cashew gum
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Author(s):  
Bruna M. Miranda ◽  
Mauricio V. Cruz ◽  
Ivan T. N. de Campos ◽  
Kátia F. Fernandes ◽  
Flávio A. Silva
Keyword(s):  

Author(s):  
Nathalia D. Gonçalves ◽  
Marta C. T. Duarte ◽  
Ana S. Prata ◽  
Rodney A. F. Rodrigues

2021 ◽  
Vol 191 ◽  
pp. 1026-1037
Author(s):  
Eryka Oliveira de Andrades ◽  
João Marcos Antônio Rodrigues da Costa ◽  
Francisco Edmar Moreira de Lima Neto ◽  
Alyne Rodrigues de Araujo ◽  
Fabio de Oliveira Silva Ribeiro ◽  
...  

Author(s):  
Thais Danyelle Santos Araujo ◽  
João Marcos Antônio Rodrigues da Costa ◽  
Fabio de Oliveira Silva Ribeiro ◽  
Antonia Carla de Jesus Oliveira ◽  
Jhones do Nascimento Dias ◽  
...  

2021 ◽  
Vol 11 (18) ◽  
pp. 8467
Author(s):  
Kahynna C. Loureiro ◽  
Alessandro Jäger ◽  
Ewa Pavlova ◽  
Isabel B. Lima-Verde ◽  
Petr Štěpánek ◽  
...  

Every year, more than thirty thousand tons of Cashew gum (Anacardium occidentale, family: Anacardiaceae) are produced in Brazil; however, only a small amount is used for different applications in foodstuff and in pharmaceutical industries. As a raw material for the production of drug delivery systems, cashew gum is still regarded as an innovative compound worth to be exploited. In this work, cashew gum was extracted from the crude exudate of cashew tree employing four methodologies resulting in a light brown powder in different yields (40.61% to 58.40%). The total ashes (0.34% to 1.05%) and moisture (12.90% to 14.81%) were also dependent on the purification approach. FTIR spectra showed the typical bands of purified cashew gum samples, confirming their suitability for the development of a pharmaceutical product. Cashew gum nanoparticles were produced by nanoprecipitation resulting in particles of low polydispersity (<0.2) and an average size depending on the percentage of the oil. The zeta potential of nanoparticles was found to be below 20 mV, which promotes electrostatic stability. Encapsulation efficiencies were above 99.9%, while loading capacity increased with the increase of the percentage of the oil content of particles. The release of the oil from the nanoparticles followed the Korsmeyer–Peppas kinetics model, while particles did not show any signs of toxicity when tested in three distinct cell lines (LLC-MK2, HepG2, and THP-1). Our study highlights the potential added value of using a protein-, lignans-, and nucleic acids-enriched resin obtained from crude extract as a new raw material for the production of drug delivery systems.


LWT ◽  
2021 ◽  
pp. 112315
Author(s):  
Weysser Felipe Cândido de Souza ◽  
Fernando Azevedo de Lucena ◽  
Kátia Gomes da Silva ◽  
Laésio Pereira Martins ◽  
Ruann Janser Soares de Castro ◽  
...  

2021 ◽  
Vol 167 ◽  
pp. 106268
Author(s):  
Airis Maria Araújo Melo ◽  
Roselayne Ferro Furtado ◽  
Maria de Fatima Borges ◽  
Atanu Biswas ◽  
Huai N. Cheng ◽  
...  

Diabetology ◽  
2021 ◽  
Vol 2 (2) ◽  
pp. 107-116
Author(s):  
Janira M. N. A. Bezerra ◽  
Antônia C. J. Oliveira ◽  
Edson C. Silva-Filho ◽  
Patricia Severino ◽  
Selma B. Souto ◽  
...  

Polyelectrolytic complexation has stood out due to its application in the development of drug delivery systems using biopolymers as raw materials. The formation of complexes between cashew gum and chitosan can be intermediated by cross-links, mediated by the action of the sodium tripolyphosphate crosslinking agent. These polymers have been used in the nanotechnological development of formulations to protect peptide drugs, such as insulin, allowing their oral administration. In this work, we describe the development of polyelectrolytic complexes from cashew gum and chitosan as biopolymers for oral administration of insulin. The obtained complexes showed a mean particle size of 234 nm and polydispersity index of 0.2. The complexes were 234 nm in size, PDI 0.2, zeta potential −4.5 mV and 22% trapping. The obtained complexes demonstrated considerable and promising characteristics for use as oral insulin delivery systems.


Author(s):  
Ana Paula de Sá Pinto Abrahão Magalhães ◽  
Helena Keiko Toma ◽  
Flávia Almada do Carmo ◽  
Claudia Regina Elias Mansur

Materials ◽  
2021 ◽  
Vol 14 (9) ◽  
pp. 2115
Author(s):  
Cassio Nazareno Silva da Silva ◽  
Maria Carolina Bezerra Di-Medeiros ◽  
Luciano Morais Lião ◽  
Kátia Flávia Fernandes ◽  
Karla de Aleluia Batista

This investigation focuses on the development and optimization of cashew gum polysaccharide (CGP) nanoparticles grafted with polypropylene glycol (PPG) as carriers for diclofenac sodium. The optimization of parameters affecting nanoparticles formulation was performed using a central composite rotatable design (CCRD). It was demonstrated that the best formulation was achieved when 10 mg of CGP was mixed with 10 μL of PPG and homogenized at 22,000 rpm for 15 min. The physicochemical characterization evidenced that diclofenac was efficiently entrapped, as increases in the thermal stability of the drug were observed. The CGP-PPG@diclofenac nanoparticles showed a globular shape, with smooth surfaces, a hydrodynamic diameter around 275 nm, a polydispersity index (PDI) of 0.342, and a zeta potential of −5.98 mV. The kinetic studies evidenced that diclofenac release followed an anomalous transport mechanism, with a sustained release up to 68 h. These results indicated that CGP-PPG nanoparticles are an effective material for the loading/release of drugs with similar structures to diclofenac sodium.


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