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Dive into the research topics where Juan-Miguel Jimenez is active.

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Featured researches published by Juan-Miguel Jimenez.


Journal of Medicinal Chemistry | 2011

Discovery and structure-activity relationship of 3-aminopyrid-2-ones as potent and selective interleukin-2 inducible T-cell kinase (Itk) inhibitors

Jean-Damien Charrier; Andrew H. Miller; David Kay; Guy Brenchley; Heather Twin; Philip N. Collier; Sharn Ramaya; Shazia B. Keily; Steven Durrant; Ronald Knegtel; Adam Tanner; Kieron Brown; Adam Curnock; Juan-Miguel Jimenez

Interleukin-2 inducible T-cell kinase (Itk) plays a role in T-cell functions, and its inhibition potentially represents an attractive intervention point to treat autoimmune and allergic diseases. Herein we describe the discovery of a series of potent and selective novel inhibitors of Itk. These inhibitors were identified by structure-based design, starting from a fragment generated de novo, the 3-aminopyrid-2-one motif. Functionalization of the 3-amino group enabled rapid enhancement of the inhibitory activity against Itk, while introduction of a substituted heteroaromatic ring in position 5 of the pyridone fragment was key to achieving optimal selectivity over related kinases. A careful analysis of the hydration patterns in the kinase active site was necessary to fully explain the observed selectivity profile. The best molecule prepared in this optimization campaign, 7v, inhibits Itk with a K(i) of 7 nM and has a good selectivity profile across kinases.


Journal of Medicinal Chemistry | 2013

Design and Optimization of Selective Protein Kinase C θ (PKCθ) Inhibitors for the Treatment of Autoimmune Diseases

Juan-Miguel Jimenez; Dean Boyall; Guy Brenchley; Philip N. Collier; Christopher John Davis; Damien Fraysse; Shazia B. Keily; Jaclyn L. Henderson; Andrew H. Miller; Francoise Pierard; Luca Settimo; Heather Twin; Claire M. Bolton; Adam Curnock; Peter J.S. Chiu; Adam Tanner; Stephen Young

Protein kinase C θ (PKCθ) has a central role in T cell activation and survival; however, the dependency of T cell responses to the inhibition of this enzyme appears to be dictated by the nature of the antigen and by the inflammatory environment. Studies in PKCθ-deficient mice have demonstrated that while antiviral responses are PKCθ-independent, T cell responses associated with autoimmune diseases are PKCθ-dependent. Thus, potent and selective inhibition of PKCθ is expected to block autoimmune T cell responses without compromising antiviral immunity. Herein, we describe the development of potent and selective PKCθ inhibitors, which show exceptional potency in cells and in vivo. By use of a structure based rational design approach, a 1000-fold improvement in potency and 76-fold improvement in selectivity over closely related PKC isoforms such as PKCδ were obtained from the initial HTS hit, together with a big improvement in lipophilic efficiency (LiPE).


Bioorganic & Medicinal Chemistry Letters | 2012

Structure-based optimization of aminopyridines as PKCθ inhibitors

Juan-Miguel Jimenez; Christopher John Davis; Dean Boyall; Damien Fraysse; Ronald Knegtel; Luca Settimo; Stephen Young; Claire M. Bolton; Peter Chiu; Adam Curnock; Richele Rasmussen; Adam Tanner; Ian Ager

The identification of a novel series of PKCθ inhibitors and subsequent optimization using docking based on a crystal structure of PKCθ is described. SAR was rapidly generated around an amino pyridine-ketone hit; (6-aminopyridin-2-yl)(2-aminopyridin-3-yl)methanone 2 leading to compound 21 which significantly inhibits production of IL-2 in a mouse SEB-IL2 model.


Bioorganic & Medicinal Chemistry Letters | 2001

Naphthalene derivatives: A new series of selective cyclooxygenase-2 inhibitors.

Joan Feixas; Juan-Miguel Jimenez; Nuria Godessart; Carles Puig; Lidia Soca; Marı́a I Crespo

A new series of potent and selective cyclooxygenase-2 inhibitors have been prepared. Some of these compounds show good oral anti-inflammatory activity in rats.


Bioorganic & Medicinal Chemistry Letters | 2014

Strategies for the modulation of phase II metabolism in a series of PKCε inhibitors.

Jeremy Clemens; Timothy Coon; Brett Bradley Busch; Juliana L. Asgian; Sarah Hudson; Andreas P. Termin; Tina B. Flores; Dao Tran; Peggy Chiang; Sam Sperry; Ray Gross; Jeffrey Abt; Roger Heim; Sandra Lechner; Heather Twin; John Studley; Guy Brenchley; Philip N. Collier; Francoise Pierard; Andrew Miller; Chau Mak; Vadims Dvornikovs; Juan-Miguel Jimenez; Dean Stamos

Extensive phase II metabolism of an advanced PKCε inhibitor resulted in sub-optimal pharmacokinetics in rat marked by elevated clearance. Synthesis of the O-glucuronide metabolite as a standard was followed by three distinct strategies to specifically temper phase II metabolic degradation of the parent molecule. In this study, it was determined that the introduction of proximal polarity to the primary alcohol generally curbed O-glucuronidation and improved PK and physical chemical properties while maintaining potency against the target. Utilization of a Jacobsen hydrolytic kinetic resolution to obtain optically enriched final compounds is also discussed.


Archive | 2004

Compositions useful as inhibitors of protein kinases

Juan-Miguel Jimenez; Jeremy Green; Huai Gao; Young-Choon Moon; Guy Brenchley; Ronald Knegtel; Francoise Pierard


Archive | 2005

Pyrazolo[1,5-a]pyrimidines useful as inhibitors of protein kinases

Ronald Knegtel; Juan-Miguel Jimenez; Jean-Damien Charrier; Dean Stamos; Pan Li; Jon H. Come; Alex Aronov


Archive | 2005

Azaindoles useful as inhibitors of protein kinases

Francoise Pierard; Juan-Miguel Jimenez; Ronald Kengtel; Guy Brenchley; Michael Mortimore; Francesca Mazzei


Archive | 2008

Aminopyrimidines useful as inhibitors of protein kinases

Juan-Miguel Jimenez; Andrew Miller; Jeremy Green; Huai Gao; Gregory Henkel; Michael Liu; Timothy Neuberger


Archive | 2005

Pyrid-2-ones useful as inhibitors of tec family protein kinases for the treatment of inflammatory, proliferative and immunologically-mediated diseases

Jean-Damien Charrier; Steven Durrant; Sharn Ramaya; Juan-Miguel Jimenez; Alistair Rutherford

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Dean Boyall

Vertex Pharmaceuticals

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