Alcalase-Based Chickpea (<i>Cicer arietinum</i> L.) Protein Hydrolysates Efficiently Reduce Systolic Blood Pressure in Spontaneously Hypertensive Rats.

Figueroa-Salcido, Oscar Gerardo; Arámburo-Gálvez, Jesús Gilberto; Mora-Melgem, José Antonio; Camacho-Cervantes, Diana Laura; Gracia-Valenzuela, Martina Hilda; Cuevas-Rodríguez, Edith Oliva; Ontiveros, Noé

Alcalase-Based Chickpea (Cicer arietinum L.) Protein Hydrolysates Efficiently Reduce Systolic Blood Pressure in Spontaneously Hypertensive Rats.

Figueroa-Salcido, Oscar Gerardo; Arámburo-Gálvez, Jesús Gilberto; Mora-Melgem, José Antonio; Camacho-Cervantes, Diana Laura; Gracia-Valenzuela, Martina Hilda; Cuevas-Rodríguez, Edith Oliva; Ontiveros, Noé.

Afiliação

Figueroa-Salcido OG; Integral Postgraduate Program in Biotechnology, Faculty of Chemical and Biological Sciences, Autonomous University of Sinaloa, Ciudad Universitaria, Culiacan 80010, Sinaloa, Mexico.
Arámburo-Gálvez JG; Nutrition Sciences Postgraduate Program, Faculty of Nutrition Sciences, Autonomous University of Sinaloa, Culiacan 80019, Sinaloa, Mexico.
Mora-Melgem JA; Nutrition Sciences Postgraduate Program, Faculty of Nutrition Sciences, Autonomous University of Sinaloa, Culiacan 80019, Sinaloa, Mexico.
Camacho-Cervantes DL; Nutrition Sciences Postgraduate Program, Faculty of Nutrition Sciences, Autonomous University of Sinaloa, Culiacan 80019, Sinaloa, Mexico.
Gracia-Valenzuela MH; National Technological Institute of Mexico, Yaqui Valley Technological Institute, Bácum 85276, Sonora, Mexico.
Cuevas-Rodríguez EO; Integral Postgraduate Program in Biotechnology, Faculty of Chemical and Biological Sciences, Autonomous University of Sinaloa, Ciudad Universitaria, Culiacan 80010, Sinaloa, Mexico.
Ontiveros N; Nutrition Sciences Postgraduate Program, Faculty of Nutrition Sciences, Autonomous University of Sinaloa, Culiacan 80019, Sinaloa, Mexico.

Foods ; 13(8)2024 Apr 16.

Article em En | MEDLINE | ID: mdl-38672889

ABSTRACT

ABSTRACT

Studies on antihypertensive chickpea protein hydrolysates have rarely performed in vivo evaluations, limiting the entry of such hydrolysates into functional food development and clinical trials. Thus, our aim was to optimize the hydrolysis conditions to produce an alcalase-based chickpea hydrolysate with a hypotensive effect in vivo at convenient oral doses. The hydrolysis reaction time, temperature, and alcalase/substrate concentration were optimized using a response surface analysis (RSA). ACE-I inhibition was the response variable. The optimized hydrolysis conditions were time = 0.5 h, temperature = 40 °C, and E/S concentration = 0.254 (U/g). The IC50 of the optimized hydrolysate (OCPH) was 0.358 mg/mL. Five hydrolysates from the RSA worksheet (one of them obtained after 5 min of hydrolysis (CPH15)) had an ACE-I inhibitory potential similar to that of OCPH (p > 0.05). At 50 mg/kg doses, OCPH and CPH15 promoted a clinically relevant hypotensive effect in spontaneously hypertensive rats, up to -47.35 mmHg and -28.95 mmHg, respectively (p < 0.05 vs. negative control). Furthermore, the hypotensive effect was sustained for at least 7 h post-supplementation. Overall, OCPH and CPH15 are promising ingredients for functional food development and as test materials for clinical trials.

Palavras-chave

ACE-I; antihypertensive peptides; bioactive peptides; chickpea; hydrolysate; hypertension

Texto completo

Imprimir

XML

PubMed Links

Buscar no Google

Texto completo: 1 Base de dados: MEDLINE Idioma: En Ano de publicação: 2024 Tipo de documento: Article

Texto completo

Imprimir

XML

PubMed Links