereochemistry at C-1' was associated with enhanced inhibition of Class A beta-lactamases and lack of synergistic activity against enterococci. AM-113 was unstable in serum and not detectable following subcutaneous or oral dosing in mice. AM-112 and AM-115 achieved good serum levels following subcutaneous dosing. AM-114 exhibited 30% bioavailability following oral dosing. AM-112 [(1'R,5R,6R)-2-(4-ammonio-1,1-dimethylbutyl)-6-(1'-hydroxyethyl)oxapenem-3-carboxylate] achieved the greatest protection of ceftazidime against Gram-negatives producing Class A or C beta-lactamases.

100 Deals associated with AM-115

R&D Status

10 top R&D records.

to view more data

Indication	Highest Phase	Country/Location	Organization	Date
Gram-Negative Bacterial Infections	Preclinical	United Kingdom	University of Aston	10 May 2003
Gram-Positive Bacterial Infections	Preclinical	United Kingdom	University of Aston	10 May 2003

Clinical Result

Indication

Phase

Evaluation

View All Results

Translational Medicine

Boost your research with our translational medicine data.

view full example data

Deal

Boost your decision using our deal data.

view full example data

Core Patent

Boost your research with our Core Patent data.

view full example data

Clinical Trial

Identify the latest clinical trials across global registries.

view full example data

Approval

Accelerate your research with the latest regulatory approval information.

view full example data

Regulation

Understand key drug designations in just a few clicks with Synapse.

view full example data

AI Agents Built for Biopharma Breakthroughs

Accelerate discovery. Empower decisions. Transform outcomes.

Get started for free today!

Accelerate Strategic R&D decision making with Synapse, PatSnap’s AI-powered Connected Innovation Intelligence Platform Built for Life Sciences Professionals.

Start your data trial now!

Synapse data is also accessible to external entities via APIs or data packages. Empower better decisions with the latest in pharmaceutical intelligence.

Bio

Bio Sequences Search & Analysis

Chemical

Chemical Structures Search & Analysis


No Data