Article(id=1220655364266184942, tenantId=1146029695717560320, journalId=1189982191388893191, issueId=1220655362521351042, articleNumber=null, orderNo=null, doi=10.16438/j.0513-4870.2020-0725, pmid=null, cstr=null, oa=null, hot=null, price=null, onlineType=0, articleFormat=0, articleType=null, articleTypeStr=research-article, receivedDate=1589126400000, receivedDateStr=2020-05-11, revisedDate=1589385600000, revisedDateStr=2020-05-14, acceptedDate=null, acceptedDateStr=null, onlineDate=1768956517520, onlineDateStr=2026-01-21, pubDate=1594483200000, pubDateStr=2020-07-12, doiRegisterDate=null, doiRegisterDateStr=null, onlineIssueDate=1768956517520, onlineIssueDateStr=2026-01-21, onlineJustAcceptDate=null, onlineJustAcceptDateStr=null, onlineFirstDate=null, onlineFirstDateStr=null, sourceXml=null, magXml=null, createTime=1768956517520, creator=13701087609, updateTime=1768956517520, updator=13701087609, issue=Issue{id=1220655362521351042, tenantId=1146029695717560320, journalId=1189982191388893191, year='2020', volume='55', issue='7', pageStart='1357', pageEnd='1706', issueExtLink='null', onlineDate='null', pubDate='null', beforeIssueId=null, nextIssueId=null, price=null, status=1, issueComplete=1, articleOrder=1, issueType=-1, specialIssue=null, createTime=1768956517105, creator=13701087609, updateTime=1768957228011, updator=13701087609, preIssue=null, nextIssue=null, ext={EN=IssueExt(id=1220658344335950505, tenantId=1146029695717560320, journalId=1189982191388893191, issueId=1220655362521351042, language=EN, specialIssueTitle=, coverIllustrator=null, specialIssueEditor=, specialIssueAbout=), CN=IssueExt(id=1220658344335950506, tenantId=1146029695717560320, journalId=1189982191388893191, issueId=1220655362521351042, language=CN, specialIssueTitle=, coverIllustrator=null, specialIssueEditor=, specialIssueAbout=)}, issueFiles=null}, startPage=1528, endPage=1539, ext={EN=ArticleExt(id=1220655364727558385, articleId=1220655364266184942, tenantId=1146029695717560320, journalId=1189982191388893191, language=EN, title=Advances in research on antitumor preparations of cardiac glycoside, columnId=1190335348648547107, journalTitle=Acta Pharmaceutica Sinica, columnName=Reviews, runingTitle=null, highlight=null, articleAbstract=
Cardiac glycoside is a class of steroidal glycosides with significant physiological activities to the heart. Several drugs had been approved for the treatment of heart failure and atrial fibrillation. In recent studies, the researchers have found that cardiac glycoside can selectively inhibit the proliferation of human tumor cells and has potent antitumor efficacy. Unfortunately, the poor solubility and severe adverse effects of cardiac glycoside hindered further clinical application in the field of anticancer. It is an effective strategy to solve the "drug-like" problem of cardiac glycoside by changing the pharmacokinetics and distribution in vivo and reducing the dosage and side effects by virtue of modern preparations technology and treatment scheme. In this review, a brief introduction of the developmental course and mechanism of cardiac glycosides in anticancer field was made, and recent research progress of cardiac glycosides preparations were summarized and discussed. Finally, the further research direction was prospected.
, correspAuthors=Hong-zhi QIAO, Li-hong HU, authorNote=null, correspAuthorsNote=null, copyrightStatement=Copyright ©2020 Acta Pharmaceutica Sinica. All rights reserved., copyrightOwner=null, extLink=null, articleAbsUrl=null, sourceXml=null, magXml=null, pdfUrl=null, pdf=null, pdfFileSize=null, pdfExtLink=null, richHtmlUrl=null, mobilePdfUrl=null, reviewReport=null, pdfFirstPage=null, abstractGraph=null, abstractGraphContent=null, abstractVideo=null, citation=null, cebUrl=null, magXmlContent=null, mapNumber=null, authorCompany=null, fund=null, authors=null, authorsList=Li-na GAO, Hong-zhi QIAO, Li-hong HU), CN=ArticleExt(id=1220655369777500686, articleId=1220655364266184942, tenantId=1146029695717560320, journalId=1189982191388893191, language=CN, title=强心苷抗肿瘤制剂的研究进展, columnId=1190335349655180086, journalTitle=药学学报, columnName=综述, runingTitle=null, highlight=null, articleAbstract=
强心苷是一类对心脏具有显著生理活性的甾体苷类化合物,曾有多个品种获批用于治疗心力衰竭和心房颤动。近年来的研究发现,强心苷可明显抑制肿瘤细胞增殖,并对人源肿瘤表现出一定的选择性。但普遍存在的水溶性差、毒副作用大等问题限制了其在抗肿瘤领域的转化应用。通过现代制剂技术和治疗方案,改变药物的体内动力学与组织分布,降低强心苷用量和毒副作用,是解决强心苷成药性问题的有效策略。本文就强心苷在抗肿瘤方面的发展历程和作用机制进行归纳,重点对其近年来新型制剂领域的研发进展进行综述,并对未来的研究方向进行展望。
, correspAuthors=乔宏志, 胡立宏, authorNote=null, correspAuthorsNote=
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Schematic illustration of the novel preparations to deliver the cardiac glycosides for reduced toxicity and enhanced antitumor efficiency , figureFileSmall=eTkw9OD/sTsZpO0+CJ9qRw==, figureFileBig=uTUNxDRjIOcIcolO7GpfcA==, tableContent=null), ArticleFig(id=1220655372533158593, tenantId=1146029695717560320, journalId=1189982191388893191, articleId=1220655364266184942, language=EN, label=null, caption=null, figureFileSmall=RcU3eYM6n2eirTLLaQbp+w==, figureFileBig=CT4o63+mem0/zM3Rhy/Sxw==, tableContent=null), ArticleFig(id=1220655372608656067, tenantId=1146029695717560320, journalId=1189982191388893191, articleId=1220655364266184942, language=CN, label=Figure 2, caption=
Schematic illustration for the fabrication of castration-resistant prostate cancer targeting micellar nanoparticles via self-assembly of the amphiphilic brush-type polymers, P(OEGMA-co-G3-C12)-g-PCL. The micelles consist of PCL as hydrophobic core and hydrophilic corona of pOEGMA and G3-C12. Hydrophobic anticancer drug, bufalin, was physically encapsulated into the hydrophobic cores of the micellar nanoparticles. p(OEGMA): Poly(oligo(ethylene glycol) monomethyl ether methacrylate; G3-C12: Peptide G3-C12 (the sequence ANTPCGPYTHDCPVKR); PCL: Poly(e-caprolactone). (Adapted from Ref. 41 with permission. Copyright © 2016 Elsevier) , figureFileSmall=RcU3eYM6n2eirTLLaQbp+w==, figureFileBig=CT4o63+mem0/zM3Rhy/Sxw==, tableContent=null), ArticleFig(id=1220655372713513669, tenantId=1146029695717560320, journalId=1189982191388893191, articleId=1220655364266184942, language=EN, label=null, caption=null, figureFileSmall=SlqjXciaw0X1IVqND5utmA==, figureFileBig=5yX3jX0fxQs2LZdyadBaEQ==, tableContent=null), ArticleFig(id=1220655372835148491, tenantId=1146029695717560320, journalId=1189982191388893191, articleId=1220655364266184942, language=CN, label=Figure 3, caption=
Illustration of the preparation route to PLTM-CS-pPLGA/Bu NPs (A); in vivo targeted bufalin delivery to a tumor site mediated by binding of P-selectin on the surface of the PLTM to CD44 receptors of the tumor cells (B). TPGS: Vitamin E polyethylene glycol succinate (pore-forming); CS: Chitosan oligosaccharide; PLGA: Poly(lactic-co-glycolic acid); PLTM: Platelet membrane; Bu: Bufalin. (Adapted from Ref. 40 with permission. Copyright © 2019 BioMed Central Ltd.) , figureFileSmall=SlqjXciaw0X1IVqND5utmA==, figureFileBig=5yX3jX0fxQs2LZdyadBaEQ==, tableContent=null), ArticleFig(id=1220655372931617488, tenantId=1146029695717560320, journalId=1189982191388893191, articleId=1220655364266184942, language=EN, label=null, caption=null, figureFileSmall=3VMCOUq8pAvfZqQMKp/xSg==, figureFileBig=Fs14RUXW/OZIwiLJ6drkNA==, tableContent=null), ArticleFig(id=1220655373049058006, tenantId=1146029695717560320, journalId=1189982191388893191, articleId=1220655364266184942, language=CN, label=Figure 4, caption=
Schematic illustration of in vivo behaviors of intratumoral injected P-Cis, including long tumor retention due to macromolecular size and dysfunctional lymphatic drainage, endocytosis into the intracellular lysosome, stimulus-responsive cisplatin release, and ultimate cytotoxicity. Dig: Digoxin; P-Cis: Cisplatin (IV) prodrug linked to the N-(2-hydroxypropyl) methacrylamide copolymer. (Adapted from Ref. 68 with permission. Copyright © 2020 American Chemical Society) , figureFileSmall=3VMCOUq8pAvfZqQMKp/xSg==, figureFileBig=Fs14RUXW/OZIwiLJ6drkNA==, tableContent=null), ArticleFig(id=1220655373162304219, tenantId=1146029695717560320, journalId=1189982191388893191, articleId=1220655364266184942, language=EN, label=null, caption=null, figureFileSmall=null, figureFileBig=null, tableContent=
| Category | Compound | Structure |
| Digoxin |  |
| Oleandrin |  |
| Ouabain |  |
| UNBS-1450 |  |
 | Bufalin |  |
| Cinobufagin |  |
| Proscillaridin A | |
), ArticleFig(id=1220655373292327648, tenantId=1146029695717560320, journalId=1189982191388893191, articleId=1220655364266184942, language=CN, label=Table 1, caption=
Typical cardiac glycosides
, figureFileSmall=null, figureFileBig=null, tableContent=
| Category | Compound | Structure |
| Digoxin |  |
| Oleandrin |  |
| Ouabain |  |
| UNBS-1450 |  |
 | Bufalin |  |
| Cinobufagin |  |
| Proscillaridin A | |
), ArticleFig(id=1220655373451711203, tenantId=1146029695717560320, journalId=1189982191388893191, articleId=1220655364266184942, language=EN, label=null, caption=null, figureFileSmall=null, figureFileBig=null, tableContent=
| Nanoplatform | Formulation | Drug | Size/nm | Tumor model* | Result | Ref |
 | Conventional liposome | Bufalin, resibufogenin, cinobufagin | ~70 | H22, Lewis | Sustained release Prolong the circulation LD50 enhanced 2.5-fold Enhance antitumor efficiency | [23] |
| Pectin-coated liposomes | Bufalin | ~300 | SW480 | Enhance stability of bufalin (BF) Increase mucosal adsorption Enhance G0/G1 block and antitumor efficiency | [24] |
| Anti-CD40 modified liposome | Bufalin | ~200 | B16 | Enhance accumulation of BF in the tumor sites Synergistically enhanced immune response Enhance targeting and reduce toxicity | [25] |
| PEGylated liposome | Bufalin, glucoevatromonoside derivative | 150-180 | Hela, A549, SGC7901, Hep G2, HL-60, SW1116, SW620, PC-3, U251, U87, MCF-7, SKBR-3, HCT116 | Improve solubility and stability Enhance cellular uptake Prolong the half-life Reduce acute toxicity Enhance antitumor efficiency | [26-28] |
| Transferrin and folic acid co-modified liposome | Bufalin | ~120 | A549 | Improve stability of BF Enhance cellular uptake Enhance antitumor efficiency | [29] |
 | Chitosan-Pluronic P123 micelle (ATB-CP) | Acetylthevetin B (ATB-CP) | 40-50 | A549 | Exert much stronger cytotoxicity Much more accumulation in the tumor Higher inhibition rate without observed cardiotoxicity | [30] |
| Vitamin E succinate-grafted-chitosan oligosaccharide/RGD conjugated TPGS mixed micelles (BU@VeC/T-RGD MM) | Bufalin | 140 | HCT116, HCT116/L-OHP, LoVo/ADR | Sustained-release pattern Higher intracellular uptake Greater cytotoxicity Enhanced apoptosis rate and P-gp efflux inhibition Enhance therapeutic efficiency | [31] |
| Hybrid peptide dendrimer micelle | Bufalin | 130 | - | Develop an amphiphilic dendrimer-based micelle Enhance solubility of BF (3.4-fold) | [32] |
| F127-based micelle | Bufalin | ~20-40 | H22, L929 | Redox responded release Enhance apoptosis and reduce systematic toxicity | [33] |
 | Wheat germ agglutinin (WGA)-grafted lipid nanoparticles | Bufalin | ~160 | Caco-2 | Enhanced the cellular uptake of nanoparticles Improve drug bioavailability (2.7-fold) | [34, 35] |
| PEG-lipid containing strophanthidin (STR-PEG-lipid) | Strophanthidin | ~80 | A549, Hep 3B, PANC1, PC3, MIN6, MCF-7, LNCaP, TOV21G, JHOC-5, JHOC-9, MDA-MB-231 | Enhance uptake in various cell types Improve marker gene silencing in vitro | [36] |
 | mPEG-PLGA-PLL-cRGD (BNPs) | Bufalin | ~160 | HUVEC, SW620 | Prolong the half-life (more 2-fold) Active target to the αv β3 integrin Improve cellular uptake and distribution in the tumor | [37] |
| Pluronic polyetherimide nanoparticles | Bufalin | ~60 | HCT116 | Controlled release and targeting to the tumor cells Inhibit the growth and metastasis of colorectal cancer | [38] |
| Biotin modified chitosan nanoparticles (Bu-BCS-NPs) | Bufalin | ~170 | MCF -7 | Linear release Enhance cytotoxicity, ROS and apoptosis Target to overexpressed biotin receptors in tumor cells | [39] |
| Chitosan -PLGA nanoparticle coated with platelet membrane (PLTM-CS-pPLGA/Bu NPs) | Bufalin | ~200 | H22, RAW 264.7 | Sustained release Enhance targeting to CD44 receptor through P-selectin Enhance cellular uptake and tumor positive targeting Enhance biodistribution in the tumor | [40] |
| P(OEGMA-co-G3-C12)-g-PCL micellar nanoparticle [BUF-NP-(G3-C12)] | Bufalin | ~70 | DU145 | Controlled release Peptide G3-C12 improved tumor accumulation and antitumor activity | [41] |
 | Octreotide-modified esterase-sensitive polymeric prodrug [P(OEGMA-co-BUF-co-Oct)] | Bufalin | ~70 | MCF-7 | Enhance cytotoxicity, cellular uptake, and apoptosis Selectively target SSTR overexpressed in tumor cells | [42] |
 | Poly(ethylene glycol)-based polymeric prodrug of BUF (PEGS-BUF) | Bufalin | - | HCT116, MDA-MB-231, A549, SMMC-7721, DU145 | Improve the water solubility and stability Exhibit comparable anticancer activity of free bufalin | [43] |
| Periplocymarin-vitamin E redox-responsive prodrug-nanoparticles (MPSSV-NPs) | Periplocymarin | ~110 | MCF-7, Hep G2, H22 | Prolong the half-life (30.04 h vs. 0.327 h) Enhance tumor distribution of PSSV-NPs Stable, redox-responsive, and low cytotoxic | [44] |
| Dipeptide (Z-Gly-Pro)-conjugated BF211 prodrug (BF211-03) | BF211 | - | HCT-116, MGC-803, MDA-MB-435, H9C2 | Sustain stable in plasma Display 30 to 40-fold lower cytotoxicity before cleavage Boost cytotoxicity after cleavage Improve selectivity by targeting FAP α | [45] |
| P(OEGMA-co-BUF-co-RGD)-g-P(DEA-co-BMA) polymeric prodrug (BUF-NP-RGD) | Bufalin | ~150 | HCT116 | Enhance cytotoxicity and apoptosis Enhance targeting and biodistribution | [46] |
 | Lipid microspheres (BU-LM) | Bufalin, resibufogenin, cinobufagin | ~180 | - | With good stability for 18 months Long-term storage for 18 months | [47] |
| Lipid microsphere (BU-LM) | Chansu | - | Hep G2, EC9706, HCT-8, BGC 803 | With good antiproliferation on human cancer cells | [48] |
 | FA-conjugated β-CD supramolecular inclusion complex (FA/BF/β-CD) | Bufalin | - | HCT116 | Enhance solubility of 24-fold Improve antitumor activity of 2-fold | [49] |
 | Peptide-dendrimer(BPDI) | Bufalin | ~140 | Caco-2 | Improve stability Enhanced intestinal permeability | [50] |
 | Oral submicron emulsion (BU-OE) | Bufalin, resibufogenin, cinobufagin | ~140 | Hep G2, HCT-8, EC9706, BGC803, GES-1, SGC7901, A549, MCF-7, HCT-116, K562 | Sustain stability for at least 18 months Improve G2/M phase and apoptosis Enhance antitumor efficiency and reduce toxicity | [51] |
| Microemulsion | Bufalin | ~40 | - | Enhance equilibrium solubility Improve absorbing ability at all intestinal segments Higher bioavailability (2.38-fold) | [52] |
 | Transdermal patch | Bufalin | - | - | Transdermal administration Sustained release at least 12 h Enhance skin permeation (22-fold) without irritation Enhance half-life and maintain the effective concentration | [53] |
), ArticleFig(id=1220655373564957414, tenantId=1146029695717560320, journalId=1189982191388893191, articleId=1220655364266184942, language=CN, label=Table 2, caption=
Novel preparations of cardiac glycoside for cancer therapy. PEG: Polyethylene glycol; cRGD: Cyclic (arginine-glycine-aspartic acid peptide); TPGS: d-alpha-Tocopheryl polyethylene glycol 1 000 succinate; PLL: Poly-L-lysine; Oct: Octreotide; p(OEGMA): Poly(oligo(ethylene glycol) monomethyl ether methacrylate; G3-C12: Peptide G3-C12 (the sequence ANTPCGPYTHDCPVKR); PCL: Poly(e-caprolactone); FA: Folic acid; β-CD: β-Cyclodextrin.*Tumor models: human cervical carcinoma: HeLa; human lung carcinoma: A549, Lewis; gastric carcinoma: SGC7901, BGC803; human liver hepatocellular carcinoma: Hep G2; leukemia: HL-60, K562; colon carcinoma: SW1116, HCT-8, HCT116, SW620, SW480, CD-26; esophageal cancer: EC9706; prostatic carcinoma: PC-3, DU145; human breast cancer: MDA-MB-231, MCF-7, SKBR-3; human colon adenocarcinoma cells: Caco-2; glioma: U251, U87; human umbilical vein endothelial cells: HUVEC; mouse macrophage: RAW 264.7; melanoma: B16; mouse hepatoma cells: H22; mouse fibroblast: L929
, figureFileSmall=null, figureFileBig=null, tableContent=
| Nanoplatform | Formulation | Drug | Size/nm | Tumor model* | Result | Ref |
 | Conventional liposome | Bufalin, resibufogenin, cinobufagin | ~70 | H22, Lewis | Sustained release Prolong the circulation LD50 enhanced 2.5-fold Enhance antitumor efficiency | [23] |
| Pectin-coated liposomes | Bufalin | ~300 | SW480 | Enhance stability of bufalin (BF) Increase mucosal adsorption Enhance G0/G1 block and antitumor efficiency | [24] |
| Anti-CD40 modified liposome | Bufalin | ~200 | B16 | Enhance accumulation of BF in the tumor sites Synergistically enhanced immune response Enhance targeting and reduce toxicity | [25] |
| PEGylated liposome | Bufalin, glucoevatromonoside derivative | 150-180 | Hela, A549, SGC7901, Hep G2, HL-60, SW1116, SW620, PC-3, U251, U87, MCF-7, SKBR-3, HCT116 | Improve solubility and stability Enhance cellular uptake Prolong the half-life Reduce acute toxicity Enhance antitumor efficiency | [26-28] |
| Transferrin and folic acid co-modified liposome | Bufalin | ~120 | A549 | Improve stability of BF Enhance cellular uptake Enhance antitumor efficiency | [29] |
 | Chitosan-Pluronic P123 micelle (ATB-CP) | Acetylthevetin B (ATB-CP) | 40-50 | A549 | Exert much stronger cytotoxicity Much more accumulation in the tumor Higher inhibition rate without observed cardiotoxicity | [30] |
| Vitamin E succinate-grafted-chitosan oligosaccharide/RGD conjugated TPGS mixed micelles (BU@VeC/T-RGD MM) | Bufalin | 140 | HCT116, HCT116/L-OHP, LoVo/ADR | Sustained-release pattern Higher intracellular uptake Greater cytotoxicity Enhanced apoptosis rate and P-gp efflux inhibition Enhance therapeutic efficiency | [31] |
| Hybrid peptide dendrimer micelle | Bufalin | 130 | - | Develop an amphiphilic dendrimer-based micelle Enhance solubility of BF (3.4-fold) | [32] |
| F127-based micelle | Bufalin | ~20-40 | H22, L929 | Redox responded release Enhance apoptosis and reduce systematic toxicity | [33] |
 | Wheat germ agglutinin (WGA)-grafted lipid nanoparticles | Bufalin | ~160 | Caco-2 | Enhanced the cellular uptake of nanoparticles Improve drug bioavailability (2.7-fold) | [34, 35] |
| PEG-lipid containing strophanthidin (STR-PEG-lipid) | Strophanthidin | ~80 | A549, Hep 3B, PANC1, PC3, MIN6, MCF-7, LNCaP, TOV21G, JHOC-5, JHOC-9, MDA-MB-231 | Enhance uptake in various cell types Improve marker gene silencing in vitro | [36] |
 | mPEG-PLGA-PLL-cRGD (BNPs) | Bufalin | ~160 | HUVEC, SW620 | Prolong the half-life (more 2-fold) Active target to the αv β3 integrin Improve cellular uptake and distribution in the tumor | [37] |
| Pluronic polyetherimide nanoparticles | Bufalin | ~60 | HCT116 | Controlled release and targeting to the tumor cells Inhibit the growth and metastasis of colorectal cancer | [38] |
| Biotin modified chitosan nanoparticles (Bu-BCS-NPs) | Bufalin | ~170 | MCF -7 | Linear release Enhance cytotoxicity, ROS and apoptosis Target to overexpressed biotin receptors in tumor cells | [39] |
| Chitosan -PLGA nanoparticle coated with platelet membrane (PLTM-CS-pPLGA/Bu NPs) | Bufalin | ~200 | H22, RAW 264.7 | Sustained release Enhance targeting to CD44 receptor through P-selectin Enhance cellular uptake and tumor positive targeting Enhance biodistribution in the tumor | [40] |
| P(OEGMA-co-G3-C12)-g-PCL micellar nanoparticle [BUF-NP-(G3-C12)] | Bufalin | ~70 | DU145 | Controlled release Peptide G3-C12 improved tumor accumulation and antitumor activity | [41] |
 | Octreotide-modified esterase-sensitive polymeric prodrug [P(OEGMA-co-BUF-co-Oct)] | Bufalin | ~70 | MCF-7 | Enhance cytotoxicity, cellular uptake, and apoptosis Selectively target SSTR overexpressed in tumor cells | [42] |
 | Poly(ethylene glycol)-based polymeric prodrug of BUF (PEGS-BUF) | Bufalin | - | HCT116, MDA-MB-231, A549, SMMC-7721, DU145 | Improve the water solubility and stability Exhibit comparable anticancer activity of free bufalin | [43] |
| Periplocymarin-vitamin E redox-responsive prodrug-nanoparticles (MPSSV-NPs) | Periplocymarin | ~110 | MCF-7, Hep G2, H22 | Prolong the half-life (30.04 h vs. 0.327 h) Enhance tumor distribution of PSSV-NPs Stable, redox-responsive, and low cytotoxic | [44] |
| Dipeptide (Z-Gly-Pro)-conjugated BF211 prodrug (BF211-03) | BF211 | - | HCT-116, MGC-803, MDA-MB-435, H9C2 | Sustain stable in plasma Display 30 to 40-fold lower cytotoxicity before cleavage Boost cytotoxicity after cleavage Improve selectivity by targeting FAP α | [45] |
| P(OEGMA-co-BUF-co-RGD)-g-P(DEA-co-BMA) polymeric prodrug (BUF-NP-RGD) | Bufalin | ~150 | HCT116 | Enhance cytotoxicity and apoptosis Enhance targeting and biodistribution | [46] |
 | Lipid microspheres (BU-LM) | Bufalin, resibufogenin, cinobufagin | ~180 | - | With good stability for 18 months Long-term storage for 18 months | [47] |
| Lipid microsphere (BU-LM) | Chansu | - | Hep G2, EC9706, HCT-8, BGC 803 | With good antiproliferation on human cancer cells | [48] |
 | FA-conjugated β-CD supramolecular inclusion complex (FA/BF/β-CD) | Bufalin | - | HCT116 | Enhance solubility of 24-fold Improve antitumor activity of 2-fold | [49] |
 | Peptide-dendrimer(BPDI) | Bufalin | ~140 | Caco-2 | Improve stability Enhanced intestinal permeability | [50] |
 | Oral submicron emulsion (BU-OE) | Bufalin, resibufogenin, cinobufagin | ~140 | Hep G2, HCT-8, EC9706, BGC803, GES-1, SGC7901, A549, MCF-7, HCT-116, K562 | Sustain stability for at least 18 months Improve G2/M phase and apoptosis Enhance antitumor efficiency and reduce toxicity | [51] |
| Microemulsion | Bufalin | ~40 | - | Enhance equilibrium solubility Improve absorbing ability at all intestinal segments Higher bioavailability (2.38-fold) | [52] |
 | Transdermal patch | Bufalin | - | - | Transdermal administration Sustained release at least 12 h Enhance skin permeation (22-fold) without irritation Enhance half-life and maintain the effective concentration | [53] |
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