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Dive into the research topics where Juliette Janson is active.

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Featured researches published by Juliette Janson.


PLOS Genetics | 2008

An Ancient Duplication of Exon 5 in the Snap25 Gene Is Required for Complex Neuronal Development/Function

Jenny U. Johansson; Jesper Ericsson; Juliette Janson; Simret Beraki; Davor Stanic; Slavena A. Mandic; Martin A. Wikström; Tomas Hökfelt; Sven Ove Ögren; Björn Rozell; Per-Olof Berggren; Christina Bark

Alternative splicing is an evolutionary innovation to create functionally diverse proteins from a limited number of genes. SNAP-25 plays a central role in neuroexocytosis by bridging synaptic vesicles to the plasma membrane during regulated exocytosis. The SNAP-25 polypeptide is encoded by a single copy gene, but in higher vertebrates a duplication of exon 5 has resulted in two mutually exclusive splice variants, SNAP-25a and SNAP-25b. To address a potential physiological difference between the two SNAP-25 proteins, we generated gene targeted SNAP-25b deficient mouse mutants by replacing the SNAP-25b specific exon with a second SNAP-25a equivalent. Elimination of SNAP-25b expression resulted in developmental defects, spontaneous seizures, and impaired short-term synaptic plasticity. In adult mutants, morphological changes in hippocampus and drastically altered neuropeptide expression were accompanied by severe impairment of spatial learning. We conclude that the ancient exon duplication in the Snap25 gene provides additional SNAP-25-function required for complex neuronal processes in higher eukaryotes.


Current Drug Metabolism | 2016

Optimizing DMPK Properties: Experiences from a Big Pharma DMPK Department

Anna-Karin Sohlenius-Sternbeck; Juliette Janson; Johan Bylund; Pawel Baranczewski; Anna Breitholtz-Emanuelsson; Yin Hu; Carrie Tsoi; Anders E. G. Lindgren; Olle Gissberg; Tjerk Bueters; Sveinn Briem; Sanja Juric; Jenny U. Johansson; Margareta Bergh; Janet Hoogstraate

BACKGROUND The disposition of a drug is dependent on interactions between the body and the drug, its molecular properties and the physical and biological barriers presented in the body. In order for a drug to have a desired pharmacological effect it has to have the right properties to be able to reach the target site in sufficient concentration. This review details how drug metabolism and pharmacokinetics (DMPK) and physicochemical deliveries played an important role in data interpretation and compound optimization at AstraZeneca R&D in Södertälje, Sweden. METHODS A selection of assays central in the evaluation of the DMPK properties of new chemical entities is presented, with guidance and consideration on assay outcome interpretation. Early in projects, solubility, LogD, permeability and metabolic stability were measured to support effective optimization of DMPK properties. Changes made to facilitate high throughput, efficient bioanalysis and the handling of large amounts of samples are described. Already early in drug discovery, we used an integrated approach for the prediction of the fate of drugs in human (early dose to man) based on data obtained from in vitro experiments. The early dose to man was refined with project progression, which triggered more intricate assays and experiments. At later stages, preclinical in vivo pharmacokinetic (PK) data was integrated with pharmacodynamics (PD) to allow predictions of required dose, dose intervals and exposure profile to achieve the desired effect in man. RESULTS AND CONCLUSIONS A well-defined work flow of DMPK activities from early lead identification up to the selection of a candidate drug was developed. This resulted in a cost effective and efficient optimization of chemical series, and facilitated informed decision making throughout project progress.


Diabetes | 2003

β-Cell Deficit and Increased β-Cell Apoptosis in Humans With Type 2 Diabetes

Alexandra E. Butler; Juliette Janson; Susan Bonner-Weir; Robert A. Ritzel; Robert A. Rizza; Peter C. Butler


Diabetes | 1999

The mechanism of islet amyloid polypeptide toxicity is membrane disruption by intermediate-sized toxic amyloid particles.

Juliette Janson; Richard H. Ashley; David G. Harrison; Susan McIntyre; Peter C. Butler


Diabetes | 2003

Increased β-cell apoptosis prevents adaptive increase in β-cell mass in mouse model of type 2 diabetes: Evidence for role of islet amyloid formation rather than direct action of amyloid

Alexandra E. Butler; Juliette Janson; Walter C. Soeller; Peter C. Butler


Proceedings of the National Academy of Sciences of the United States of America | 1996

Spontaneous diabetes mellitus in transgenic mice expressing human islet amyloid polypeptide

Juliette Janson; W C Soeller; Patrick C. Roche; R T Nelson; A J Torchia; D K Kreutter; P C Butler


Diabetes | 1998

Islet amyloid-associated diabetes in obese A(vy)/a mice expressing human islet amyloid polypeptide.

Walter C. Soeller; Juliette Janson; Susan Emeigh Hart; Janice C. Parker; Maynard D. Carty; Ralph W. Stevenson; David K. Kreutter; Peter C. Butler


Diabetes | 2006

Tomosyn Is Expressed in β-Cells and Negatively Regulates Insulin Exocytosis

Wei Zhang; Lena Lilja; Slavena A. Mandic; Jesper Gromada; Kamille Smidt; Juliette Janson; Yoshimi Takai; Christina Bark; Per-Olof Berggren; Björn Meister


Proceedings of the National Academy of Sciences of the United States of America | 2005

Neuronal calcium sensor-1 potentiates glucose-dependent exocytosis in pancreatic β cells through activation of phosphatidylinositol 4-kinase β

Jesper Gromada; Christina Bark; Kamille Smidt; Alexander M. Efanov; Juliette Janson; Slavena A. Mandic; Dominic-Luc Webb; Wei Zhang; Björn Meister; Andreas Jeromin; Per-Olof Berggren


Archive | 2012

Discovery of AZD3839, a Potent and Selective BACE1 Inhibitor Clinical Candidate for the Treatment of Alzheimer

Fredrik Jeppsson; Juliette Janson; Susanne Gustavsson; Lise-Lotte Olsson; Bart Ploeger; Gvido Cebers; Karin Kolmodin; Britt-Marie Swahn; Stefan Berg; Tjerk Bueters; Johanna Fälting

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Jenny U. Johansson

Karolinska University Hospital

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