Engineering kinetics of TLR7/8 agonist release from bottlebrush prodrugs enables tumor-focused immune stimulation

Bhagchandani, Sachin; Vohidov, Farrukh; Milling, Lauren E.; Tong, Evelyn Yuzhou; Brown, C M; Ramseier, Michelle; Liu, Bin; Fessenden, Tim; Nguyen, Hung V.-T.; Kiel, Gavin R; Won, Lori; Langer, Robert; Spranger, Stefani; Shalek, Alex K.; Irvine, Darrell J.; Johnson, Jeremiah A.

doi:10.1126/sciadv.adg2239

Cited by 20 publications

(14 citation statements)

References 73 publications

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“…59–62 A library of “bottlebrush-like” polynorbornene nanostructures covalently linked to polyethylene glycol (PEG) chains was synthesized by modifying the linker chemistry of conjugated resiquimod, a TLR7/8 agonist. 63 Changing the azido- and ester-based linker chemistry that conjugated resiquimod allowed for control over the hydrolytic and esterase degradation kinetics, while maintaining the size and morphology of the structure. Increasing local steric hindrance and the charge of each aryl ester linker by modifying the R groups slowed degradation and increased the release half-life of resiquimod.…”

Section: Transport and Processing Characteristics For Immunomodulator...mentioning

confidence: 99%

“…Increasing local steric hindrance and the charge of each aryl ester linker by modifying the R groups slowed degradation and increased the release half-life of resiquimod. 63 In addition to bulkier chemical groups, steric hindrance can be increased through high-density clustering to protect conjugated cargo and reduce the effects of enzymatic degradation and hydrolysis. This technique has widely been employed using DNA-based structures, including spherical nucleic acids (SNAs), 64–66 DNA origami, 67 and single and double stranded DNA nanostructures.…”

Section: Transport and Processing Characteristics For Immunomodulator...mentioning

confidence: 99%

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Harnessing biomaterial architecture to drive anticancer innate immunity

Davis,

Cho,

Teplensky

2023

J. Mater. Chem. B

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Section: Transport and Processing Characteristics For Immunomodulator...mentioning

confidence: 99%

Section: Transport and Processing Characteristics For Immunomodulator...mentioning

confidence: 99%

Harnessing biomaterial architecture to drive anticancer innate immunity

Davis,

Cho,

Teplensky

2023

J. Mater. Chem. B

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“…The dense grafting of side chains distinguishes this subclass of macromolecules, known as bottlebrushes (BBs), from other branched or comb polymers due to an unorthodox combination of high molar mass yet low viscosity. − This behavior is attributed to steric repulsions between neighboring side chains, which occupy the excluded volume near the backbone and increase the BB persistence length. The BB molecular architecture is inspired by naturally occurring proteoglycans present in biological constructs, such as articular cartilage, where lubrication and impact damping are required. , BB syntheses have progressed rapidly since their introduction, ,,− showing promise in applications such as super soft gels/elastomers, − drug delivery agents − photonic crystals, , energy storage, and advanced nanoscale patterning. − Despite recent experimental and theoretical efforts, distinct relationships between BB polymer architecture and material properties are still ongoing due to the many modifiable architectural parameters. These include the chemical composition of the backbone and side chains, the number of backbone atoms between side chains ( n g ), the side chain degree of polymerization ( N sc ), and the backbone degree of polymerization ( N bb ).…”

Section: Introductionmentioning

confidence: 99%

Comparison of Polypentenamer and Polynorbornene Bottlebrushes in Dilute Solution

Leo,

Jang,

Corey

et al. 2024

ACS Polym. Au

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Bottlebrush (BB) polymers were synthesized via grafting-from-atom transfer radical polymerization (ATRP) of styrene on polypentenamer and polynorbornene macroinitiators with matched grafting density (n g = 4) and backbone degrees of polymerization (122 ≥ N bb ≥ 61) to produce a comparative study on their respective dilute solution properties as a function of increasing side chain degree of polymerization (116 ≥ N sc ≥ 5). The grafting-from technique produced near quantitative grafting efficiency and narrow dispersity N sc as evidenced by spectroscopic analysis and ring closing metathesis depolymerization of the polypentenamer BBs. The versatility of this synthetic approach permitted a comprehensive survey of power law expressions that arise from monitoring intrinsic viscosity, hydrodynamic radius, and radius of gyration as a function of increasing the molar mass of the BBs by increasing N sc . These values were compared to a series of linear (nongrafted, N sc = 0) macroinitiators in addition to linear grafts. This unique study allowed elucidation of the onset of bottlebrush behavior for two different types of bottlebrush backbones with identical grafting density but inherently different flexibility. In addition, grafting-from ATRP of methyl acrylate on a polypentenamer macroinitiator allowed the observation of the effects of graft chemistry in comparison to polystyrene. Differences in the observed scaling relationships in dilute solution as a function of each of these synthetic variants are discussed.

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“…In contrast, OEGMA-11 NPs demonstrated not only superior immune evasion but also significantly high tumor accumulation across three subcutaneous cancer models as well as orthotopic glioblastoma and pancreatic cancer models, which showed the best overall performance in tumor-targeted delivery (Figure B and Table S1). ,− The strong correlation between tumor accumulation and blood-circulation time revealed immune-evasion-mediated tumor targeting. We further found that the OEGMA-11 NPs showed deep penetration into tumor tissues and maintained relatively high concentrations 21 days post injection, thereby facilitating favorable antitumor efficacy.…”

Section: Introductionmentioning

confidence: 99%

Theranostic Bottle-Brush Polymers Tailored for Universal Solid-Tumor Targeting

Zhang,

Xu,

Guo

et al. 2024

ACS Nano

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Designing an efficient nanocarrier to target multiple types of cancer remains a major challenge in the development of cancer nanomedicines. The majority of systemically administered nanoparticles (NPs) are rapidly cleared by the liver, resulting in poor tumor-targeting efficiency and severe side effects. Here, we present a delicately tailored design and synthesis of fluorescent bottle-brush polymers and screen nine derived NPs, each varying in size and surface coatings, for tumor imaging and targeted delivery. Our optimized polymer bearing (oligo(ethylene glycol) methyl ether methacrylate) in the side chains shows reduced macrophage uptake, prolonged blood-circulation time (up to 27 h), and exceptionally high accumulation in the tumor compared to the liver, elucidating an immune-evasion-induced tumor-targeting mechanism. High tumor accumulation significantly improved the antitumor efficacy. The outstanding tumor-targeting ability has been further validated across five distinct tumor models, including orthotopic glioblastoma and pancreatic cancer, which demonstrate the universality of our polymeric nanocarrier for tumor-targeting delivery.

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Engineering kinetics of TLR7/8 agonist release from bottlebrush prodrugs enables tumor-focused immune stimulation

Cited by 20 publications

References 73 publications

Harnessing biomaterial architecture to drive anticancer innate immunity

Harnessing biomaterial architecture to drive anticancer innate immunity

Comparison of Polypentenamer and Polynorbornene Bottlebrushes in Dilute Solution

Theranostic Bottle-Brush Polymers Tailored for Universal Solid-Tumor Targeting

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