Your search keyword '"MARCH HN"' showing total 11 results

1. Anilinoquinazoline inhibitors of the RET kinase domain-Elaboration of the 7-position.

Author

Jordan AM, Begum H, Fairweather E, Fritzl S, Goldberg K, Hopkins GV, Hamilton NM, Lyons AJ, March HN, Newton R, Small HF, Vishwanath S, Waddell ID, Waszkowycz B, Watson AJ, and Ogilvie DJ

Subjects

Aniline Compounds chemical synthesis, Aniline Compounds chemistry, Dose-Response Relationship, Drug, Humans, Models, Molecular, Molecular Structure, Protein Kinase Inhibitors chemical synthesis, Protein Kinase Inhibitors chemistry, Proto-Oncogene Proteins c-ret metabolism, Quinazolines chemical synthesis, Quinazolines chemistry, Structure-Activity Relationship, Aniline Compounds pharmacology, Protein Kinase Inhibitors pharmacology, Proto-Oncogene Proteins c-ret antagonists & inhibitors, Quinazolines pharmacology

Abstract

We have previously reported a series of anilinoquinazoline derivatives as potent and selective biochemical inhibitors of the RET kinase domain. However, these derivatives displayed diminished cellular potency. Herein we describe further optimisation of the series through modification of their physicochemical properties, delivering improvements in cell potency. However, whilst cellular selectivity against key targets could be maintained, combining cell potency and acceptable pharmacokinetics proved challenging., (Copyright © 2016 Elsevier Ltd. All rights reserved.)

Published

2016

2. Identification of selective inhibitors of RET and comparison with current clinical candidates through development and validation of a robust screening cascade.

Author

Watson AJ, Hopkins GV, Hitchin S, Begum H, Jones S, Jordan A, Holt S, March HN, Newton R, Small H, Stowell A, Waddell ID, Waszkowycz B, and Ogilvie DJ

Abstract

RET (REarranged during Transfection) is a receptor tyrosine kinase, which plays pivotal roles in regulating cell survival, differentiation, proliferation, migration and chemotaxis. Activation of RET is a mechanism of oncogenesis in medullary thyroid carcinomas where both germline and sporadic activating somatic mutations are prevalent. At present, there are no known specific RET inhibitors in clinical development, although many potent inhibitors of RET have been opportunistically identified through selectivity profiling of compounds initially designed to target other tyrosine kinases. Vandetanib and cabozantinib, both multi-kinase inhibitors with RET activity, are approved for use in medullary thyroid carcinoma, but additional pharmacological activities, most notably inhibition of vascular endothelial growth factor - VEGFR2 (KDR), lead to dose-limiting toxicity. The recent identification of RET fusions present in ~1% of lung adenocarcinoma patients has renewed interest in the identification and development of more selective RET inhibitors lacking the toxicities associated with the current treatments. In an earlier publication [Newton et al, 2016; 1] we reported the discovery of a series of 2-substituted phenol quinazolines as potent and selective RET kinase inhibitors. Here we describe the development of the robust screening cascade which allowed the identification and advancement of this chemical series.  Furthermore we have profiled a panel of RET-active clinical compounds both to validate the cascade and to confirm that none display a RET-selective target profile.

Published

2016

3. Identification of selective inhibitors of RET and comparison with current clinical candidates through development and validation of a robust screening cascade.

Author

Watson AJ, Hopkins GV, Hitchin S, Begum H, Jones S, Jordan A, Holt S, March HN, Newton R, Small H, Stowell A, Waddell ID, Waszkowycz B, and Ogilvie DJ

Abstract

RET (REarranged during Transfection) is a receptor tyrosine kinase, which plays pivotal roles in regulating cell survival, differentiation, proliferation, migration and chemotaxis. Activation of RET is a mechanism of oncogenesis in medullary thyroid carcinomas where both germline and sporadic activating somatic mutations are prevalent. At present, there are no known specific RET inhibitors in clinical development, although many potent inhibitors of RET have been opportunistically identified through selectivity profiling of compounds initially designed to target other tyrosine kinases. Vandetanib and cabozantinib, both multi-kinase inhibitors with RET activity, are approved for use in medullary thyroid carcinoma, but additional pharmacological activities, most notably inhibition of vascular endothelial growth factor - VEGFR2 (KDR), lead to dose-limiting toxicity. The recent identification of RET fusions present in ~1% of lung adenocarcinoma patients has renewed interest in the identification and development of more selective RET inhibitors lacking the toxicities associated with the current treatments. In an earlier publication [Newton et al, 2016; 1] we reported the discovery of a series of 2-substituted phenol quinazolines as potent and selective RET kinase inhibitors. Here we describe the development of the robust screening cascade which allowed the identification and advancement of this chemical series.  Furthermore we have profiled a panel of RET-active clinical compounds both to validate the cascade and to confirm that none display a RET-selective target profile., Competing Interests: There are no competing financial interests to declare.

Published

2016

4. Nuclear receptor binding protein 1 regulates intestinal progenitor cell homeostasis and tumour formation.

Author

Wilson CH, Crombie C, van der Weyden L, Poulogiannis G, Rust AG, Pardo M, Gracia T, Yu L, Choudhary J, Poulin GB, McIntyre RE, Winton DJ, March HN, Arends MJ, Fraser AG, and Adams DJ

Subjects

Animals, Carrier Proteins analysis, Cell Differentiation genetics, Cell Differentiation physiology, Cell Proliferation, Cell Transformation, Neoplastic genetics, Cell Transformation, Neoplastic metabolism, DNA-Binding Proteins analysis, Female, Gene Deletion, Humans, Intestines cytology, Intracellular Signaling Peptides and Proteins genetics, Male, Mice, Neoplasms genetics, Neoplasms metabolism, Neoplasms pathology, Oxidoreductases, Prognosis, Receptors, Cytoplasmic and Nuclear genetics, Stem Cells cytology, Transcription Factors analysis, Tumor Suppressor Proteins physiology, Ubiquitination genetics, Ubiquitination physiology, Vesicular Transport Proteins genetics, Homeostasis physiology, Intestines physiology, Intracellular Signaling Peptides and Proteins physiology, Receptors, Cytoplasmic and Nuclear physiology, Stem Cells physiology, Tumor Suppressor Proteins genetics, Vesicular Transport Proteins physiology

Abstract

Genetic screens in simple model organisms have identified many of the key components of the conserved signal transduction pathways that are oncogenic when misregulated. Here, we identify H37N21.1 as a gene that regulates vulval induction in let-60(n1046gf), a strain with a gain-of-function mutation in the Caenorhabditis elegans Ras orthologue, and show that somatic deletion of Nrbp1, the mouse orthologue of this gene, results in an intestinal progenitor cell phenotype that leads to profound changes in the proliferation and differentiation of all intestinal cell lineages. We show that Nrbp1 interacts with key components of the ubiquitination machinery and that loss of Nrbp1 in the intestine results in the accumulation of Sall4, a key mediator of stem cell fate, and of Tsc22d2. We also reveal that somatic loss of Nrbp1 results in tumourigenesis, with haematological and intestinal tumours predominating, and that nuclear receptor binding protein 1 (NRBP1) is downregulated in a range of human tumours, where low expression correlates with a poor prognosis. Thus NRBP1 is a conserved regulator of cell fate, that plays an important role in tumour suppression.

Published

2012

5. Insertional mutagenesis identifies multiple networks of cooperating genes driving intestinal tumorigenesis.

Author

March HN, Rust AG, Wright NA, ten Hoeve J, de Ridder J, Eldridge M, van der Weyden L, Berns A, Gadiot J, Uren A, Kemp R, Arends MJ, Wessels LF, Winton DJ, and Adams DJ

Subjects

Adenomatous Polyposis Coli Protein genetics, Animals, Cell Transformation, Neoplastic metabolism, Genes, Neoplasm, Humans, Intestinal Neoplasms metabolism, Intracellular Signaling Peptides and Proteins genetics, Kaplan-Meier Estimate, Mice, Mice, Transgenic, Models, Genetic, Monte Carlo Method, Signal Transduction, Transposases, Tumor Burden, beta Catenin metabolism, Cell Transformation, Neoplastic genetics, Epistasis, Genetic, Intestinal Neoplasms genetics, Mutagenesis, Insertional

Abstract

The evolution of colorectal cancer suggests the involvement of many genes. To identify new drivers of intestinal cancer, we performed insertional mutagenesis using the Sleeping Beauty transposon system in mice carrying germline or somatic Apc mutations. By analyzing common insertion sites (CISs) isolated from 446 tumors, we identified many hundreds of candidate cancer drivers. Comparison to human data sets suggested that 234 CIS-targeted genes are also dysregulated in human colorectal cancers. In addition, we found 183 CIS-containing genes that are candidate Wnt targets and showed that 20 CISs-containing genes are newly discovered modifiers of canonical Wnt signaling. We also identified mutations associated with a subset of tumors containing an expanded number of Paneth cells, a hallmark of deregulated Wnt signaling, and genes associated with more severe dysplasia included those encoding members of the FGF signaling cascade. Some 70 genes had co-occurrence of CIS pairs, clustering into 38 sub-networks that may regulate tumor development.

Published

2011

6. mTOR regulation by JNK: rescuing the starving intestinal cancer cell?

Author

March HN and Winton DJ

Subjects

Animals, Female, Humans, Intestinal Neoplasms metabolism, JNK Mitogen-Activated Protein Kinases genetics, Male, TOR Serine-Threonine Kinases metabolism, DNA, Neoplasm genetics, Gene Expression Regulation, Neoplastic, Intestinal Neoplasms genetics, JNK Mitogen-Activated Protein Kinases metabolism, TOR Serine-Threonine Kinases genetics

Published

2011

7. ERK1/2, but not ERK5, is necessary and sufficient for phosphorylation and activation of c-Fos.

Author

Gilley R, March HN, and Cook SJ

Subjects

Animals, Cell Line, Cell Nucleus drug effects, Cell Nucleus metabolism, Enzyme Activation drug effects, Epidermal Growth Factor pharmacology, Humans, JNK Mitogen-Activated Protein Kinases metabolism, Mice, Mitogen-Activated Protein Kinase 1 antagonists & inhibitors, Mitogen-Activated Protein Kinase 3 antagonists & inhibitors, Phosphorylation drug effects, Protein Kinase Inhibitors pharmacology, Protein Structure, Tertiary, Protein Transport drug effects, Proto-Oncogene Proteins c-fos chemistry, Proto-Oncogene Proteins c-fos metabolism, Transcription Factor AP-1 metabolism, Transcriptional Activation drug effects, p38 Mitogen-Activated Protein Kinases metabolism, Mitogen-Activated Protein Kinase 1 metabolism, Mitogen-Activated Protein Kinase 3 metabolism, Mitogen-Activated Protein Kinase 7 metabolism, Proto-Oncogene Proteins c-fos genetics, Transcriptional Activation genetics

Abstract

Growth factor-stimulated expression and activation of c-Fos is regulated by the ERK1/2 pathway. However, recent reports have also suggested a prominent role for the closely related ERK5 pathway in regulating the expression, transcriptional activation and nuclear localization of c-Fos. Here we have compared the role of ERK1/2 and ERK5 in regulating c-Fos using a combination of conditional protein kinases, selective biochemical inhibitors and ERK5 null fibroblasts. We demonstrate that activation of the ERK1/2 pathway, but not ERK5, is sufficient for c-Fos phosphorylation and transcriptional activation. Furthermore, growth factor-dependent expression of c-Fos is blocked by low doses of PD184352 that selectively inhibit the ERK1/2 pathway but proceeds normally in ERK5-/- 3T9 cells; in addition, nuclear localization of c-Fos is normal in ERK5-/- cells. ERK5-/- cells are, however, defective for c-Jun expression but this is reversed by re-expression of ERK5. In addition to ERK5, neither the JNK nor p38 pathways can substitute for ERK1/2 in the regulation of c-Fos transcriptional activity. These results demonstrate that c-Fos transcriptional activity is not regulated by the ERK5 pathway; rather, of all the MAPKs and SAPKs, c-Fos activation appears to be predominantly linked to the ERK1/2 pathway.

Published

2009

8. The duration of ERK1/2 activity determines the activation of c-Fos and Fra-1 and the composition and quantitative transcriptional output of AP-1.

Author

Chalmers CJ, Gilley R, March HN, Balmanno K, and Cook SJ

Subjects

Cell Line, DNA metabolism, Enzyme Activation drug effects, Fibroblasts drug effects, Fibroblasts enzymology, JNK Mitogen-Activated Protein Kinases metabolism, Protein Binding drug effects, Protein Structure, Tertiary drug effects, Protein Transport drug effects, Proto-Oncogene Proteins c-fos genetics, Proto-Oncogene Proteins c-jun metabolism, Receptor, PAR-1 metabolism, Thrombin pharmacology, Time Factors, Transcriptional Activation drug effects, p38 Mitogen-Activated Protein Kinases metabolism, Mitogen-Activated Protein Kinase 1 metabolism, Mitogen-Activated Protein Kinase 3 metabolism, Proto-Oncogene Proteins c-fos metabolism, Transcription Factor AP-1 genetics, Transcription, Genetic drug effects

Abstract

The duration of ERK1/2 activation influences the nature of the biological response to agonist. Members of the AP-1 transcription factor family are well known targets of the ERK1/2 pathway and are expressed in a temporally coordinated fashion during cell cycle re-entry. In CCl39 fibroblasts, sustained ERK1/2 activation is required for the expression of Fra-1, Fra-2, c-Jun and JunB, whereas expression of c-Fos is still strongly induced even in response to transient ERK activation. However, the significance of this pattern of expression for AP-1 activity has not been addressed. Here we show that growth factor stimulated activation of the C-terminal c-Fos transactivation domain (TAD) serves as a sensor for ERK1/2 signal duration whereas the c-JunTAD is not responsive to growth factors. In addition, sustained ERK1/2 activation determines the duration of increases in AP-1 DNA binding complexes as well as their qualitative make up. Finally, this is reflected in both the duration and quantitative transcriptional output of stably integrated AP-1 reporter constructs, indicating that AP-1 activity is finely tuned to ERK1/2 signal duration. These results provide new insights into the importance of ERK1/2 signal duration in the regulation of AP-1 and provide an explanation for how differences in signal duration can lead to both quantitative and qualitative changes in gene expression.

Published

2007

9. Action of cortisone and prednisone on elephantiasis.

Author

LAIGRET J, MARCH HN, and KESSEL JF

Subjects

Humans, Cortisone therapeutic use, Filariasis therapy

Published

1957

10. Reduction in the prevalence of clinical filariasis in Tahiti following adoption of a control program.

Author

MARCH HN, LAIGRET J, KESSEL JF, and BAMBRIDGE B

Subjects

Humans, Polynesia, Prevalence, Biomedical Research, Filariasis prevention & control

Published

1960

11. The effect of cortisone and prednisone on bullous reactions following treatment of filariasis with diethylcarbamazine.

Author

MARCH HN and LAIGRET J

Subjects

Humans, Anthelmintics adverse effects, Blister etiology, Cortisone therapeutic use, Diethylcarbamazine, Filariasis therapy, Prednisone therapeutic use

Published

1958