2022
DOI: 10.1016/j.mtbio.2022.100245
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Activatable “Matryoshka” nanosystem delivery NgBR siRNA and control drug release for stepwise therapy and evaluate drug resistance cancer

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Cited by 5 publications
(4 citation statements)
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“…Besides, due to the difference in the oxidative environment and pH gradient within the tumor, the effect is obvious, and the combination of the two stimulations has also attracted much attention. Many research results have successfully codelivered chemotherapy drugs and RNA molecules and improved treatment efficacy. …”
Section: Tme-based Stimuli-responsive Rna Delivery Systemsmentioning
confidence: 99%
“…Besides, due to the difference in the oxidative environment and pH gradient within the tumor, the effect is obvious, and the combination of the two stimulations has also attracted much attention. Many research results have successfully codelivered chemotherapy drugs and RNA molecules and improved treatment efficacy. …”
Section: Tme-based Stimuli-responsive Rna Delivery Systemsmentioning
confidence: 99%
“…What is more, siRNA drugs‐induced transient genetic disruption could elicit controllable and durable therapeutic safety, rather than producing the risk of changing the genome of patients induced by shRNA‐mediated nucleic acids therapy and CRISPR‐Cas9 system‐mediated gene editing. Currently, siRNA therapy has been widely used in cancer treatment, with the representative applicational direction including inhibiting EMT, [ 148 ] inhibiting angiogenesis, [ 149 ] inhibiting invasion and metastasis, [ 150 ] enhancing chemotherapy sensitivity, [ 151 ] and immune therapy. [ 152 ] However, the undesirable stability induced by ubiquitous RNase in blood circulation and the potential off‐target effects are the deficiency that needed to be solved in siRNA drug therapeutic strategy.…”
Section: Nucleic Acid Drugs For Cancer Therapymentioning
confidence: 99%
“…Nowadays, cancer has gradually become a major disease which seriously threatens the health and life of humans. As the traditional treatment, chemotherapy relies on toxic chemical groups to kill cancer cells and has been widely used for the therapy of tumor. To improve therapeutic efficacy, various prodrugs have been developed to overcome the shortcomings (such as systemic toxicity, the lack of tumor selectivity, and poor solubility) of traditional chemotherapy. Generally, the prodrugs can be activated by the tumor microenvironment (pH, , enzyme, etc.) or external stimuli (light, etc.).…”
Section: Introductionmentioning
confidence: 99%