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Dive into the research topics where Gerald Bacher is active.

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Featured researches published by Gerald Bacher.


Cancer Research | 2009

Indibulin, a Novel Microtubule Inhibitor, Discriminates between Mature Neuronal and Nonneuronal Tubulin

Anke Wienecke; Gerald Bacher

Microtubule inhibitors interfere with microtubule dynamics, causing cell cycle arrest and apoptosis. These effects are responsible for the chemotherapeutic activities of members of the taxane and Vinca alkaloid families in oncology. Unfortunately, a major side effect of the taxanes and Vinca alkaloids is the development of peripheral neuropathies. Indibulin (N-[pyridin-4-yl]-[1-(4-chlorbenzyl)-indol-3-yl]-glyoxyl-amid; D-24851; ZIO-301), a novel synthetic small molecule microtubule inhibitor, destabilizes microtubules and has antitumor activity but does not exhibit neurotoxicity in preclinical animal studies. In the present study, it has been found that indibulin is able to discriminate between highly posttranslationally modified tubulin present in mature neuronal microtubules, and less-modified tubulin present in immature neuronal or nonneuronal microtubules. Vincristine and colchicine act on either tubulin equally well. The binding site of indibulin on mature neuronal microtubules seems to be inaccessible due to the posttranslational modifications, a theory that is supported by the observation that indibulin did not disrupt the integrity of highly modified microtubules present in neurites of pheochromocytoma (PC12) cells. The specificity of indibulin for unmodified microtubules seems to be dependent on the pyridyl moiety of indibulin because derivatives that have the pyridyl moiety replaced are not able to discriminate between highly and less-modified tubulins. The observed broad antitumor activity of indibulin and the lack of central and peripheral nervous system toxicity in preclinical studies make it a promising candidate for development as a cancer treatment. Indibulin is currently in phase I clinical trials.


Cancer Research | 2001

D-24851, a Novel Synthetic Microtubule Inhibitor, Exerts Curative Antitumoral Activity in Vivo, Shows Efficacy toward Multidrug-resistant Tumor Cells, and Lacks Neurotoxicity

Gerald Bacher; Bernd Nickel; Peter Emig; Udo Vanhoefer; Siegfried Seeber; Alexei Shandra; Thomas Klenner; Thomas Dr. Beckers


Molecular Pharmacology | 2001

Differential Roles of p21 Waf1 and p27 Kip1 in Modulating Chemosensitivity and Their Possible Application in Drug Discovery Studies

Mathias Schmidt; Yang Lu; John M. Parant; Guillermina Lozano; Gerald Bacher; Thomas Dr. Beckers; Zhen Fan


Archive | 2003

Indolyl-3-glyoxylic acid derivatives having therapeutically valuable properties

Bernd Nickel; Gerald Bacher; Thomas Klenner; Thomas Beckers; Peter Emig; Jurgen Engel; Erik Bruyneel; Günter Kamp; Kirsten Peters


Archive | 2000

Indolyl-3-glyoxylic acid derivatives serving as antitumor agents

Bernd Nickel; Thomas Klenner; Gerald Bacher; Thomas Beckers; Peter Emig; Juergen Engel; Erik Bruyneel; Guenter Kamp; Kirsten Peters


Archive | 2000

Substituted N-benzylindol-3-ylglyoxylic acid derivatives having antitumor action

Eckhard Günther; Peter Emig; Dietmar Reichert; Guillaume Le Baut; Bernd Nickel; Gerald Bacher


Archive | 2001

Novel indole derivatives and their use as medicament

Peter Emig; Gerald Bacher; Dietmar Reichert; Silke Basner; Beate Aue; Bernd Nickel; Eckhard Günther


Archive | 2000

Substituted n-benzyl-indol-3-yl glyoxylic acid derivatives having an anti-tumoral effect

Gerald Bacher; Le Guillaume Baut; Peter Emig; Eckhard Guenther; Bernd Nickel; Dietmar Reichert


Archive | 2001

Novel heteroaryl derivatives and the use thereof as pharmaceuticals

Peter Emig; Eckhard Günther; Silke Baasner; Gerald Bacher; Thomas Beckers; Beate Aue; Bernd Nickel


Archive | 2001

Indole derivatives and their use as medicaments

Peter Emig; Gerald Bacher; Dietmar Reichert; Silke Basner; Beate Aue; Bernd Nickel; Eckhard Günther

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Thomas Beckers

Goethe University Frankfurt

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Thomas Dr. Beckers

Takeda Pharmaceutical Company

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Guillermina Lozano

University of Texas MD Anderson Cancer Center

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John M. Parant

University of Alabama at Birmingham

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Mathias Schmidt

University of Texas MD Anderson Cancer Center

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