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1.
Site-Specific Conjugation of the Indolinobenzodiazepine DGN549 to Antibodies Affords Antibody-Drug Conjugates with an Improved Therapeutic Index as Compared with Lysine Conjugation.
Bai, Chen; Reid, Emily E; Wilhelm, Alan; Shizuka, Manami; Maloney, Erin K; Laleau, Rassol; Harvey, Lauren; Archer, Katie E; Vitharana, Dilrukshi; Adams, Sharlene; Kovtun, Yelena; Miller, Michael L; Chari, Ravi; Keating, Thomas A; Yoder, Nicholas C.
Bioconjug Chem ; 31(1): 93-103, 2020 01 15.
Article de Anglais | MEDLINE | ID: mdl-31747250

RÉSUMÉ

Antibody-drug conjugates have elicited great interest recently as targeted chemotherapies for cancer. Recent preclinical and clinical data have continued to raise questions about optimizing the design of these complex therapeutics. Biochemical methods for site-specific antibody conjugation have been a design feature of recent clinical ADCs, and preclinical reports suggest that site-specifically conjugated ADCs generically offer improved therapeutic indices (i.e., the fold difference between efficacious and maximum tolerated doses). Here we present the results of a systematic preclinical comparison of ADCs embodying the DNA-alkylating linker-payload DGN549 generated with both heterogeneous lysine-directed and site-specific cysteine-directed conjugation chemistries. Importantly, the catabolites generated by each ADC are the same regardless of the conjugation format. In two different model systems evaluated, the site-specific ADC showed a therapeutic index benefit. However, the therapeutic index benefit is different in each case: both show evidence of improved tolerability, though with different magnitudes, and in one case significant efficacy improvement is also observed. These results support our contention that conjugation chemistry of ADCs is best evaluated in the context of a particular antibody, target, and linker-payload, and ideally across multiple disease models.


Sujet(s)
Antinéoplasiques immunologiques/usage thérapeutique , Benzodiazépines/usage thérapeutique , Immunoconjugués/usage thérapeutique , Lysine/usage thérapeutique , Tumeurs/traitement médicamenteux , Oxindoles/usage thérapeutique , Animaux , Antinéoplasiques alcoylants/effets indésirables , Antinéoplasiques alcoylants/composition chimique , Antinéoplasiques alcoylants/pharmacocinétique , Antinéoplasiques alcoylants/usage thérapeutique , Antinéoplasiques immunologiques/effets indésirables , Antinéoplasiques immunologiques/composition chimique , Antinéoplasiques immunologiques/pharmacocinétique , Benzodiazépines/effets indésirables , Benzodiazépines/composition chimique , Benzodiazépines/pharmacocinétique , Lignée cellulaire tumorale , Femelle , Humains , Immunoconjugués/effets indésirables , Immunoconjugués/composition chimique , Immunoconjugués/pharmacocinétique , Lysine/effets indésirables , Lysine/composition chimique , Lysine/pharmacocinétique , Souris , Souris SCID , Oxindoles/effets indésirables , Oxindoles/composition chimique , Oxindoles/pharmacocinétique , Index thérapeutique
2.
A DNA-Interacting Payload Designed to Eliminate Cross-Linking Improves the Therapeutic Index of Antibody-Drug Conjugates (ADCs).
Miller, Michael L; Shizuka, Manami; Wilhelm, Alan; Salomon, Paulin; Reid, Emily E; Lanieri, Leanne; Sikka, Surina; Maloney, Erin K; Harvey, Lauren; Qiu, Qifeng; Archer, Katie E; Bai, Chen; Vitharana, Dilrukshi; Harris, Luke; Singh, Rajeeva; Ponte, Jose F; Yoder, Nicholas C; Kovtun, Yelena; Lai, Katharine C; Ab, Olga; Pinkas, Jan; Keating, Thomas A; Chari, Ravi V J.
Mol Cancer Ther ; 17(3): 650-660, 2018 03.
Article de Anglais | MEDLINE | ID: mdl-29440292

RÉSUMÉ

Tumor-selective delivery of cytotoxic agents in the form of antibody-drug conjugates (ADCs) is now a clinically validated approach for cancer treatment. In an attempt to improve the clinical success rate of ADCs, emphasis has been recently placed on the use of DNA-cross-linking pyrrolobenzodiazepine compounds as the payload. Despite promising early clinical results with this class of ADCs, doses achievable have been low due to systemic toxicity. Here, we describe the development of a new class of potent DNA-interacting agents wherein changing the mechanism of action from a cross-linker to a DNA alkylator improves the tolerability of the ADC. ADCs containing the DNA alkylator displayed similar in vitro potency, but improved bystander killing and in vivo efficacy, compared with those of the cross-linker. Thus, the improved in vivo tolerability and antitumor activity achieved in rodent models with ADCs of the novel DNA alkylator could provide an efficacious, yet safer option for cancer treatment. Mol Cancer Ther; 17(3); 650-60. ©2018 AACR.


Sujet(s)
Immunoconjugués/pharmacologie , Intercalants/pharmacologie , Tumeurs/traitement médicamenteux , Index thérapeutique du médicament , Tests d'activité antitumorale sur modèle de xénogreffe , Animaux , Antinéoplasiques alcoylants/composition chimique , Antinéoplasiques alcoylants/métabolisme , Antinéoplasiques alcoylants/pharmacologie , Lignée cellulaire tumorale , Survie cellulaire/effets des médicaments et des substances chimiques , Réactifs réticulants/composition chimique , ADN/génétique , ADN/métabolisme , Conception de médicament , Humains , Immunoconjugués/composition chimique , Immunoconjugués/métabolisme , Intercalants/composition chimique , Intercalants/métabolisme , Souris , Tumeurs/anatomopathologie , Charge tumorale/effets des médicaments et des substances chimiques
3.
Discovery of novel spiro 1,3,4-thiadiazolines as potent, orally bioavailable and brain penetrant KSP inhibitors.
Mansoor, Umar Faruk; Angeles, Angie R; Dai, Chaoyang; Yang, Liping; Vitharana, Dilrukshi; Basso, Andrea D; Gray, Kimberly; Tang, Huadong; Liu, Ming; Liang, Lianzhu; Allbritton, Omaira; Siddiqui, M Arshad.
Bioorg Med Chem ; 23(10): 2424-34, 2015 May 15.
Article de Anglais | MEDLINE | ID: mdl-25868746

RÉSUMÉ

Kinesin spindle protein (KSP) is a mitotic kinesin that is expressed only in proliferating cells and plays a key role in spindle pole separation, formation of a bipolar mitotic spindle, as well as centrosome separation and maturation. Inhibition of KSP has the potential to provide anti-tumor activity while avoiding peripheral neuropathy associated with some microtubule-targeted drugs. Based on MK-0731 and related heterocyclic compounds targeting the KSP monastrol binding site, structurally constrained spiro-cyclic KSP inhibitors were designed. In particular, rapid evaluation and optimization of the novel spiro 1,3,4-thiadiazolines resulted in a series of potent KSP inhibitors demonstrating mechanism based activities in cells, including induction of the mitotic marker phospho-histone H3 and induction of monaster spindle formation. Further optimization of the pharmacokinetic (PK) properties afforded MK-8267 as a potent, orally bioavailable and brain penetrant KSP inhibitor which showed anti-tumor activity in preclinical xenograft models.


Sujet(s)
Antinéoplasiques/synthèse chimique , Tumeurs du cerveau/traitement médicamenteux , Kinésine/antagonistes et inhibiteurs , Spiranes/synthèse chimique , Thiadiazoles/synthèse chimique , Modulateurs de la polymérisation de la tubuline/synthèse chimique , Administration par voie orale , Animaux , Antinéoplasiques/pharmacocinétique , Antinéoplasiques/pharmacologie , Marqueurs biologiques/métabolisme , Barrière hémato-encéphalique/effets des médicaments et des substances chimiques , Tumeurs du cerveau/génétique , Tumeurs du cerveau/métabolisme , Tumeurs du cerveau/anatomopathologie , Lignée cellulaire tumorale , Chiens , Découverte de médicament , Cellules HCT116 , Histone/métabolisme , Humains , Kinésine/génétique , Kinésine/métabolisme , Mâle , Souris , Perméabilité , Pipéridines/composition chimique , Pyrimidines/composition chimique , Pyrroles/composition chimique , Rats , Spiranes/pharmacocinétique , Spiranes/pharmacologie , Thiadiazoles/pharmacocinétique , Thiadiazoles/pharmacologie , Thiones/composition chimique , Modulateurs de la polymérisation de la tubuline/pharmacocinétique , Modulateurs de la polymérisation de la tubuline/pharmacologie , Tests d'activité antitumorale sur modèle de xénogreffe
4.
Design, synthesis, and pharmacological evaluation of glutamate carboxypeptidase II (GCPII) inhibitors based on thioalkylbenzoic acid scaffolds.
Stoermer, Doris; Vitharana, Dilrukshi; Hin, Niyada; Delahanty, Greg; Duvall, Bridget; Ferraris, Dana V; Grella, Brian S; Hoover, Randall; Rojas, Camilo; Shanholtz, Megan K; Smith, Kyle P; Stathis, Marigo; Wu, Ying; Wozniak, Krystyna M; Slusher, Barbara S; Tsukamoto, Takashi.
J Med Chem ; 55(12): 5922-32, 2012 Jun 28.
Article de Anglais | MEDLINE | ID: mdl-22642259

RÉSUMÉ

A series of thiol-based glutamate carboxypeptidase II (GCPII) inhibitors have been synthesized with either a 3-(mercaptomethyl)benzoic acid or 2-(2-mercaptoethyl)benzoic acid scaffold. Potent inhibitors were identified from each of the two scaffolds with IC(50) values in the single-digit nanomolar range, including 2-(3-carboxybenzyloxy)-5-(mercaptomethyl)benzoic acid 27c and 3-(2-mercaptoethyl)biphenyl-2,3'-dicarboxylic acid 35c. Compound 35c was found to be metabolically stable and selective over a number of targets related to glutamate-mediated neurotransmission. Furthermore, compound 35c was found to be orally available in rats and exhibited efficacy in an animal model of neuropathic pain following oral administration.


Sujet(s)
Benzoates/synthèse chimique , Benzoates/pharmacologie , Conception de médicament , Antienzymes/synthèse chimique , Antienzymes/pharmacologie , Glutamate carboxypeptidase II/antagonistes et inhibiteurs , Animaux , Benzoates/pharmacocinétique , Benzoates/usage thérapeutique , Techniques de chimie synthétique , Antienzymes/pharmacocinétique , Antienzymes/usage thérapeutique , Humains , Concentration inhibitrice 50 , Névralgie/traitement médicamenteux , Rats
5.
Design and synthesis of potent Gram-negative specific LpxC inhibitors.
Mansoor, U Faruk; Vitharana, Dilrukshi; Reddy, Panduranga Adulla; Daubaras, Dayna L; McNicholas, Paul; Orth, Peter; Black, Todd; Siddiqui, M Arshad.
Bioorg Med Chem Lett ; 21(4): 1155-61, 2011 Feb 15.
Article de Anglais | MEDLINE | ID: mdl-21273067

RÉSUMÉ

Antibiotic resistant hospital acquired infections are on the rise, creating an urgent need for novel bactericidal drugs. Enzymes involved in lipopolysaccharide (LPS) biosynthesis are attractive antibacterial targets since LPS is the major structural component of the outer membrane of Gram-negative bacteria. Lipid A is an essential hydrophobic anchor of LPS and the first committed step in lipid A biosynthesis is catalyzed by a unique zinc dependent metalloamidase, UDP-3-O-(R-3-hydroxymyristoyl)-N-acetylglucosamine deacetylase (LpxC). LpxC is an attractive Gram-negative only target that has been chemically validated by potent bactericidal hydroxamate inhibitors that work by coordination of the enzyme's catalytic zinc ion. An exploratory chemistry effort focused on expanding the SAR around hydroxamic acid zinc-binding 'warheads' lead to the identification of novel compounds with enzyme potency and antibacterial activity similar to CHIR-090.


Sujet(s)
Amidohydrolases/antagonistes et inhibiteurs , Antibactériens/synthèse chimique , Bactéries à Gram négatif/effets des médicaments et des substances chimiques , Amidohydrolases/métabolisme , Antibactériens/composition chimique , Antibactériens/pharmacologie , Benzodiazépinones/composition chimique , Sites de fixation , Catalyse , Domaine catalytique , Cristallographie aux rayons X , Conception de médicament , Acides hydroxamiques/composition chimique , Tests de sensibilité microbienne , Relation structure-activité , Zinc/composition chimique
6.
Enantiospecificity of glutamate carboxypeptidase II inhibition.
Tsukamoto, Takashi; Majer, Pavel; Vitharana, Dilrukshi; Ni, Chiyou; Hin, Bunda; Lu, Xi-Chun M; Thomas, Ajit G; Wozniak, Krystyna M; Calvin, David C; Wu, Ying; Slusher, Barbara S; Scarpetti, David; Bonneville, George W.
J Med Chem ; 48(7): 2319-24, 2005 Apr 07.
Article de Anglais | MEDLINE | ID: mdl-15801825

RÉSUMÉ

Two representative glutamate carboxypeptidase II (GCP II) inhibitors, 2-(hydroxypentafluorophenylmethyl-phosphinoylmethyl)pentanedioic acid 2 and 2-(3-mercaptopropyl)pentanedioic acid 3, were synthesized in high optical purities (>97%ee). The two enantiomers of 2 were prepared from previously reported chiral intermediates, (R)- and (S)-2-(hydroxyphosphinoylmethyl)pentanedioic acid benzyl esters 8. The synthesis of (R)- and (S)-3 involves the hydrolysis of (R)- and (S)-3-(2-oxo-tetrahydro-thiopyran-3-yl)propionic acids, (R)- and (S)-11, the corresponding optically pure thiolactones delivered by chiral chromatographic separation of the racemic 11. GCP II inhibitory assay revealed that (S)-2 is 40-fold more potent than (R)-2. In contrast, both enantiomers of 3 inhibited GCP II with nearly equal potency. The efficacy observed in subsequent animal studies with these enantiomers correlated well with the inhibitory potency in a GCP II assay.


Sujet(s)
Glutamate carboxypeptidase II/antagonistes et inhibiteurs , Glutarates/synthèse chimique , Acides phosphiniques/synthèse chimique , Thiols/synthèse chimique , Analgésiques/synthèse chimique , Analgésiques/composition chimique , Analgésiques/pharmacologie , Animaux , Encéphalopathie ischémique/métabolisme , Cortex cérébral/effets des médicaments et des substances chimiques , Cortex cérébral/métabolisme , Sténose pathologique/complications , Cristallographie aux rayons X , Glutamate carboxypeptidase II/composition chimique , Glutarates/composition chimique , Glutarates/pharmacologie , Infarctus du territoire de l'artère cérébrale moyenne/traitement médicamenteux , L-Lactate dehydrogenase/métabolisme , Structure moléculaire , Neuroprotecteurs/synthèse chimique , Neuroprotecteurs/composition chimique , Neuroprotecteurs/pharmacologie , Douleur/traitement médicamenteux , Douleur/étiologie , Neuropathies périphériques/traitement médicamenteux , Neuropathies périphériques/étiologie , Acides phosphiniques/composition chimique , Acides phosphiniques/pharmacologie , Rats , Stéréoisomérie , Relation structure-activité , Thiols/composition chimique , Thiols/pharmacologie , Techniques de culture de tissus
7.
Synthesis and biological evaluation of thiol-based inhibitors of glutamate carboxypeptidase II: discovery of an orally active GCP II inhibitor.
Majer, Pavel; Jackson, Paul F; Delahanty, Greg; Grella, Brian S; Ko, Yao-Sen; Li, Weixing; Liu, Qun; Maclin, Keith M; Poláková, Jana; Shaffer, Kathryn A; Stoermer, Doris; Vitharana, Dilrukshi; Wang, Eric Yanjun; Zakrzewski, Anthony; Rojas, Camilo; Slusher, Barbara S; Wozniak, Krystyna M; Burak, Eric; Limsakun, Tharin; Tsukamoto, Takashi.
J Med Chem ; 46(10): 1989-96, 2003 May 08.
Article de Anglais | MEDLINE | ID: mdl-12723961

RÉSUMÉ

A series of 2-(thioalkyl)pentanedioic acids were synthesized and evaluated as inhibitors of glutamate carboxypeptidase II (GCP II, EC 3.4.17.21). The inhibitory potency of these thiol-based compounds against GCP II was found to be dependent on the number of methylene units between the thiol group and pentanedioic acid. A comparison of the SAR of the thiol-based inhibitors to that of the phosphonate-based inhibitors provides insight into the role of each of the two zinc-binding groups in GCP II inhibition. The most potent thiol-based inhibitor, 2-(3-mercaptopropyl)pentanedioic acid (IC(50) = 90 nM), was found to be orally bioavailable in rats and exhibited efficacy in an animal model of neuropathic pain following oral administration.


Sujet(s)
Analgésiques/synthèse chimique , Carboxypeptidases/antagonistes et inhibiteurs , Antienzymes/synthèse chimique , Glutarates/synthèse chimique , Thiols/synthèse chimique , Administration par voie orale , Analgésiques/composition chimique , Analgésiques/pharmacologie , Animaux , Biodisponibilité , Carboxypeptidases/composition chimique , Sténose pathologique/complications , Antienzymes/composition chimique , Antienzymes/pharmacologie , Glutamate carboxypeptidase II , Glutarates/composition chimique , Glutarates/pharmacologie , Température élevée , Hyperalgésie/traitement médicamenteux , Hyperalgésie/étiologie , Mâle , Douleur/traitement médicamenteux , Douleur/étiologie , Neuropathies périphériques/complications , Rats , Rat Sprague-Dawley , Nerf ischiatique , Relation structure-activité , Thiols/composition chimique , Thiols/pharmacologie
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