E. O. M. Orlemans scite author profile

E. O. M. Orlemans

5Publications

85Citation Statements Received

28Citation Statements Given

How they've been cited

195

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University of Twente

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Synthesis, mechanism of action, and biological evaluation of mitosenes

Orlemans

Verboom²,

Scheltinga³

et al. 1989

J. Med. Chem.

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Mitosenes of both the pyrrolo- and pyrido[1,2-a]indole type have been prepared via modification of these heterotricyclic compounds. Several mitosenes have been studied for their reactions with nucleophiles under reductive conditions. The results of these experiments show that the biological activity of mitosenes is based on the mechanism of bioreductive activation. When both leaving groups at C-1 and C-10 in the mitosene are the same, the nucleophile preferably adds to C-10 under reductive conditions. All mitosenes were studied for their biological activities in vitro against L1210, WiDr, and A204. On the basis of these results a selection of three mitosenes was made for a more detailed biological evaluation. Several tumor model systems were used, viz. P388, human tumor xenografts, MAC 13, and MAC 16. The results of these studies show that mitosenes have a more limited range of activities than mitomycin C. Surprisingly, the in vivo activities of mitosene diol 8b and mitosene diacetate 10b against the gastric human tumor xenograft GXF 97 were very high and comparable with that of mitomycin C.

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Pharmacological Properties of a New Selective Antiprogestagen: Org 33628

Kloosterboer¹,

Deckers²,

Gooyer³

et al. 1995

Annals of the New York Academy of Sciences

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Clinical trial: evaluation of gastric acid suppression with three doses of immediate‐release esomeprazole in the fixed‐dose combination of PN 400 (naproxen/esomeprazole magnesium) compared with naproxen 500 mg and enteric‐coated esomeprazole 20 mg: a randomized, open‐label, Phase I study in healthy volunteers

Miner

Plachetka²,

Orlemans³

et al. 2010

Aliment Pharmacol Ther

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Synihesis of 3-substituied indoles via a modified madeling reaction

et al. 1987

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responding imines 2a-c,e could be easily synthesized using benzaldehyde in benzene under azeotropic removal of water. Selective reduction of the imines 2 using NaCNEH312 in nmthanolic HCl gave the N-bensylated anilines 3 in gcod overall yields fran 1 (75-86%). Ihe aniline derivatives 3 were converted into the amides 4 usiq different conditions, dependent on the ES. In mDst cases the mnides 4 were formed under acid catalysis (plbsoH). However, when a tert-butyl ester is applied as kW (4b and lib these conditions \*xlld result in the loss of the tert-butyl grcxlp. CH,EWG

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Preclinical evaluation of the Hsp90 inhibitor SNX-5422 in ibrutinib resistant CLL

et al. 2021

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B-cell receptor (BCR) antagonists such as the BTK inhibitor ibrutinib have proven to effectively target chronic lymphocytic leukemia (CLL) tumor cells, leading to impressive response rates in these patients. However patients do still relapse on ibrutinib, and the progressive disease is often quite aggressive requiring immediate treatment. Several strategies are being pursued to treat patients who relapse on ibrutinib therapy. As the most common form of relapse is the development of a mutant form of BTK which limits ibrutinib binding, agents which lead to degradation of the BTK protein are a promising strategy. Our study explores the efficacy of the Hsp90 inhibitor, SNX-5422, in CLL. The SNX Hsp90 inhibitor was effective in primary CLL cells, as well as B-cell lines expressing either BTK wild type or C481 mutant BTK, which has been identified as the primary resistance mechanism to ibrutinib in CLL patients. Furthermore the combination of SNX-5422 and ibrutinib provided a remarkable in vivo survival benefit in the Eμ-TCL1 mouse model of CLL compared to the vehicle or single agent groups (51 day median survival in the vehicle and ibrutinib groups versus 100 day median survival in the combination). We report here preclinical data suggesting that the Hsp90 inhibitor SNX-5422, which has been pursued in clinical trials in both solid tumor and hematological malignancies, is a potential therapy for ibrutinib resistant CLL.

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E. O. M. Orlemans

Synthesis, mechanism of action, and biological evaluation of mitosenes

Pharmacological Properties of a New Selective Antiprogestagen: Org 33628

Synihesis of 3-substituied indoles via a modified madeling reaction

Preclinical evaluation of the Hsp90 inhibitor SNX-5422 in ibrutinib resistant CLL

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