Conformational Selection in Anion Recognition: CGMP-Selective Binding by a Naphthalimide-Functionalized Amido-Amine Macrocycle

Amido-amine macrocycles with two and four naphthalimide dyes were designed to bind nucleoside monophosphates and oligonucleotides in an aqueous buffered solution. Anion-templated synthesis was used to direct the macrocyclization reaction to the [2+2] product, while high dilution conditions favored the formation of the [4+4] macrocycle with an unprecedented geometry, as revealed from the X-ray analysis. The [2+2] product was found to exhibit a remarkable binding strength and fluorescence response for cyclic guanosine monophosphate (cGMP) in an aqueous solution. To our knowledge, this is the first synthetic receptor for cGMP, which also demonstrates a high preference to bind guanine-rich sequences accomplished by a strong fluorescence quenching. The receptor conformation is very sensitive to the guest structure in an aqueous solution, thus modeling the adaptive behavior of proteins. The study of synthetic systems with a detectable conformational equilibrium represents a great potential for understanding highly specific and tightly regulated interactions in biological systems. © 2019 American Chemical Society.

Авторы
Oshchepkov A.S. 1, 2 , Shumilova T.A.1 , Zerson M.1 , Magerle R.1 , Khrustalev V.N. 2, 3 , Kataev E.A.1
Номер выпуска
14
Язык
Английский
Страницы
9034-9043
Статус
Опубликовано
Том
84
Год
2019
Организации
  • 1 Faculty of Natural Sciences, Technische Universität Chemnitz, Chemnitz, 09107, Germany
  • 2 Peoples' Friendship University of Russia, RUDN University, Moscow, 117198, Russian Federation
  • 3 National Research Center, Kurchatov Institute, Moscow, 123098, Russian Federation
Ключевые слова
Energy dispersive X ray analysis; Oligonucleotides; Quenching; X ray diffraction analysis; Conformational equilibrium; Conformational selection; Guanine rich sequence; High-dilution conditions; Macrocyclization reactions; Nucleoside monophosphates; Synthetic receptors; Templated synthesis; Fluorescence; amide; amine; anion; artificial receptor; cyclic GMP; dinucleoside phosphate; macrocyclic compound; nucleotide; oligonucleotide; aqueous solution; Article; atomic force microscopy; conformation; crystal structure; crystallization; molecular model; molecular recognition; photochemical quenching; protonation; synthesis; ultraviolet visible spectroscopy; X ray analysis
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