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Dive into the research topics where Bert Nolte is active.

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Featured researches published by Bert Nolte.


Molecular Pharmaceutics | 2017

Quantitative Assessment of Drug Delivery to Tissues and Association with Phospholipidosis: A Case Study with Two Structurally Related Diamines in Development

Irena Loryan; Edmund Hoppe; Klaus Hansen; Felix Held; Achim Kless; Klaus Linz; Virginia Marossek; Bert Nolte; Paul Ratcliffe; Derek Saunders; Rolf Terlinden; Anita Wegert; André Welbers; Olaf Will; Margareta Hammarlund-Udenaes

Drug induced phospholipidosis (PLD) may be observed in the preclinical phase of drug development and pose strategic questions. As lysosomes have a central role in pathogenesis of PLD, assessment of lysosomal concentrations is important for understanding the pharmacokinetic basis of PLD manifestation and forecast of potential clinical appearance. Herein we present a systematic approach to provide insight into tissue-specific PLD by evaluation of unbound intracellular and lysosomal (reflecting acidic organelles) concentrations of two structurally related diprotic amines, GRT1 and GRT2. Their intratissue distribution was assessed using brain and lung slice assays. GRT1 induced PLD both in vitro and in vivo. GRT1 showed a high intracellular accumulation that was more pronounced in the lung, but did not cause cerebral PLD due to its effective efflux at the blood-brain barrier. Compared to GRT1, GRT2 revealed higher interstitial fluid concentrations in lung and brain, but more than 30-fold lower lysosomal trapping capacity. No signs of PLD were seen with GRT2. The different profile of GRT2 relative to GRT1 is due to a structural change resulting in a reduced basicity of one amino group. Hence, by distinct chemical modifications, undesired lysosomal trapping can be separated from desired drug delivery into different organs. In summary, assessment of intracellular unbound concentrations was instrumental in delineating the intercompound and intertissue differences in PLD induction in vivo and could be applied for identification of potential lysosomotropic compounds in drug development.


Archive | 2009

Substituted spirocyclic cyclohexane derivatives

Saskia Zemolka; Bert Nolte; Sven Frormann; Claudia Hinze; Klaus Linz; Wolfgang Schröder; Werner Englberger; Hans Schick; Helmut Dr. Sonnenschein


Archive | 2009

Substituted 4-aminocyclohexane derivatives

Bert Nolte; Wolfgang Schröder; Klaus Linz; Werner Englberger; Hans Schick; Heinz Graubaum; Birgit Roloff; Sigrid Ozegowski; József Bálint; Helmut Dr. Sonnenschein


Archive | 2011

Cis-tetrahydro-spiro(cyclohexane-1,1'-pyrido[3,4-b]indole)-4-amine Compounds

Klaus Linz; Saskia Zemolka; Bert Nolte; Stefan Schunk; Hans Schick


Archive | 2009

(hetero-)aryl cyclohexane derivatives

Saskia Zemolka; Stefan Schunk; Bert Nolte; Klaus Linz; Wolfgang Schröder; Werner Englberger; Hans Schick; Helmut Sonnenschein; Birgitta Henkel; József Bálint


Archive | 2011

Cis-tetrahydro-spiro(cyclohexan-1,1'-pyrido[3,4-b]indol)-4-amine derivatives

Klaus Linz; Saskia Zemolka; Bert Nolte; Stefan Schunk; Hans Schick


Archive | 2013

DERIVADOS DE AMINA CIS-TETRAHIDRO-ESPIRO(CICLOHEXAN-1,1'-PIRIDO[3,4-B]INDOL)-4

Stefan Schunk; Klaus Linz; Saskia Zemolka; Bert Nolte; Hans Schick


Archive | 2011

Derivatives of cis-tetrahydro-spiro (cyclohexane-1,1'-pyrido [3,4-b] indole) -4-amine

Klaus Linz; Saskia Zemolka; Bert Nolte; Stefan Schunk; Hans Schick


Archive | 2009

Dérivés de cyclohexane spirocycliques substitués

Saskia Zemolka; Bert Nolte; Sven Frormann; Claudia Hinze; Klaus Linz; Wolfgang Schröder; Werner Englberger; Hans Schick; Helmut Sonnenschein


Archive | 2009

(hetero-)aryl-cyclohexan-derivate

Saskia Zemolka; Stefan Schunk; Bert Nolte; Klaus Linz; Wolfgang Schröder; Werner Englberger; Hans Schick; Helmut Sonnenschein; Birgitta Henkel; József Bálint

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Helmut Sonnenschein

Bundesanstalt für Materialforschung und -prüfung

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