Self‐Assembly of Therapeutic Peptide into Stimuli‐Responsive Clustered Nanohybrids for Cancer‐Targeted Therapy

He, Wangxiao; Wang, Simeng; Yan, Jin; Qu, Yiping; Jin, Liang; Sui, Fang; Li, Yujun; You, Weiming; Guang, Yang; Yang, Qi; Ji, Meiju; Shao, Yongping; Peter, X.; Lu, Wuyuan; Hou, Peng

doi:10.1002/adfm.201807736

Cited by 65 publications

(53 citation statements)

References 64 publications

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“…As previous report, the dodecameric peptide PMI is designed for competitive antagonism MDM2 to restore p53, thereby reactivating the anti-cancer function of p53 to kill cancer cells (Figure 5 A) 47 . The 20-mer BBI was dedicated to targeting β-catenin toward disturbing the β-catenin/Bcl9 interaction and as a result of the blockage of the cancerogenic Wnt signaling pathway (Figure 5 B) 48 . Besides, dextrorotary peptide DPA has similar functions as PMI to restore p53 (Figure 5 C) 45 .…”

Section: Resultsmentioning

confidence: 99%

“…To address them, we turn our gaze to a de novo synthesis of nanoparticle by Au(I) thiolate precursors 32 , 33 . By this approach, previous reports successfully fabricated size-tuned gold nanoparticles via reducing Au(I)-glutathione precursors 32 , 34 . But that reaction, in which thiol peptide strains the conversion of the ionic gold precursor into metallic gold nuclei, has to be driven by strong reducing agent, such as sodium borohydride (NaBH 4 ) 33 .…”

Section: Introductionmentioning

confidence: 99%

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A general-purpose Nanohybrid fabricated by Polymeric Au(I)-peptide precursor to wake the function of Peptide Therapeutics

Yan¹,

Ji²,

Yan³

et al. 2020

Theranostics

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Peptide-derived nanocomposites have been exhibiting fascinating biological advantages, including but not limited to excellent biocompatibility, biological degradation, high targetability and subsequent potent therapeutic efficacy. While some successes have been achieved in the nanoengineering of peptide-based architectures with defined dimensions and medical functions, enormous challenges remain about clinical nano-pharmaceutics of peptides, especially those modulating intracellular protein-protein interactions (PPIs). Methods: We developed a general method to translate intracellular-PPI-targeted peptides into a bioavailable peptide-auric s pheroidal n ano h ybrid (SNH), for which polymeric peptide-Auric precursors [Au 1+ -S-peptide] n are in-situ reduced on the surface of gold nanoseeds via a simple and mild reaction. As proofs of concept, three cytomembrane-impenetrable peptides with different physicochemical properties were successfully engineered into stable and tumor-specific SNH respectively. Results: To highlight the advantage of SNH, PMI, a hydrophobic and enzyme-intolerant peptide capable of p53 restoration, was selected to challenge the power of SNH in a colon tumor xenografts model. PMI-Au SNH in vivo suppressed tumor growth potently after three administrations: intravenous injection, intraperitoneal injection and gastric perfusion, and maintained a favorable therapeutic safety. Conclusion: This therapeutically feasible strategy of peptide nanoengineering will allow us to fabricate a series of nanomedicines to modulate carcinogenic PPIs that hide and multiply inside cells, and in all likelihood reinvigorate the development of peptide drug against wide varieties of human diseases.

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Section: Resultsmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

A general-purpose Nanohybrid fabricated by Polymeric Au(I)-peptide precursor to wake the function of Peptide Therapeutics

Yan¹,

Ji²,

Yan³

et al. 2020

Theranostics

Self Cite

View full text Add to dashboard Cite

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“…After synthesis, peptides were cleaved by a reagent cocktail, which is consist of TFA (88%), phenol (5%), H2O (5%) and TIPS (2%). Next, products were identified and purified by C18 or C4 reversed-phase HPLC [49]. ESI-MS was used to ascertain the molecular weights of peptides.…”

Section: Methodsmentioning

confidence: 99%

A lanthanide-peptide-derived bacterium-like nanotheranostic with high tumor-targeting, -imaging and -killing properties

Yan

Wang

et al. 2019

Biomaterials

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Nanostructures formed with bioactive peptides offer an exciting prospect in clinical oncology as a novel class of therapeutic agents for human cancers. Despite their therapeutic potential, however, peptide-based nanomedicines are often inefficacious in vivo due to low cargo-loading efficiency, poor tumor cell-targeting specificity and limited drug accumulation in tumor tissues. Here, we describe the design, via assembly of a p53-activating peptide termed PMI, functionalized PEG and fluorescent lanthanide oxyfluoride nanocrystals, of a novel nanotheranostic shaped in flexible rods. This lanthanide-peptide nanorod or LProd of bionic nature exhibited significantly enhanced tumor-targeting and -imaging properties compared to its spherical counterpart. Importantly, LProd potently inhibited tumor growth in a mouse model of human colon cancer through activating tumor suppressor protein p53 via MDM2/MDMX antagonism, while maintaining a highly favorable biosafety profile. Our data demonstrate that LProd as a multifunctional theranostic platform is ideally suited for tumor-specific peptide drug delivery with real-time disease tracking, thereby broadly impacting clinical development of antitumor peptides.

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“…In another study, He et al fabricated Au-peptide nanohybrids (pParticles) via the copolymerization of HAuCl 4 and a β-catenin/Bcl9 inhibitor (BBI). 60 Then, the pParticle self-assembled into a size-switchable and pH-responsive nanocluster (pCluster) triggered by poly-L-lysine. In the acidic TME, pCluster accumulated at the tumor site due to the EPR effect and disintegrated into small nanoparticles, which contributed to deep penetration and cellular internalization.…”

Section: The Wnt/β-catenin Pathwaymentioning

confidence: 99%

Nanomaterials Enhance the Immunomodulatory Effect of Molecular Targeted Therapy

Li¹,

Liu²,

Fang³

et al. 2021

IJN

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Self‐Assembly of Therapeutic Peptide into Stimuli‐Responsive Clustered Nanohybrids for Cancer‐Targeted Therapy

Cited by 65 publications

References 64 publications

A general-purpose Nanohybrid fabricated by Polymeric Au(I)-peptide precursor to wake the function of Peptide Therapeutics

A general-purpose Nanohybrid fabricated by Polymeric Au(I)-peptide precursor to wake the function of Peptide Therapeutics

A lanthanide-peptide-derived bacterium-like nanotheranostic with high tumor-targeting, -imaging and -killing properties

Nanomaterials Enhance the Immunomodulatory Effect of Molecular Targeted Therapy

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