Idioma:

Structural modifications of 2,3-indolobetulinic acid: Design and synthesis of highly potent α-glucosidase inhibitors

Khusnutdinova, Elmira F. ; Petrova, Anastasiya V. ; Thu, Ha Nguyen Thi ; Tu, Anh Le Thi ; Thanh, Tra Nguyen ; Thi, Cham Ba ; Babkov, Denis A. ; Kazakova, Oxana B.

Bioorganic chemistry, 2019-07, Vol.88, p.102957-102957, Article 102957 [Periódico revisado por pares]

United States: Elsevier Inc

Texto completo disponível

Citações Citado por

Enviar para

Título:
Structural modifications of 2,3-indolobetulinic acid: Design and synthesis of highly potent α-glucosidase inhibitors
Autor: Khusnutdinova, Elmira F. ; Petrova, Anastasiya V. ; Thu, Ha Nguyen Thi ; Tu, Anh Le Thi ; Thanh, Tra Nguyen ; Thi, Cham Ba ; Babkov, Denis A. ; Kazakova, Oxana B.
Assuntos: Acarbose ; Betulinic acid ; Indole ; Lupanes ; Natural products ; Synthesis ; Triterpenoids ; Type II diabetes ; α-Glucosidase inhibitor
É parte de: Bioorganic chemistry, 2019-07, Vol.88, p.102957-102957, Article 102957
Notas: ObjectType-Article-1
SourceType-Scholarly Journals-1
ObjectType-Feature-2
content type line 23
Descrição: [Display omitted] •A set of nineteen nitrogen-containing lupane triterpenoids were designed and synthesized.•Most compounds showed high α-glucosidase inhibition activity: IC50 ranged from 76 to 0.04 μM.•Indolo betulinic acid glycine and L-phenylalanine amides were found to be the most active.•Molecular basis of improved potency was elucidated with molecular docking approach. A series of nineteen nitrogen-containing lupane triterpenoids was obtained by modification of C2, C3, C20 and C28 positions of betulonic acid and their α-glucosidase inhibiting activity was investigated. Being a leader compound from our previous study, 2,3-indolo-betulinic acid was used as the main template for different modifications at C-(28)-carboxyl group to obtain cyano-, methylcyanoethoxy-, propargyloxy- and carboxamide derivatives. 20-Oxo- and 29-hydroxy-20-oxo-30-nor-analogues of 2,3-indolo-betulinic acid were synthesized by ozonolysis of betulonic acid followed by Fischer indolization reaction. To compare the influence of the fused indole or the seven-membered A-ring on the inhibitory activity, lupane A-azepanones with different substituents at C28 were synthesized. The structure-activity relationships revealed that the enzyme inhibition activity dramatically increased (up to 4730 times) when the carboxylic group of 2,3-indolo-betulinic acid was converted to the corresponding amide. Thus, the IC50 values for glycine amide and L-phenylalanine amides were 0.04 and 0.05 μM, respectively. This study also revealed that 2,3-indolo-platanic acid is 4.5 times more active than the parent triterpenoid with IC50 of 0.4 μM. Molecular modeling suggested that improved potency is due to additional polar interactions formed between C28 side chain and a sub-pocket of the α-glucosidase allosteric site.
Editor: United States: Elsevier Inc
Idioma: Inglês

Links

View this record in MEDLINE/PubMed

Voltar para lista de resultados

Realização: Logos de Redes Sociais:

Structural modifications of 2,3-indolobetulinic acid: Design and synthesis of highly potent α-glucosidase inhibitors

Khusnutdinova, Elmira F. ; Petrova, Anastasiya V. ; Thu, Ha Nguyen Thi ; Tu, Anh Le Thi ; Thanh, Tra Nguyen ; Thi, Cham Ba ; Babkov, Denis A. ; Kazakova, Oxana B.

United States: Elsevier Inc

Buscando em bases de dados remotas. Favor aguardar.