Your search keyword '"Mark S. Tichenor"' showing total 18 results

1. Discovery of JNJ-64264681: A Potent and Selective Covalent Inhibitor of Bruton’s Tyrosine Kinase

Author

Mark S. Tichenor, John J. M. Wiener, Navin L. Rao, Genesis M. Bacani, Jianmei Wei, Charlotte Pooley Deckhut, J. Kent Barbay, Kevin D. Kreutter, Leon Chang, Kathleen W. Clancy, Heather E. Murrey, Weixue Wang, Kay Ahn, Michael Huber, Elizabeth Rex, Kevin J. Coe, Jiejun Wu, Haopeng Rui, Kia Sepassi, Marcello Gaudiano, Mariette Bekkers, Ivo Cornelissen, Kathryn Packman, Mark Seierstad, Christos Xiouras, Scott D. Bembenek, Richard Alexander, Cynthia Milligan, Sriram Balasubramanian, Alec D. Lebsack, Jennifer D. Venable, Ulrike Philippar, James P. Edwards, and Gavin Hirst

Subjects

Arthritis, Rheumatoid, Drug Discovery, Agammaglobulinaemia Tyrosine Kinase, Humans, Lupus Erythematosus, Systemic, Molecular Medicine, Protein Kinase Inhibitors, Autoimmune Diseases

Abstract

Bruton's tyrosine kinase (BTK) is a Tec family kinase that plays an essential role in B-cell receptor (BCR) signaling as well as Fcγ receptor signaling in leukocytes. Pharmacological inhibition of BTK has been shown to be effective in treating hematological malignancies and is hypothesized to provide an effective strategy for the treatment of autoimmune diseases such as rheumatoid arthritis and systemic lupus erythematosus. We report the discovery and preclinical properties of JNJ-64264681 (

Published

2022

2. Discovery of a Potent and Selective Covalent Inhibitor of Bruton’s Tyrosine Kinase with Oral Anti-Inflammatory Activity

Author

Jennifer D. Venable, Weixue Wang, Jianmei Wei, Heather E. Murrey, Mark S. Tichenor, Kristi A. Leonard, Michael Huber, Alec D. Lebsack, Genesis M. Bacani, Scott D. Bembenek, Kay Ahn, J. Kent Barbay, Leon Chang, Kevin D. Kreutter, Navin Rao, Charlotte Pooley Deckhut, Jiejun Wu, Kevin J. Coe, Elizabeth B. Rex, John J. M. Wiener, James P. Edwards, and Mark Seierstad

Subjects

Cell type, biology, 010405 organic chemistry, Chemistry, medicine.drug_class, Organic Chemistry, Arthritis, Inflammation, medicine.disease, 01 natural sciences, Biochemistry, Anti-inflammatory, 0104 chemical sciences, 010404 medicinal & biomolecular chemistry, immune system diseases, In vivo, hemic and lymphatic diseases, Drug Discovery, Cancer research, medicine, biology.protein, Bruton's tyrosine kinase, medicine.symptom, Tyrosine kinase, Cysteine

Abstract

[Image: see text] Bruton’s tyrosine kinase (BTK) is a cytoplasmic tyrosine kinase that plays a critical role in the activation of B cells, macrophages, and osteoclasts. Given the key role of these cell types in the pathology of autoimmune disorders, BTK inhibitors have the potential to improve treatment outcomes in multiple diseases. Herein, we report the discovery and characterization of a novel potent and selective covalent 4-oxo-4,5-dihydro-3H-1-thia-3,5,8-triazaacenaphthylene-2-carboxamide BTK inhibitor chemotype. Compound 27 irreversibly inhibits BTK by targeting a noncatalytic cysteine residue (Cys481) for covalent bond formation. Compound 27 is characterized by selectivity for BTK, potent in vivo BTK occupancy that is sustained after it is cleared from systemic circulation, and dose-dependent efficacy at reducing joint inflammation in a rat collagen-induced arthritis model.

Published

2021

3. Novel Reagent Space: Identifying Unorderable but Readily Synthesizable Building Blocks

Author

Eduardo V. Mercado-Marin, Jim Na, Renee L. DesJarlais, Helena C. Steffens, Genesis M. Bacani, Mark Seierstad, De Michael Chung, Taraneh Mirzadegan, and Mark S. Tichenor

Subjects

Drug discovery, Computer science, Reagent, Distributed computing, Organic Chemistry, Drug Discovery, Space (commercial competition), Biochemistry, Chemical space

Abstract

[Image: see text] Drug discovery building blocks available commercially or within an internal inventory cover a diverse range of chemical space and yet describe only a tiny fraction of all chemically feasible reagents. Vendors will eagerly provide tools to search the former; there is no straightforward method of mining the latter. We describe a procedure and use case in assembling chemical structures not available for purchase but that could likely be synthesized in one robust chemical transformation starting from readily available building blocks. Accessing this vast virtual chemical space dramatically increases our curated collection of reagents available for medicinal chemistry exploration and novel hit generation, almost tripling the number of those with 10 or fewer atoms.

Published

2021

4. Discovery of a Gut-Restricted JAK Inhibitor for the Treatment of Inflammatory Bowel Disease

Author

Kristi A. Leonard, Kevin D. Kreutter, Suzie Kim, Tadimeti S. Rao, Michael C. Harris, Wenying Chai, Tatiana Koudriakova, Paul J. Krawczuk, Russell C. Smith, James P. Edwards, Mark Seierstad, Marguerite E. Johnson, Lisa Madge, Jennifer D. Venable, Gavin C. Hirst, Genesis M. Bacani, Aihua Wang, Ravi Malaviya, Mark S. Tichenor, Michele C. Rizzolio, and Ashok S. Mathur

Subjects

Pyridines, Administration, Oral, Pharmacology, 01 natural sciences, Inflammatory bowel disease, Permeability, Madin Darby Canine Kidney Cells, 03 medical and health sciences, chemistry.chemical_compound, Mice, Dogs, Drug Discovery, medicine, Animals, Humans, Janus Kinase Inhibitors, Dosing, Phosphorylation, Adverse effect, 030304 developmental biology, Janus Kinases, 0303 health sciences, Chemistry, Drug discovery, medicine.disease, Inflammatory Bowel Diseases, 0104 chemical sciences, Mice, Inbred C57BL, 010404 medicinal & biomolecular chemistry, Pharmacodynamics, Molecular Medicine, Female, Janus kinase, Lead compound

Abstract

To identify Janus kinase (JAK) inhibitors that selectively target gastrointestinal tissues with limited systemic exposures, a class of imidazopyrrolopyridines with a range of physical properties was prepared and evaluated. We identified compounds with low intrinsic permeability and determined a correlation between permeability and physicochemical properties, clogP and tPSA, for a subset of compounds. This low intrinsic permeability translated into compounds displaying high colonic exposure and low systemic exposure after oral dosing at 25 mg/kg in mouse. In a mouse PK/PD model, oral dosing of lead compound 2 demonstrated dose-dependent inhibition of pSTAT phosphorylation in colonic explants post-oral dose but low systemic exposure and no measurable systemic pharmacodynamic activity. We thus demonstrate the utility of JAK inhibitors with low intrinsic permeability as a feasible approach to develop gut-restricted, pharmacologically active molecules with a potential advantage over systemically available compounds that are limited by systemic on-target adverse events.

Published

2020

5. Functional Profiling of 2-Aminopyrimidine Histamine H4 Receptor Modulators

Author

Brad M. Savall, Jennifer D. Venable, Robin L. Thurmond, and Mark S. Tichenor

Subjects

Allergy, Drug discovery, Inflammation, Pharmacology, Biology, medicine.disease, Histamine agonist, chemistry.chemical_compound, Histamine receptor, chemistry, Drug Discovery, Immunology, medicine, Molecular Medicine, Histamine H4 receptor, medicine.symptom, Receptor, Histamine

Abstract

Histamine is an important endogenous signaling molecule that is involved in a number of physiological processes including allergic reactions, gastric acid secretion, neurotransmitter release, and inflammation. The biological effects of histamine are mediated by four histamine receptors with distinct functions and distribution profiles (H1-H4). The most recently discovered histamine receptor (H4) has emerged as a promising drug target for treating inflammatory diseases. A detailed understanding of the role of the H4 receptor in human disease remains elusive, in part because low sequence similarity between the human and rodent H4 receptors complicates the translation of preclinical pharmacology to humans. This review provides an overview of H4 drug discovery programs that have studied cross-species structure-activity relationships, with a focus on the functional profiling of the 2-aminopyrimidine chemotype that has advanced to the clinic for allergy, atopic dermatitis, asthma, and rheumatoid arthritis.

Published

2015

6. The SAR of brain penetration for a series of heteroaryl urea FAAH inhibitors

Author

Sandy J. Wilson, Brian Scott, Mark S. Tichenor, Michele C. Rizzolio, Sandra R. Chaplan, Michael Webb, James A. Palmer, J. Guy Breitenbucher, Michelle L. Wennerholm, Raymond Rynberg, Mark Seierstad, Wei Xiao, Mark J. Karbarz, Richard Apodaca, John M. Keith, William M. Jones, and Joan Pierce

Subjects

0301 basic medicine, Stereochemistry, Clinical Biochemistry, Central nervous system, Pharmaceutical Science, Blood–brain barrier, Biochemistry, Amidohydrolases, 03 medical and health sciences, chemistry.chemical_compound, Structure-Activity Relationship, 0302 clinical medicine, Pharmacokinetics, Fatty acid amide hydrolase, Drug Discovery, medicine, Humans, Urea, Enzyme Inhibitors, Molecular Biology, chemistry.chemical_classification, Dose-Response Relationship, Drug, Molecular Structure, Organic Chemistry, Target engagement, Brain, Penetration (firestop), 030104 developmental biology, medicine.anatomical_structure, Enzyme, chemistry, Molecular Medicine, 030217 neurology & neurosurgery

Abstract

The SAR of brain penetration for a series of heteroaryl piperazinyl- and piperadinyl-urea fatty acid amide hydrolase (FAAH) inhibitors is described. Brain/plasma (B/P) ratios ranging from >4:1 to as low as 0.02:1 were obtained through relatively simple structural changes to various regions of the heteroaryl urea scaffold. It was not possible to predict the degree of central nervous system (CNS) penetration from the volumes of distribution (Vd) obtained from pharmacokinetic (PK) experiments as very high Vds did not correlate with high B/P ratios. Similarly, calculated topological polar surface areas (TPSAs) did not consistently correlate with the degree of brain penetration. The lowest B/P ratios were observed for those compounds that were significantly ionized at physiological pH. However, as this class of compounds inhibits the FAAH enzyme through covalent modification, low B/P ratios did not preclude effective central target engagement.

Published

2016

7. Aryl Piperazinyl Ureas as Inhibitors of Fatty Acid Amide Hydrolase (FAAH) in Rat, Dog, and Primate

Author

Michael Webb, Sean Brown, Sandy J. Wilson, John M. Keith, Michelle Wennerholm, James A. Palmer, Lin Luo, Mark S. Tichenor, Wei Xiao, Michele C. Rizzolio, Brian Scott, Leon Chang, J. Guy Breitenbucher, William M. Jones, Sandra R. Chaplan, Raymond Rynberg, Joan Pierce, Rich Apodaca, Mark Seierstad, and Mark J. Karbarz

Subjects

chemistry.chemical_classification, Aryl, Organic Chemistry, Fatty acid, Anandamide, Pharmacology, Biochemistry, chemistry.chemical_compound, Enzyme, chemistry, Covalent bond, Fatty acid amide hydrolase, Drug Discovery, Urea, Ethanolamide, lipids (amino acids, peptides, and proteins)

Abstract

A series of aryl piperazinyl ureas that act as covalent inhibitors of fatty acid amide hydrolase (FAAH) is described. A potent and selective (does not inhibit FAAH-2) member of this class, JNJ-40355003, was found to elevate the plasma levels of three fatty acid amides: anandamide, oleoyl ethanolamide, and palmitoyl ethanolamide, in the rat, dog, and cynomolgous monkey. The elevation of the levels of these lipids in the plasma of monkeys suggests that FAAH-2 may not play a significant role in regulating plasma levels of fatty acid ethanolamides in primates.

Published

2012

8. Yatakemycin: total synthesis, DNA alkylation, and biological properties

Author

Dale L. Boger and Mark S. Tichenor

Subjects

Indoles, Natural product, Alkylation, Molecular Structure, Chemistry, Organic Chemistry, Molecular Conformation, Total synthesis, Stereoisomerism, DNA, Crystallography, X-Ray, Yatakemycin, Biochemistry, Combinatorial chemistry, Small molecule, Duocarmycins, DNA Alkylation, chemistry.chemical_compound, Biological property, Drug Discovery, Pyrroles, Biological evaluation

Abstract

Covering: up to 2007 DNA-binding small molecules are an important source of anticancer therapeutics that display a diverse array of mechanisms of action. Synthetic studies on the new DNA-alkylating natural product yatakemycin, detailed in this Highlight, have served to reassign its structure, assign the absolute stereochemistry, and provide access to yatakemycin and a series of structural analogues for biological evaluation. Studies on the DNA alkylation properties of (+)- and ent-(−)-yatakemycin and related analogues have demonstrated the enhanced DNA alkylation properties of this class of agents and provided insight into their interaction with DNA.

Published

2008

9. Preclinical Characterization of the FAAH Inhibitor JNJ-42165279

Author

John M. Keith, Sandy J. Wilson, Michelle L. Wennerholm, William M. Jones, Raymond Rynberg, Leon Chang, Breitenbucher Jg, Jing Liu, Michael Webb, Lin Luo, Brian Scott, Mark S. Tichenor, Michele C. Rizzolio, Chaplan, James A. Palmer, Mark J. Karbarz, and Mark Seierstad

Subjects

chemistry.chemical_classification, business.industry, Organic Chemistry, Transporter, Anandamide, Pharmacology, Biochemistry, chemistry.chemical_compound, Enzyme, chemistry, Fatty acid amide hydrolase, Drug Discovery, Ethanolamide, Medicine, lipids (amino acids, peptides, and proteins), business, Receptor, Ion channel, ADME

Abstract

The pre-clinical characterization of the aryl piperazinyl urea inhibitor of fatty acid amide hydrolase (FAAH) JNJ-42165279 is described. JNJ-42165279 covalently inactivates the FAAH enzyme, but is highly selective with regard to other enzymes, ion channels, transporters, and receptors. JNJ-42165279 exhibited excellent ADME and pharmacodynamic properties as evidenced by its ability to block FAAH in the brain and periphery of rats and thereby cause an elevation of the concentrations of anandamide (AEA), oleoyl ethanolamide (OEA), and palmitoyl ethanolamide (PEA). The compound was also efficacious in the spinal nerve ligation (SNL) model of neuropathic pain. The combination of good physical, ADME, and PD properties of JNJ-42165279 supported it entering the clinical portfolio.

Published

2015

10. Functional Profiling of 2-Aminopyrimidine Histamine H4 Receptor Modulators

Author

Mark S, Tichenor, Robin L, Thurmond, Jennifer D, Venable, and Brad M, Savall

Subjects

Histamine Antagonists, Aminopyridines, Asthma, Dermatitis, Atopic, Receptors, G-Protein-Coupled, Arthritis, Rheumatoid, Drug Partial Agonism, Histamine Agonists, Structure-Activity Relationship, Hypersensitivity, Animals, Humans, Receptors, Histamine, Receptors, Histamine H4

Abstract

Histamine is an important endogenous signaling molecule that is involved in a number of physiological processes including allergic reactions, gastric acid secretion, neurotransmitter release, and inflammation. The biological effects of histamine are mediated by four histamine receptors with distinct functions and distribution profiles (H1-H4). The most recently discovered histamine receptor (H4) has emerged as a promising drug target for treating inflammatory diseases. A detailed understanding of the role of the H4 receptor in human disease remains elusive, in part because low sequence similarity between the human and rodent H4 receptors complicates the translation of preclinical pharmacology to humans. This review provides an overview of H4 drug discovery programs that have studied cross-species structure-activity relationships, with a focus on the functional profiling of the 2-aminopyrimidine chemotype that has advanced to the clinic for allergy, atopic dermatitis, asthma, and rheumatoid arthritis.

Published

2015

11. Asymmetric Total Synthesis of (+)- and ent-(−)-Yatakemycin and Duocarmycin SA: Evaluation of Yatakemycin Key Partial Structures and Its Unnatural Enantiomer

Author

David B. Kastrinsky, Dale L. Boger, Futoshi Shiga, Inkyu Hwang, John David Trzupek, and Mark S. Tichenor

Subjects

Alkylating Agents, Indoles, Alkylation, Base pair, Stereochemistry, Stereoisomerism, Biochemistry, Article, Catalysis, Adduct, Duocarmycins, Colloid and Surface Chemistry, Pyrroles, Base Pairing, Antibiotics, Antineoplastic, Base Sequence, Chemistry, Adenine, Temperature, Enantioselective synthesis, Absolute configuration, Total synthesis, DNA, General Chemistry, Hydrogen-Ion Concentration, Streptomyces, Kinetics, Models, Chemical, Enantiomer

Abstract

Complementary to studies that provided the first yatakemycin total synthesis resulting in its structure revision and absolute stereochemistry assignment, a second-generation asymmetric total synthesis is disclosed herein. Since the individual yatakemycin subunits are identical to those of duocarmycin SA (alkylation subunit) or CC-1065 (central and right-hand subunits), the studies also provide an improvement in our earlier total synthesis of CC-1065 and, as detailed herein, have been extended to an asymmetric total synthesis of (+)-duocarmycin SA. Further extensions of the studies provided key yatakemycin partial structures and analogues for comparative assessments. This included the definition of the DNA selectivity (adenine central to a five-base-pair AT sequence, e.g., 5'-AAAAA), efficiency, relative rate, and reversibility of ent-(-)-yatakemycin and its comparison with the natural enantiomer (identical selectivity and efficiency), structural characterization of the adenine N3 adduct confirming the nature of the DNA reaction, and comparisons of the cytotoxic activity of the natural product (L1210, IC50 = 5 pM) with those of its unnatural enantiomer (IC50 = 5 pM) and a series of key partial structures including those that probe the role of the C-terminus thiomethyl ester. The only distinguishing features between the enantiomers is that ent-(-)-yatakemycin alkylates DNA at a slower rate (krel = 0.13) and is reversible, whereas (+)-yatakemycin is not. Nonetheless, even ent-(-)-yatakemycin alkylates DNA at a faster rate and with a greater thermodynamic stability than (+)-duocarmycin SA, illustrating the unique characteristics of such "sandwiched" agents.

Published

2006

12. Rational design, synthesis, and evaluation of key analogues of CC-1065 and the duocarmycins

Author

Gianpiero Spalluto, Pier Giovanni Baraldi, Lorenzo Zanella, Dale L. Boger, Karen S. MacMillan, Abdel Naser Zaid, Maria Giovanna Pavani, Thomas J. Rayl, Scott E. Wolkenberg, James S. Stover, Inkyu Hwang, Mark S. Tichenor, MARK S., Tichenor, KAREN S., Macmillan, JAMES S., Stover, SCOTT E., Wolkenberg, MARIA G., Pavani, Lorenzo, Zanella, ABDEL N., Zaid, Spalluto, Giampiero, THOMAS J., Rayl, Inkyu, Hwang, PIER GIOVANNI, Baraldi, and DALE L., Boger

Subjects

Alkylating Agents, DNA, antitumor, Indoles, Alkylation, Stereochemistry, Stereoisomerism, Biochemistry, Catalysis, Drug Administration Schedule, Article, chemistry.chemical_compound, Duocarmycins, Mice, Colloid and Surface Chemistry, Cell Line, Tumor, Potency, Animals, Combinatorial Chemistry Techniques, Reactivity (chemistry), Pyrroles, Natural product, Antiparasitic Agents, Dose-Response Relationship, Drug, Molecular Structure, Chemistry, Rational design, General Chemistry, Combinatorial chemistry, Xenograft Model Antitumor Assays, Survival Rate, DNA Alkylation, Disease Models, Animal, Mice, Inbred DBA, Drug Design, Selectivity, Injections, Intraperitoneal

Abstract

The design, synthesis, and evaluation of a predictably more potent analogue of CC-1065 entailing the substitution replacement of a single skeleton atom in the alkylation subunit are disclosed and were conducted on the basis of design principles that emerged from a fundamental parabolic relationship between chemical reactivity and cytotoxic potency. Consistent with projections, the 7-methyl-1,2,8,8a-tetrahydrocyclopropa[c]thieno[3,2-e]indol-4-one (MeCTI) alkylation subunit and its isomer 6-methyl-1,2,8,8a-tetrahydrocyclopropa[c]thieno[2,3-e]indol-4-one (iso-MeCTI) were found to be 5-6 times more stable than the MeCPI alkylation subunit found in CC-1065 and slightly more stable than even the DSA alkylation subunit found in duocarmycin SA, placing it at the point of optimally balanced stability and reactivity for this class of antitumor agents. Their incorporation into the key analogues of the natural products provided derivatives that surpassed the potency of MeCPI derivatives (3-10-fold), matching or slightly exceeding the potency of the corresponding DSA derivatives, consistent with projections made on the basis of the parabolic relationship. Notable of these, MeCTI-TMI proved to be as potent as or slightly more potent than the natural product duocarmycin SA (DSA-TMI, IC50 = 5 vs 8 pM), and MeCTI-PDE2 proved to be 3-fold more potent than the natural product CC-1065 (MeCPI-PDE2, IC50 = 7 vs 20 pM). Both exhibited efficiencies of DNA alkylation that correlate with this enhanced potency without impacting the intrinsic selectivity characteristic of this class of antitumor agents.

Published

2007

13. Heteroaryl urea inhibitors of fatty acid amide hydrolase: structure-mutagenicity relationships for arylamine metabolites

Author

William M. Jones, Mark S. Tichenor, Sean Brown, Natalie A. Hawryluk, James A. Palmer, Lin Luo, Marlies De Boeck, Filip Woestenborghs, J. Guy Breitenbucher, Michelle Wennerholm, Joan Pierce, D. Beerens, Michael Webb, John M. Keith, Sandy J. Wilson, Jeff Merit, Sandra R. Chaplan, Mark Seierstad, and Mark J. Karbarz

Subjects

Clinical Biochemistry, Pharmaceutical Science, Biochemistry, Amidohydrolases, Mixed Function Oxygenases, Serine, chemistry.chemical_compound, Structure-Activity Relationship, Fatty acid amide hydrolase, Drug Discovery, Structure–activity relationship, Organic chemistry, Animals, Humans, Urea, Amines, Enzyme Inhibitors, Molecular Biology, chemistry.chemical_classification, biology, Dose-Response Relationship, Drug, Molecular Structure, Chemistry, Mutagenicity Tests, Organic Chemistry, Aromatic amine, Active site, Rats, Electrophile, biology.protein, Molecular Medicine, lipids (amino acids, peptides, and proteins), Amine gas treating, Mutagens

Abstract

The structure-activity relationships for a series of heteroaryl urea inhibitors of fatty acid amide hydrolase (FAAH) are described. Members of this class of inhibitors have been shown to inactivate FAAH by covalent modification of an active site serine with subsequent release of an aromatic amine from the urea electrophile. Systematic Ames II testing guided the optimization of urea substituents by defining the structure-mutagenicity relationships for the released aromatic amine metabolites. Potent FAAH inhibitors were identified having heteroaryl amine leaving groups that were non-mutagenic in the Ames II assay.

Published

2012

14. ChemInform Abstract: Yatakemycin: Total Synthesis, DNA Alkylation, and Biological Properties

Author

Dale L. Boger and Mark S. Tichenor

Subjects

chemistry.chemical_compound, DNA Alkylation, Natural product, chemistry, Biological property, Total synthesis, General Medicine, Yatakemycin, Small molecule, Combinatorial chemistry, DNA, Biological evaluation

Abstract

Covering: up to 2007 DNA-binding small molecules are an important source of anticancer therapeutics that display a diverse array of mechanisms of action. Synthetic studies on the new DNA-alkylating natural product yatakemycin, detailed in this Highlight, have served to reassign its structure, assign the absolute stereochemistry, and provide access to yatakemycin and a series of structural analogues for biological evaluation. Studies on the DNA alkylation properties of (+)- and ent-(−)-yatakemycin and related analogues have demonstrated the enhanced DNA alkylation properties of this class of agents and provided insight into their interaction with DNA.

Published

2008

15. Systematic exploration of the structural features of yatakemycin impacting DNA alkylation and biological activity

Author

Karen S. MacMillan, Mark S. Tichenor, Thomas J. Rayl, John David Trzupek, Dale L. Boger, and Inkyu Hwang

Subjects

Models, Molecular, Antibiotics, Antineoplastic, Indoles, Alkylation, Chemistry, Stereochemistry, Protein subunit, Absolute configuration, General Chemistry, DNA, Biochemistry, Catalysis, Article, DNA Alkylation, chemistry.chemical_compound, Duocarmycins, Structure-Activity Relationship, Colloid and Surface Chemistry, Structure–activity relationship, Pyrroles, Enantiomer, Selectivity

Abstract

A systematic examination of the impact of the yatakemycin left and right subunits and their substituents is detailed along with a study of its unique three subunit arrangement (sandwiched vs extended and reversed analogues). The examination of the ca. 50 analogues prepared illustrate that within the yatakemycin three subunit structure, the subunit substituents are relatively unimportant and that it is the unique sandwiched arrangement that substantially increases the rate and optimizes the efficiency of its DNA alkylation reaction. This potentiates the cytotoxic activity of yatakemycin and its analogues overcoming limitations typically observed with more traditional compounds in the series (CC-1065, duocarmycins). Moreover, a study of the placement of the alkylation subunit within the three subunit arrangement (sandwiched vs extended and reversed analogues) indicates that it has a profound impact not only on the rate and efficiency of DNA alkylation, but that it controls and establishes the DNA alkylation selectivity as well, where both enantiomers of such sandwiched agents alkylate the same adenine sites exhibiting the same DNA alkylation selectivity independent of their absolute configuration.

Published

2007

16. Asymmetric Total Synthesis of (+)- and ent-(-)-Yatakemycin (I) and Duocarmycin SA (II): Evaluation of Yatakemycin Key Partial Structures and Its Unnatural Enantiomer

Author

John David Trzupek, David B. Kastrinsky, Inkyu Hwang, Mark S. Tichenor, Dale L. Boger, and Futoshi Shiga

Subjects

Duocarmycin SA, Chemistry, Stereochemistry, Total synthesis, General Medicine, Enantiomer, Yatakemycin

Published

2007

17. Ruthenium-mediated cycloaromatization of acyclic enediynes and dienynes at ambient temperature

Author

Mark S. Tichenor, Seth J. Friese, and Joseph M. O'Connor

Subjects

Temperature, chemistry.chemical_element, General Chemistry, Reaction intermediate, Biochemistry, Medicinal chemistry, Catalysis, Ruthenium, Solvent, Colloid and Surface Chemistry, chemistry, Alkynes, Organometallic Compounds, Organic chemistry, Polycyclic Aromatic Hydrocarbons

Abstract

The ruthenium(II) cation, [Cp*Ru(NCMe)3]OTf (4), triggers the Bergman cycloaromatization of acyclic endiynes at room temperature in THF solvent. Treatment of 1,2-di(1-alkynynyl)cyclopentenes (13-Me, alkynyl = propynyl; 13-Prn, alkynyl = pentynyl; 13-Bui, alkynyl = 4-methyl-pent-1-ynyl) with 4 in THF solvent at room temperature gives rise to the ruthenium arene complexes: [Cp*Ru{(3a,4,5,6,7,7a-eta)-2,3-dihydro-5,6-dialkyl-1H-indene}]OTf (15-Me, alkyl = methyl, 64% yield; 15-Prn, alkyl = n-propyl, 73% yield; 15-Bui, alkyl = 4-methyl-1-pentynyl, 88% yield). In a similar fashion, the room-temperature reaction of 4 with 1-ethynyl-2-(1-propynyl)cyclopentene (11) and [2-(1-propynyl)-1-cyclopenten-1-yl]trimethylsilane (14) leads to the formation of [Cp*Ru{(3a,4,5,6,7,7a-eta)-2,3-dihydro-5-methyl-1H-indene}]OTf (12, 92% yield) and [Cp*Ru{(3a,4,5,6,7,7a-eta)-2,3-dihydro-6-methyl-1H-inden-5-yl)trimethylsilane}]OTf (16, 77% yield), respectively. The bis(TMS)-substituted enediyne (1-cyclopentene-1,2-diyldi-2,1-ethynediyl)bis(trimethylsilane) (9-TMS) and 4 underwent reaction at 100 degrees C to give [Cp*Ru{(3a,4,5,6,7,7a-eta)-2,3-dihydro-1H-inden-5-yl)trimethylsilane}]OTf (10, 69% yield). Deuterium-labeling studies rule out a mechanism that involves a ruthenium-vinylidene intermediate, and provide support for the involvement of a p-benzyne intermediate. In a similar fashion, complex 4 is shown to trigger the cycloaromatization of the conjugated dienyne, 1-ethenyl-2-(1-pentynyl)cyclopentene (19), at room temperature in chloroform-d1 solvent to give [Cp*Ru{(3a,4,5,6,7,7a-eta)-2,3-dihydro-5-(1-propyl)-1H-indene}]OTf (20, 96% yield), with no deuterium enrichment. In the absence of ruthenium the thermal cyclization reactions of unsubstituted acyclic enediynes (Bergman cycloaromatization) and acyclic conjugated dienynes (Hopf cyclization) typically require elevated temperatures (150-250 degrees C). Complexes 10 and 15-Prn were characterized structurally by X-ray crystallography.

Published

2002

18. Functional Profilingof 2-Aminopyrimidine HistamineH4Receptor Modulators.

Author

Mark S. Tichenor, Robin L. Thurmond, Jennifer D. Venable, and Brad M. Savall

Subjects

*PYRIMIDINES, *HISTAMINE receptors, *GASTRIC acid, *ALLERGIES, *NEUROTRANSMITTERS, *LABORATORY rodents

Abstract

Histamine is an important endogenoussignaling molecule that isinvolved in a number of physiological processes including allergicreactions, gastric acid secretion, neurotransmitter release, and inflammation.The biological effects of histamine are mediated by four histaminereceptors with distinct functions and distribution profiles (H1–H4). The most recently discovered histaminereceptor (H4) has emerged as a promising drug target fortreating inflammatory diseases. A detailed understanding of the roleof the H4receptor in human disease remains elusive, inpart because low sequence similarity between the human and rodentH4receptors complicates the translation of preclinicalpharmacology to humans. This review provides an overview of H4drug discovery programs that have studied cross-species structure–activityrelationships, with a focus on the functional profiling of the 2-aminopyrimidinechemotype that has advanced to the clinic for allergy, atopic dermatitis,asthma, and rheumatoid arthritis. [ABSTRACT FROM AUTHOR]

Published

2015