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Dive into the research topics where Maxwell Sehested is active.

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Featured researches published by Maxwell Sehested.


Biochemical Pharmacology | 1993

Different modes of anthracycline interaction with topoisomerase II. Separate structures critical for DNA-cleavage, and for overcoming topoisomerase II-related drug resistance.

Peter Buhl Jensen; Boe Sandahl Sorensen; Maxwell Sehested; Erland J.F. Demant; Eigil Kjeldsen; Ellen Friche; Heine H. Hansen

In contrast to the classic anthracyclines (doxorubicin and daunorubicin), aclarubicin (ACLA) does not stimulate topoisomerase II (topo II) mediated DNA-cleavage. This distinction may be important with respect to topo II-related drug resistance, and the aim of this study was to clarify drug-structures responsible for this difference. Various ACLA analogs were tested for: (a) interaction with purified topo II, (b) induction of DNA cleavage in cells, (c) cellular uptake and (d) cytotoxicity. A remarkable distinction was seen between analogs containing the chromophore aklavinone (AKV) (e.g. ACLA) which have a carboxymethyl group (COOCH3) at C-10 and drugs with a beta-rhodomycinone (RMN) chromophore with hydroxyl groups at C-10 and at C-11. Thus, RMN-containing analogs, including the aglycone RMN itself, effectively stimulated topo II-mediated DNA cleavage. In contrast, AKV-containing drugs inhibited DNA cleavage and antagonized cytotoxicity mediated by RMN-containing drugs. In OC-NYH/VM cells, exhibiting multidrug resistance due to an altered topo II phenotype (at-MDR), cross-resistance was only seen to the RMN-containing drugs whereas no cross-resistance was seen to the non-DNA cleaving AKV-containing compounds. Thus, our data show that one domain in the anthracycline is of particular importance for the interaction with topo II, namely the positions C-10 and C-11 in the chromophore, and further that at-MDR was circumvented by a COOCH3 substitution at position C-10. These findings may provide guidance for the synthesis and development of new analogs with activity in at-MDR cells.


Archive | 2011

METHOD FOR PREDICTING THE UTILITY OF ADMINISTERING NICOTINIC ACID OR A PRECURSOR OR PRODRUG THEREOF TO REDUCE THE SEVERITY OF SIDE-EFFECTS OF CANCER TREATMENT WITH NICOTINAMIDE PHOSPHORIBOSYLTRANSFERASE INHIBITORS

Uffe Olesen; Annemette V. Thougaard; Maxwell Sehested


Archive | 2009

Methods of Treatment Employing Prolonged Continuous Infusion of Belinostat

Maxwell Sehested; Peter Buhl Jensen; Nis I. Nissen


Archive | 1997

Topoisomerase II poison and bis-dioxopiperazine derivative combination therapy

Peter Buhl Jensen; Maxwell Sehested


Archive | 2000

Treatment of accidental extravasation of anthracyclines

Seppo W. Langer; Peter Buhl Jensen; Maxwell Sehested


Archive | 2005

Cancer treatment with topoisomerase-ii inhibitor, a bis-dioxypiperazine and radiation

Kenneth Francis Hofland; Maxwell Sehested; Paul E.G. Kristjansen; Annemette V. Thougaard; Peter Buhl Jensen


Archive | 2012

NOVEL METHOD OF TREATMENT

Uffe Olesen; Annemette V. Thougaard; Maxwell Sehested


Archive | 2005

Traitement contre le cancer au moyen de l'inhibiteur de la topoisomerase-ii, un bis-dioxypiperazine et par radiotherapie

Kenneth Francis Hofland; Maxwell Sehested; Paul E.G. Kristjansen; Annemette V. Thougaard; Peter Buhl Jensen


Archive | 2000

Bisdioxopiperazine for the treatment of accidental extravasation of anthracyclines

Peter Buhl Jensen; Seppo W. Langer; Maxwell Sehested


Archive | 2000

Dexrazoxano para el tratamiento de la extravasacion accidental de antraciclinas.

Peter Buhl Jensen; Seppo W. Langer; Maxwell Sehested

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Peter Buhl Jensen

St. Jude Children's Research Hospital

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Kenneth Francis Hofland

Copenhagen University Hospital

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Ellen Friche

University of Copenhagen

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Peter Buhl Jensen

St. Jude Children's Research Hospital

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