Evidence of Protein Adsorption in Pegylated Liposomes: Influence of Liposomal Decoration

Sangrà, Marc; Estelrich, Joan; Sabaté, Raimon; Espargaró, Alba; Busquets, Maria Antònia

doi:10.3390/nano7020037

Cited by 21 publications

(28 citation statements)

References 57 publications

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“…As shown in Figure 6, the HSA, hFIB, and hTRF CD spectra exhibited two negative bands at $209 and 220 nm, while the hIgG spectrum showed positive and negative bands at 206 and 216 nm, respectively. The results were consistent with previous reports that HSA, hFIB, and hTRF exhibit typical α-helical structures, [24,25] whereas hIgG exhibits a typical β-folded structure. [26] At low SG-CCD concentrations (<20 μM), the addition of SG-CCDs produced no significant changes in the characteristic peptide CD bands of HSA and hIgG, indicating that the SG-CCDs did not induce any changes to protein folding.…”

Section: Conformation Investigationssupporting

confidence: 93%

Synthesis of cationic carbon dots and their effects on human serum proteins and in vitro blood coagulation

et al. 2021

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Cationic carbon dots (CCDs) are a promising alternative to gene-delivery systems, and good biosafety levels are crucial for their in vivo use. In this study, spherical and monodispersed CCDs with an average surface potential of +28.7 mV were prepared using sucrose and glutamate (denoted SG-CCDs) using a one-pot autoclave-assisted method. Molecular interactions between the SG-CCDs and four major human serum proteins (albumin, immunoglobulin G, fibrinogen, and transferrin) were investigated.The results were further verified on human serum, and the effect of the SG-CCDs on in vitro blood coagulation was examined. The results showed that the fluorescence of human serum was clearly quenched by the SG-CCDs through a dynamic collision mechanism. Moreover, SG-CCDs at a concentration of 20 μM exhibited minor effects on the secondary structure of human serum. The activated partial thromboplastin and prothrombin time as well as the fibrinogen concentration were not changed, indicating that the SG-CCDs did not interfere with the coagulation process. This study provided an understandable background on the behaviour of CCDs in clinical applications.

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Section: Conformation Investigationssupporting

confidence: 93%

Synthesis of cationic carbon dots and their effects on human serum proteins and in vitro blood coagulation

et al. 2021

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“…Surface charge of the liposome was made positive by incubating the stealth liposome formulations with histone. On incubation protein gets adsorbed on the surface of the liposome [42]. It is reported earlier that neutral and anionic liposomes clear extravasations from the tumor vasculature [43].…”

Section: Discussionmentioning

confidence: 95%

Physicochemical characterization of dual action liposomal formulations: anticancer and antimicrobial

Das

Konyak

Das

et al. 2019

Heliyon

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Background: Cancer till date remains one of the world's most life threatening disease accompanied by risk of secondary infections. Therefore formulations carrying anticancer drugs which can also decrease the risk of secondary infection are inevitable. Chemotherapeutic drug doxorubicin along with flavonoids quercetin and epigallocatechin gallate (EGCG) is simultaneously loaded on liposomal formulation exploiting the amphiphilic property of the liposomes. Results: Atomic force microscope imaging reveal the size of liposomal formulation loaded with doxorubicin, quercetin and EGCG to be greater than void liposome confirming the presence of drugs. Liposomal stability is improved by PEGylation; adding to the drug release time in vitro. The charge of phosphatidylcholine is rendered positive by coating the formulation with histone. The average size of the formulation is 342 nm. The encapsulation efficiency of doxorubicin, quercetin and EGCG is found to be 65.8%, 96.8% and 98% respectively. The above formulation demonstrated both anticancer and antimicrobial activity. Conclusion: The formulation will provide dual anticancer and antimicrobial therapy thereby evading secondary infection in cancer patients along with chemotherapy.

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“…Geometry of liposomes was observed by cryo-TEM as described previously by others [39][40][41] with minor modifications. For TEM observations, a Jeol Jem F-200 microscope (Jeol, Tokyo, Japan) operating at 200,000 V was used.…”

Section: Liposome Morphologymentioning

confidence: 99%

Design of a novel vaccine nanotechnology-based delivery system comprising CpGODN-protein conjugate anchored to liposomes

Chatzikleanthous

Schmidt

Buffi

et al. 2020

Journal of Controlled Release

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Although the well-known Toll like receptor (TLR9) agonist CpGODN has shown promising results as vaccine adjuvant in preclinical and clinical studies, its in vivo stability and potential systemic toxicity remain a concern. In an effort to circumvent these issues, different strategies have been employed to increase its stability, localise action and reduce dosage. These include conjugation of CpGODN with proteins or encapsulation/adsorption of CpGODN into/onto liposomes and have resulted in enhanced immunopotency compared to co-administration of free CpGODN and antigen. Here, we designed a novel delivery system of CpGODN based on its conjugation to serve as anchor for liposomes. Thiolmaleimide chemistry was utilised to covalently ligate the Group B Streptococcus (GBS) GBS67 protein antigen with the CpGODN TLR9 agonist. This treatment did not alter protein's ability to be recognised by specific antibodies or the CpGODN to function as a TLR9 agonist. Due to its negative charge, the protein conjugate readily electrostatically bound cationic liposomes composed of 1, 2-distearoyl-snglycero-3-phosphocholine (DSPC), cholesterol and dimethyldioctadecylammonium bromide (DDA).The novel cationic liposomes-protein conjugate complex (GBS67-CpGODN+L) shared similar vesicle characteristics (size and charge) compared to free liposomes but exhibited different structure and morphology. Following intramuscular immunisation, GBS67-CpGODN+L formed a vaccine depot at the injection site and induced a remarkable increase of functional immune responses against GBS compared to the simple co-administration of GBS67, CpGODN and liposomes. This work demonstrates that the conjugation of CpGODN to GBS67 in conjunction with adsorption on cationic liposomes, can promote co-delivery leading to the induction of a multifaceted immune response at low antigen and CpGODN doses. Our findings highlight the potential for harnessing the immunostimulatory properties of different adjuvants to develop more effective nanostructure-based vaccine platforms.

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Evidence of Protein Adsorption in Pegylated Liposomes: Influence of Liposomal Decoration

Cited by 21 publications

References 57 publications

Synthesis of cationic carbon dots and their effects on human serum proteins and in vitro blood coagulation

Synthesis of cationic carbon dots and their effects on human serum proteins and in vitro blood coagulation

Physicochemical characterization of dual action liposomal formulations: anticancer and antimicrobial

Design of a novel vaccine nanotechnology-based delivery system comprising CpGODN-protein conjugate anchored to liposomes

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