Conformational properties of amphotericin B amide derivatives - Impact on selective toxicity

H. Resat; F. A. Sungur; M. Baginski; E. Borowski; V. Aviyente

doi:10.1023/A:1008144208706

Conformational properties of amphotericin B amide derivatives - Impact on selective toxicity

H. Resat^*
, F. A. Sungur
, M. Baginski
, E. Borowski
, V. Aviyente

^*Corresponding author for this work

Research output: Contribution to journal › Article › peer-review

29 Citations (Scopus)

Abstract

Even though it is highly toxic, Amphotericin B (AmB), an amphipathic polyene macrolide antibiotic, is used in the treatment of severe systemic fungal infections as a life-saving drug. To examine the influence of conformational factors on selective toxicity of these compounds, we have investigated the conformational properties of five AmB amide derivatives. It was found that the extended conformation with torsional angles (ΦΨ)=(290°, 180°) is a common minimum of the potential energy surfaces (PES) of unsubstituted AmB and its amide derivatives. The extended conformation of the studied compounds allows for the formation of an intermolecular hydrogen bond network between adjacent antibiotic molecules in the open channel configuration. Therefore, the extended conformation is expected to be the dominant conformer in an open AmB (or its amide derivatives) membrane channel. The derivative compounds for calculations were chosen according to their selective toxicity compared to AmB and they had a wide range of selective toxicity. Except for two AmB derivatives, the PES maps of the derivatives reveal that the molecules can coexist in more than one conformer. Taking into account the cumulative conclusions drawn from the earlier MD simulation studies of AmB membrane channel, the results of the potential energy surface maps, and the physical considerations of the molecular structures, we hypothesize a new model of structure-selective toxicity of AmB derivatives. In this proposed model the presence of the extended conformation as the only well defined global conformer for AmB derivatives is taken as the indicator of their higher selective toxicity. This model successfully explains our results. To further test our model, we also investigated an AmB derivative whose selective toxicity has not been experimentally measured before. Our prediction for the selective toxicity of this compound can be tested in experiments to validate or invalidate the proposed model.

Original language	English
Pages (from-to)	689-703
Number of pages	15
Journal	Journal of Computer-Aided Molecular Design
Volume	14
Issue number	7
DOIs	https://doi.org/10.1023/A:1008144208706
Publication status	Published - 2000
Externally published	Yes

Funding

A.S. performed the calculations reported in this manuscript and this study forms a part of her Ph.D. thesis. The computations were performed using the computing resources of Bogaziçi and Koç Universities. This study was funded in part by a grant from the State Committee of Scientific Research, Warsaw (Poland) – grant number 3T09A07014. We would like to thank Jaroslav Koca for his help in preparing the figures.

Funders	Funder number
State Committee of Scientific Research, Warsaw (Poland)	3T09A07014

Keywords

Amide derivatives of Amphotericin B
Amphotericin B
Cholesterol
Conformation analysis
Drug design
Ergosterol
Membrane ion channel
Potential energy surface
Semiempirical quantum chemistry methods

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10.1023/A:1008144208706

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@article{b79131b33977406ba7f434a2abc47f10,

title = "Conformational properties of amphotericin B amide derivatives - Impact on selective toxicity",

abstract = "Even though it is highly toxic, Amphotericin B (AmB), an amphipathic polyene macrolide antibiotic, is used in the treatment of severe systemic fungal infections as a life-saving drug. To examine the influence of conformational factors on selective toxicity of these compounds, we have investigated the conformational properties of five AmB amide derivatives. It was found that the extended conformation with torsional angles (ΦΨ)=(290°, 180°) is a common minimum of the potential energy surfaces (PES) of unsubstituted AmB and its amide derivatives. The extended conformation of the studied compounds allows for the formation of an intermolecular hydrogen bond network between adjacent antibiotic molecules in the open channel configuration. Therefore, the extended conformation is expected to be the dominant conformer in an open AmB (or its amide derivatives) membrane channel. The derivative compounds for calculations were chosen according to their selective toxicity compared to AmB and they had a wide range of selective toxicity. Except for two AmB derivatives, the PES maps of the derivatives reveal that the molecules can coexist in more than one conformer. Taking into account the cumulative conclusions drawn from the earlier MD simulation studies of AmB membrane channel, the results of the potential energy surface maps, and the physical considerations of the molecular structures, we hypothesize a new model of structure-selective toxicity of AmB derivatives. In this proposed model the presence of the extended conformation as the only well defined global conformer for AmB derivatives is taken as the indicator of their higher selective toxicity. This model successfully explains our results. To further test our model, we also investigated an AmB derivative whose selective toxicity has not been experimentally measured before. Our prediction for the selective toxicity of this compound can be tested in experiments to validate or invalidate the proposed model.",

keywords = "Amide derivatives of Amphotericin B, Amphotericin B, Cholesterol, Conformation analysis, Drug design, Ergosterol, Membrane ion channel, Potential energy surface, Semiempirical quantum chemistry methods",

author = "H. Resat and Sungur, \{F. A.\} and M. Baginski and E. Borowski and V. Aviyente",

year = "2000",

doi = "10.1023/A:1008144208706",

language = "English",

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T1 - Conformational properties of amphotericin B amide derivatives - Impact on selective toxicity

AU - Resat, H.

AU - Sungur, F. A.

AU - Baginski, M.

AU - Borowski, E.

AU - Aviyente, V.

PY - 2000

Y1 - 2000

N2 - Even though it is highly toxic, Amphotericin B (AmB), an amphipathic polyene macrolide antibiotic, is used in the treatment of severe systemic fungal infections as a life-saving drug. To examine the influence of conformational factors on selective toxicity of these compounds, we have investigated the conformational properties of five AmB amide derivatives. It was found that the extended conformation with torsional angles (ΦΨ)=(290°, 180°) is a common minimum of the potential energy surfaces (PES) of unsubstituted AmB and its amide derivatives. The extended conformation of the studied compounds allows for the formation of an intermolecular hydrogen bond network between adjacent antibiotic molecules in the open channel configuration. Therefore, the extended conformation is expected to be the dominant conformer in an open AmB (or its amide derivatives) membrane channel. The derivative compounds for calculations were chosen according to their selective toxicity compared to AmB and they had a wide range of selective toxicity. Except for two AmB derivatives, the PES maps of the derivatives reveal that the molecules can coexist in more than one conformer. Taking into account the cumulative conclusions drawn from the earlier MD simulation studies of AmB membrane channel, the results of the potential energy surface maps, and the physical considerations of the molecular structures, we hypothesize a new model of structure-selective toxicity of AmB derivatives. In this proposed model the presence of the extended conformation as the only well defined global conformer for AmB derivatives is taken as the indicator of their higher selective toxicity. This model successfully explains our results. To further test our model, we also investigated an AmB derivative whose selective toxicity has not been experimentally measured before. Our prediction for the selective toxicity of this compound can be tested in experiments to validate or invalidate the proposed model.

AB - Even though it is highly toxic, Amphotericin B (AmB), an amphipathic polyene macrolide antibiotic, is used in the treatment of severe systemic fungal infections as a life-saving drug. To examine the influence of conformational factors on selective toxicity of these compounds, we have investigated the conformational properties of five AmB amide derivatives. It was found that the extended conformation with torsional angles (ΦΨ)=(290°, 180°) is a common minimum of the potential energy surfaces (PES) of unsubstituted AmB and its amide derivatives. The extended conformation of the studied compounds allows for the formation of an intermolecular hydrogen bond network between adjacent antibiotic molecules in the open channel configuration. Therefore, the extended conformation is expected to be the dominant conformer in an open AmB (or its amide derivatives) membrane channel. The derivative compounds for calculations were chosen according to their selective toxicity compared to AmB and they had a wide range of selective toxicity. Except for two AmB derivatives, the PES maps of the derivatives reveal that the molecules can coexist in more than one conformer. Taking into account the cumulative conclusions drawn from the earlier MD simulation studies of AmB membrane channel, the results of the potential energy surface maps, and the physical considerations of the molecular structures, we hypothesize a new model of structure-selective toxicity of AmB derivatives. In this proposed model the presence of the extended conformation as the only well defined global conformer for AmB derivatives is taken as the indicator of their higher selective toxicity. This model successfully explains our results. To further test our model, we also investigated an AmB derivative whose selective toxicity has not been experimentally measured before. Our prediction for the selective toxicity of this compound can be tested in experiments to validate or invalidate the proposed model.

KW - Amide derivatives of Amphotericin B

KW - Amphotericin B

KW - Cholesterol

KW - Conformation analysis

KW - Drug design

KW - Ergosterol

KW - Membrane ion channel

KW - Potential energy surface

KW - Semiempirical quantum chemistry methods

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AN - SCOPUS:0033835486

SN - 0920-654X

VL - 14

SP - 689

EP - 703

JO - Journal of Computer-Aided Molecular Design

JF - Journal of Computer-Aided Molecular Design

IS - 7

ER -

Conformational properties of amphotericin B amide derivatives - Impact on selective toxicity

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Keywords

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