Novel Integrin-Targeted Binding-Triggered Drug Delivery System for Methotrexate

Kotamraj, Phanidhara R.; Russu, Wade A.; Jasti, Bhaskara; Wu, Jay J.-Q.; Li, Xiaoling

doi:10.1007/s11095-011-0495-5

Cited by 9 publications

(4 citation statements)

References 24 publications

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“…2 we estimated ∆H b = −12.22 k B T for IB and ∆H b = −1.71 k B T for WB. The values of ∆H b computed through the two methods are in excellent agreement with each other and also with experimentally obtained binding energies [74,75]; this comparison is displayed in Table 1. Explicit calculations show that the receptor-ligand interactions follow a Bell potential: The PMFs shown in Fig.…”

Section: Computed Values Of Receptor-ligand Binding Energies Compare supporting

confidence: 80%

“…The SB system corresponds to an Inter-cellular adhesion molecule (ICAM aka CD54) receptor interacting with its YN1 antibody, while the IB and WB systems correspond to the α 5 β 1 domain of integrin interacting with peptide sequences KGGEPRGDTYR and GERGDGSFFAFRSPF, both of which contain the well-recognized RGD (Arg-Gly-Asp) binding domain. These sequences are peptidomimetics that mimic the integrin binding domains found in the extracellular matrix proteins, fibronectin and collagen, respectively [74][75][76][77]. The interaction energies of each of these pairs are listed in Table 1, and the snapshots of the IB and WB systems in their respective bound states are shown in Suppl.…”

Section: Receptor-ligand Pairs Of Interestmentioning

confidence: 99%

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Multivalent Binding of a Ligand-Coated Particle: Role of Shape, Size, and Ligand Heterogeneity

McKenzie

Rammohan

et al. 2018

Biophysical Journal

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We utilize a multiscale modeling framework to study the effect of shape, size, and ligand composition on the efficacy of binding of a ligand-coated particle to a substrate functionalized with the target receptors. First, we show how molecular dynamics along with steered molecular dynamics calculations can be used to accurately parameterize the molecular-binding free energy and the effective spring constant for a receptor-ligand pair. We demonstrate this for two ligands that bind to the αβ-domain of integrin. Next, we show how these effective potentials can be used to build computational models at the meso- and continuum-scales. These models incorporate the molecular nature of the receptor-ligand interactions and yet provide an inexpensive route to study the multivalent interaction of receptors and ligands through the construction of Bell potentials customized to the molecular identities. We quantify the binding efficacy of the ligand-coated-particle in terms of its multivalency, binding free-energy landscape, and the losses in the configurational entropies. We show that 1) the binding avidity for particle sizes less than 350 nm is set by the competition between the enthalpic and entropic contributions, whereas that for sizes above 350 nm is dominated by the enthalpy of binding; 2) anisotropic particles display higher levels of multivalent binding compared to those of spherical particles; and 3) variations in ligand composition can alter binding avidity without altering the average multivalency. The methods and results presented here have wide applications in the rational design of functionalized carriers and also in understanding cell adhesion.

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Section: Computed Values Of Receptor-ligand Binding Energies Compare supporting

confidence: 80%

Section: Receptor-ligand Pairs Of Interestmentioning

confidence: 99%

Multivalent Binding of a Ligand-Coated Particle: Role of Shape, Size, and Ligand Heterogeneity

McKenzie

Rammohan

et al. 2018

Biophysical Journal

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“…Covalent linkage of two chemically distinct moieties into one conjugated molecule presents a facile yet effective chemistry approach to achieve new molecular characteristics and synergistic properties. Examples include the incorporation of a small auxiliary group to a biologically, electronically, or optically active segment to create self-assembling amphiphilic molecules, − and the use of polyethylene glycol (PEGylation) to reduce protein immunogenicity. , In the context of anticancer drug delivery, drug–peptide conjugates have been used as a widely adopted strategy to increase the drug’s aqueous solubility, to create enzyme-cleavable prodrugs, to modify the drug’s pharmacokinetic properties, to achieve cell penetration or selectivity, , and to target a subcellular organelle . Unlike the design of fusion proteins, in which the effect of fusion site ( N - or C -terminal) is already under serious consideration, − the effect of conjugation site in drug–peptide conjugate design is still largely ignored, but could be very important .…”

Section: Introductionmentioning

confidence: 99%

Cellular Uptake and Cytotoxicity of Drug–Peptide Conjugates Regulated by Conjugation Site

et al. 2013

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Conjugation of anticancer drugs to hydrophilic peptides such as Tat is a widely adopted strategy to improve the drug’s solubility, cellular uptake and potency against cancerous cells. Here we report that attachment of an anticancer drug doxorubicin to the N- or C-terminal of the Tat peptide can have a significant impact on their cellular uptake, cytotoxicity against both drug-sensitive and drug-resistant cancer cells. We observed higher cellular uptake by both cell lines for C-terminal conjugate relative to the N-terminal analogue. Our results reveal that the C-terminal conjugate partially overcame the multi-drug resistance of cervical cancer cells, while the N-terminal conjugate showed no significant improvement in cytotoxicity when compared with free doxorubicin. We also found that both N- and C- conjugates offers a mechanism to circumvent drug efflux associated with multidrug resistance.

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“…Tumor-targeted drug delivery approaches, such as PDCs, can improve accumulation of the therapeutic in the diseased tissue, reduce damage to healthy tissues and minimize unwanted side-effects. PDCs have been developed for targeting a wide range of receptors, including integrins, − with a variety of cytotoxic agents including doxorubicin (Dox), paclitaxel (PXT), camptothecin (CPT), and MMAE. ,,,− One emerging therapeutic target in oncology is the integrin α v β 6 , a cell surface receptor highly overexpressed in a wide range of malignancies with little to no expression on normal tissue. − The integrin α v β 6 is present in approximately 90% of pancreatic cancers and nearly all cases of metastatic disease. − Pancreatic cancer remains one of the most lethal malignancies worldwide with a 5 year survival of less than 10%, in part due to limited treatment options. Surgery is the only cure and unfortunately less than 20% of patients are eligible for resection at the time of diagnosis due to the presence of metastasis. − A clear unmet need for more effective and targeted treatments exists.…”

Section: Discussionmentioning

confidence: 99%

Synthesis and Evaluation of a Monomethyl Auristatin E─Integrin α_vβ₆ Binding Peptide–Drug Conjugate for Tumor Targeted Drug Delivery

et al. 2023

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Many anticancer drugs exhibit high systemic off-target toxicities causing severe side effects. Peptide–drug conjugates (PDCs) that target tumor-specific receptors such as integrin αvβ6 are emerging as powerful tools to overcome these challenges. The development of an integrin αvβ6-selective PDC was achieved by combining the therapeutic efficacy of the cytotoxic drug monomethyl auristatin E with the selectivity of the αvβ6-binding peptide (αvβ6-BP) and with the ability of positron emission tomography (PET) imaging by copper-64. The [64Cu]PDC-1 was produced efficiently and in high purity. The PDC exhibited high human serum stability, integrin αvβ6-selective internalization, cell binding, and cytotoxicity. Integrin αvβ6-selective tumor accumulation of the [64Cu]PDC-1 was visualized with PET-imaging and corroborated by biodistribution, and [64Cu]PDC-1 showed promising in vivo pharmacokinetics. The [natCu]PDC-1 treatment resulted in prolonged survival of mice bearing αvβ6 (+) tumors (median survival: 77 days, vs αvβ6 (−) tumor group 49 days, and all other control groups 37 days).

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Novel Integrin-Targeted Binding-Triggered Drug Delivery System for Methotrexate

Abstract: Binding-induced conformation change of hairpin peptide can be used to design integrin-targeted drug delivery system.

Cited by 9 publications

References 24 publications

Multivalent Binding of a Ligand-Coated Particle: Role of Shape, Size, and Ligand Heterogeneity

Multivalent Binding of a Ligand-Coated Particle: Role of Shape, Size, and Ligand Heterogeneity

Cellular Uptake and Cytotoxicity of Drug–Peptide Conjugates Regulated by Conjugation Site

Synthesis and Evaluation of a Monomethyl Auristatin E─Integrin α_vβ₆ Binding Peptide–Drug Conjugate for Tumor Targeted Drug Delivery

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Novel Integrin-Targeted Binding-Triggered Drug Delivery System for Methotrexate

Abstract: Binding-induced conformation change of hairpin peptide can be used to design integrin-targeted drug delivery system.

Cited by 9 publications

References 24 publications

Multivalent Binding of a Ligand-Coated Particle: Role of Shape, Size, and Ligand Heterogeneity

Multivalent Binding of a Ligand-Coated Particle: Role of Shape, Size, and Ligand Heterogeneity

Cellular Uptake and Cytotoxicity of Drug–Peptide Conjugates Regulated by Conjugation Site

Synthesis and Evaluation of a Monomethyl Auristatin E─Integrin αvβ6 Binding Peptide–Drug Conjugate for Tumor Targeted Drug Delivery

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Product

Resources

About

Synthesis and Evaluation of a Monomethyl Auristatin E─Integrin α_vβ₆ Binding Peptide–Drug Conjugate for Tumor Targeted Drug Delivery