ABSTRACT
The matrix metalloprotease ADAMTS7 has been identified by multiple genome-wide association studies as being involved in the development of coronary artery disease. Subsequent research revealed the proteolytic function of the enzyme to be relevant for atherogenesis and restenosis after vessel injury. Based on a publicly known dual ADAMTS4/ADAMTS5 inhibitor, we have in silico designed an ADAMTS7 inhibitor of the catalytic domain, which served as a starting point for an optimization campaign. Initially our inhibitors suffered from low selectivity vs MMP12. An X-ray cocrystal structure inspired us to exploit amino acid differences in the binding site of MMP12 and ADAMTS7 to improve selectivity. Further optimization composed of employing 5-membered heteroaromatic groups as hydantoin substituents to become more potent on ADAMTS7. Finally, fine-tuning of DMPK properties yielded BAY-9835, the first orally bioavailable ADAMTS7 inhibitor. Further optimization to improve selectivity vs ADAMTS12 seems possible, and a respective starting point could be identified.
Subject(s)
Atherosclerosis , Coronary Artery Disease , Humans , ADAMTS7 Protein/genetics , ADAMTS7 Protein/metabolism , Genome-Wide Association Study , Matrix Metalloproteinase 12ABSTRACT
The efficacy of BAY 57-1293, a novel non-nucleosidic inhibitor of herpes simplex virus 1 and 2 (HSV-1 and HSV-2), bovine herpesvirus and pseudorabies virus, was studied in the guinea pig model of genital herpes in comparison with the licensed drug valaciclovir (Valtrex). Early therapy with BAY 57-1293 almost completely suppressed the symptoms of acute HSV-2 infection, and reduced virus shedding and viral load in the sacral dorsal root ganglia by up to three orders of magnitude, resulting in decreased latency and a greatly diminished frequency of subsequent recurrent episodes. In contrast, valaciclovir showed only moderate effects in this set of experiments. When treatment was initiated late during the course of disease after symptoms were apparent, that is, a setting closer to most clinical situations, the efficacy of therapy with BAY 57-1293 was even more pronounced. Compared with valaciclovir, BAY 57-1293 halved the time necessary for complete healing. Moreover, the onset of action was fast, so that only very few animals developed new lesions after treatment commenced. Finally, in a study addressing the treatment of recurrent disease in animals whose primary infection had remained untreated BAY 57-1293 was efficient in suppressing the episodes. In summary, superior potency and efficacy of BAY 57-1293 over standard treatment with valaciclovir was demonstrated in relevant animal models of human genital herpes disease in terms of abrogating an HSV infection, reducing latency and the frequency of subsequent recurrences. Furthermore, BAY 57-1293 shortens the time to healing even if initiation of therapy is delayed.
Subject(s)
Antiviral Agents/pharmacology , DNA Helicases/antagonists & inhibitors , DNA Primase/antagonists & inhibitors , Disease Models, Animal , Enzyme Inhibitors/pharmacology , Herpes Genitalis/drug therapy , Pyridines/pharmacology , Thiazoles/pharmacology , Animals , Antiviral Agents/therapeutic use , DNA, Viral/genetics , Enzyme Inhibitors/therapeutic use , Guinea Pigs , Herpesvirus 2, Human/genetics , Humans , Polymerase Chain Reaction , Pyridines/therapeutic use , Sulfonamides , Thiazoles/therapeutic useABSTRACT
Here we show that a new class of antibiotics-acyldepsipeptides-has antibacterial activity against Gram-positive bacteria in vitro and in several rodent models of bacterial infection. The acyldepsipeptides are active against isolates that are resistant to antibiotics in clinical application, implying a new target, which we identify as ClpP, the core unit of a major bacterial protease complex. ClpP is usually tightly regulated and strictly requires a member of the family of Clp-ATPases and often further accessory proteins for proteolytic activation. Binding of acyldepsipeptides to ClpP eliminates these safeguards. The acyldepsipeptide-activated ClpP core is capable of proteolytic degradation in the absence of the regulatory Clp-ATPases. Such uncontrolled proteolysis leads to inhibition of bacterial cell division and eventually cell death.
Subject(s)
Anti-Bacterial Agents/classification , Anti-Bacterial Agents/pharmacology , Bacteria/drug effects , Bacteria/metabolism , Depsipeptides/pharmacology , Endopeptidase Clp/metabolism , Escherichia coli Proteins/metabolism , Animals , Anti-Bacterial Agents/pharmacokinetics , Anti-Bacterial Agents/toxicity , Bacillus subtilis/drug effects , Bacteria/enzymology , Depsipeptides/metabolism , Depsipeptides/pharmacokinetics , Depsipeptides/toxicity , Drug Resistance, Multiple, Bacterial , Escherichia coli/drug effects , Female , Mice , Molecular Structure , Mutation , Pneumococcal Infections/drug therapy , Pneumococcal Infections/microbiology , Protein Binding , Protein Processing, Post-Translational , Rats , Rats, Wistar , Sepsis/drug therapy , Sepsis/microbiologyABSTRACT
Specific interference with molecular mechanisms guiding tissue localization of leukocytes may be of great utility for selective immunosuppressive therapies. We have discovered and characterized efomycines, a new family of selective small-molecule inhibitors of selectin functions. Members of this family significantly inhibited leukocyte adhesion in vitro. Efomycine M, which was nontoxic and showed the most selective inhibitory effects on selectin-mediated leukocyte-endothelial adhesion in vitro, significantly diminished rolling in mouse ear venules in vivo as seen by intravital microscopy. In addition, efomycine M alleviated cutaneous inflammation in two complementary mouse models of psoriasis, one of the most common chronic inflammatory skin disorders. Molecular modeling demonstrated a spatial conformation of efomycines mimicking naturally occurring selectin ligands. Efomycine M might be efficacious in the treatment of human inflammatory disorders through a similar mechanism.
Subject(s)
Anti-Inflammatory Agents, Non-Steroidal/pharmacology , E-Selectin/drug effects , Leukocytes/drug effects , Macrolides/pharmacology , Psoriasis/drug therapy , Animals , Anti-Inflammatory Agents, Non-Steroidal/chemistry , Cell Adhesion/drug effects , Cell Movement/drug effects , Female , Humans , In Vitro Techniques , Macrolides/chemistry , Mice , Mice, Inbred C57BL , Mice, SCID , Models, Molecular , Oligosaccharides/chemistry , Psoriasis/pathology , Sialyl Lewis X Antigen , Skin Transplantation , Streptomyces/chemistry , Transplantation, HeterologousABSTRACT
The vast majority of the world population is infected with at least one member of the human herpesvirus family. Herpes simplex virus (HSV) infections are the cause of cold sores and genital herpes as well as life-threatening or sight-impairing disease mainly in immunocompromized patients, pregnant women and newborns. Since the milestone development in the late 1970s of acyclovir (Zovirax), a nucleosidic inhibitor of the herpes DNA polymerase, no new non-nucleosidic anti-herpes drugs have been introduced. Here we report new inhibitors of the HSV helicase-primase with potent in vitro anti-herpes activity, a novel mechanism of action, a low resistance rate and superior efficacy against HSV in animal models. BAY 57-1293 (N-[5-(aminosulfonyl)-4-methyl-1,3-thiazol-2-yl]-N-methyl-2-[4-(2-pyridinyl)phenyl]acetamide), a well-tolerated member of this class of compounds, significantly reduces time to healing, prevents rebound of disease after cessation of treatment and, most importantly, reduces frequency and severity of recurrent disease. Thus, this class of drugs has significant potential for the treatment of HSV disease in humans, including those resistant to current medications.
