纳米载体药物用于缓解慢性肾脏病纤维化的研究进展

来源期刊：广州医药 | 1-10 发布时间：2022-10-11 收稿时间：2025/11/13 18:16:26 阅读量：20

作者：: 李恒亦,

李冬冬,

梁鸣,

关键词：: 慢性肾脏病纳米药物肾脏递送抗纤维化治疗; chronic kidney disease nanomedicines renal delivery antifibrotic therapy

DOI：: 10.3969/j.issn.1000-8535.2022.05.001

收稿时间：: 2022-05-15
修订日期：
接收日期：
引用总数：: 0

慢性肾脏病是一类具有高发病率、高死亡率的慢性疾病群。临床上一般采用血液透析和肾脏移植治疗终末期的慢性肾脏病。研究表明,小分子药物或核酸类药物在慢性肾脏病治疗中极具潜力,但是缺乏特异性导致肾脏纤维化治疗效果有限,亟需开发新的治疗策略。纳米载体因具有良好的理化性质,被广泛应用于生物医学领域。本文综述了近年来纳米载体递送小分子或核酸类药物在慢性肾脏病中的研究进展。

1、 HUANG H, LIU Q, ZHANG T, et al. Farnesylthiosalicylic acid-loaded albumin nanoparticle alleviates renal fibrosis by inhibiting Ras/Raf1/p38 signaling pathway[J]. Int J Nanomed, 2021(16): 6441-6453.

2、 ELZOGHBY A O, SAMY W M, ELGINDY N A. Albumin-based nanoparticles as potential controlled release drug delivery systems[J]. J Control Release, 2012, 157(2): 168-182.

3、 ZHANG X, CHEN Q, ZHANG L,et al. Tubule-specific protein nanocages potentiate targeted renal fibrosis therapy[J]. J Nanobiotechnol, 2021, 19(1): 1-17.

4、 HILL B D, ZAK A, KHERA E, et al. Engineering virus-like particles for antigen and drug delivery[J]. Curr Protein Pept Sc, 2018, 19(1): 112-127.

5、 JI C, ZHANG J, ZHU Y, et al. Exosomes derived from hucMSC attenuate renal fibrosis through CK1 delta/beta-TRCP-mediated YAP degradation[J]. Cell Death Dis, 2020, 11(5): 1-10.

6、 TANG T T, LV L L, WANG B,et al. Employing macrophage-derived microvesicle for kidney-targeted delivery of dexamethasone: an efficient therapeutic strategy against renal inflammation and fibrosis[J]. Theranostics, 2019, 9(16): 4740-4755.

7、 SHARMA S, MASUD M K, KANETI Y V, et al. Extracellular vesicle nanoarchitectonics for novel drug delivery applications[J]. Small, 2021, 17(42): 2102220.

8、 TAN L, LAI X, ZHANG M, et al. A stimuli-responsive drug release nanoplatform for kidney-specific anti-fibrosis treatment[J]. Biomater Sci, 2019, 7(4): 1554-1564.

9、 TANAKA T, KOJIMA I, OHSE T, et al. Cobalt promotes angiogenesis via hypoxia-inducible factor and protects tubulointerstitium in the remnant kidney model[J]. Lab Invest, 2005, 85(10): 1292-1307.

10、 NORDQUIST L, FRIEDERICH-PERSSON M, FASCHING A, et al. Activation of hypoxia-inducible factors prevents diabetic nephropathy[J]. J Am Soc Nephrol, 2015, 26(2): 328-338.

11、 ZHENG Z, DENG G, QI C, et al. Porous Se@SiO₂ nanospheres attenuate ischemia/reperfusion (I/R)-induced acute kidney injury (AKI) and inflammation by antioxidative stress[J]. Int J Nanomed, 2019(14): 215-229.

12、 SAIFI M A, PEDDAKKULAPPAGARI C S, AHMAD A, et al. Leveraging the pathophysiological alterations of obstructive nephropathy to treat renal fibrosis by cerium oxide nanoparticles[J]. ACS Biomater Sci Eng, 2020, 6(6): 3563-3573.

13、 WANG M, ZENG F, NING F, et al. Ceria nanoparticles ameliorate renal fibrosis by modulating the balance between oxidative phosphorylation and aerobic glycolysis[J]. J Nanobiotechnol, 2022, 20(1): 1-18.

14、 NELSON B C, JOHNSON M E, WALKER M L, et al. Antioxidant cerium oxide nanoparticles in biology and medicine[J]. Antioxid, 2016, 5(2): 15.

15、 WANG P, MIN D, CHEN G, et al. Inorganic nanozymes: prospects for disease treatments and detection applications[J]. Front Chem, 2021(9):773285.

16、 MIDGLEY A C, WEI Y, ZHU D,et al. Multifunctional natural polymer nanoparticles as antifibrotic gene carriers for CKD therapy[J]. J Am Soc Nephrol, 2020, 31(10): 2292-2311.

17、 MUMPER R J, CUI Z R. Genetic immunization by jet injection of targeted pDNA-coated nanoparticles[J]. Methods, 2003, 31(3): 255-262.

18、 GENG X, ZHANG M, LAI X, et al. Small-sized cationic miRi-PCNPs selectively target the kidneys for high-efficiency antifibrosis treatment[J]. Adv Healthc Mater, 2018, 7(21): 1800558.

19、 XU Y, NIU Y, WU B, et al. Extended-release of therapeutic microRNA via a host-guest supramolecular hydrogel to locally alleviate renal interstitial fibrosis[J]. Biomaterials, 2021(275): 120902.

20、 HE Y, HUANG C, LIN X, LI J. MicroRNA-29 family, a crucial therapeutic target for fibrosis diseases[J]. Biochimie, 2013, 95(7): 1355-1359.

21、 WANG B, KOMERS R, CAREW R, et al. Suppression of microRNA-29 expression by tgf-beta 1 promotes collagen expression and renal fibrosis[J]. J Am Soc Nephrol, 2012, 23(2): 252-265.

22、 LI Y F, JING Y, HAO J, et al. MicroRNA-21 in the pathogenesis of acute kidney injury[J]. Protein Cell, 2013, 4(11): 813-819.

23、 LI C, WANG N, RAO P, et al. Role of the microRNA-29 family in myocardial fibrosis[J]. J Physiol Biochem, 2021, 77(3): 365-376.

24、 PENG B, CHEN Y, LEONG K W. MicroRNA delivery for regenerative medicine[J]. Adv Drug Delivery Rev, 2015(88): 108-122.

25、 YANG C, NILSSON L, CHEEMA M U, et al. Chitosan/siRNA nanoparticles targeting cyclooxygenase type 2 attenuate unilateral ureteral obstruction-induced kidney injury in mice[J]. Theranostics, 2015, 5(2): 110-123.

26、 STOKMAN G, QIN Y, RACZ Z, et al. Application of siRNA in targeting protein expression in kidney disease[J]. Adv Drug Delivery Rev, 2010, 62(14): 1378-1389.

27、 SUBHAN M A, TORCHILIN V P. siRNA based drug design, quality, delivery and clinical translation[J]. Nanomed-Nanotechnol, 2020(29): 102239.

28、 ZHAO Z, WANG J, MAO H Q,et al. Polyphosphoesters in drug and gene delivery[J]. Adv Drug Delivery Rev, 2003, 55(4): 483-499.

29、 BRODY H. GENE THERAPY[J]. Nature, 2018, 564(7735): S5-S5.

30、 WEI S, XU C, ZHANG Y, et al. Ultrasound assisted a peroxisome proliferator-activated receptor (PPAR)gamma agonist-loaded nanoparticle-microbubble complex to attenuate renal interstitial fibrosis[J]. Int J Nanomed, 2020(15): 7315-7327.

31、 WANG Z, LIN Q, DAI W, et al. Pioglitazone downregulates Twist-1 expression in the kidney and protects renal function of Zucker diabetic fatty rats[J]. Biomed Pharmacother, 2019(118): 109346.

32、 LIU B C, LAN H Y, LV L L. Renal Fibrosis: Mechanisms and Therapies[M]. Springer Singapore, 2019.

33、 VITIELLO P P, CARDONE C, MARTINI G, et al. Receptor tyrosine kinase-dependent PI3K activation is an escape mechanism to vertical suppression of the EGFR/RAS/MAPK pathway in KRAS-mutated human colorectal cancer cell lines[J]. J Exp Clin Canc Res, 2019, 38(1): 1-12.

34、 WANG X, DENG B, YU M, et al. Constructing a passive targeting and long retention therapeutic nanoplatform based on water-soluble, non-toxic and highly-stable core-shell poly(amino acid) nanocomplexes[J]. Biomater Sci, 2021, 9(21): 7065-7075.

35、 QIAO H, SUN M, SU Z, et al. Kidney-specific drug delivery system for renal fibrosis based on coordination-driven assembly of catechol-derived chitosan[J]. Biomaterials, 2014, 35(25): 7157-7171.

36、 LI J, ZHANG C, HE W, et al. Coordination-driven assembly of catechol-modified chitosan for the kidney-specific delivery of salvianolic acid B to treat renal fibrosis[J]. Biomater Sci, 2017, 6(1): 179-188.

37、 GUO P, WANG J, GAO W, et al. Salvianolic acid B reverses multidrug resistance in nude mice bearing human colon cancer stem cells[J]. Mol Med Rep, 2018, 18(2): 1323-1334.

38、 FAN J M, NG Y Y, HILL P A, et al. Transforming growth factor-beta regulates tubular epithelial-myofibroblast transdifferentiation in vitro[J]. Kidney Int, 1999, 56(4): 1455-1467.

39、 LI R, LI Y, ZHANG J, et al. Targeted delivery of celastrol to renal interstitial myofibroblasts using fibronectin-binding liposomes attenuates renal fibrosis and reduces systemic toxicity[J]. J Control Release, 2020(320): 32-44.

40、 LIN L, SUN Y, WANG D, et al. Celastrol ameliorates ulcerative colitis-related colorectal cancer in mice via suppressing inflammatory responses and epithelial-mesenchymal transition[J]. Front Pharmacol, 2016(6): 320.

41、 LI S, ZHANG H, CHEN K, et al. Application of chitosan/alginate nanoparticle in oral drug delivery systems: prospects and challenges[J]. Drug Deliv, 2022, 29(1): 1142-1149.

42、 WILLIAMS R M, SHAH J, NG B D, et al. Mesoscale nanoparticles selectively target the renal proximal tubule epithelium[J]. Nano Lett, 2015, 15(4): 2358-2364.

43、 SANCEY L, KOTB S, TRULLLET C, et al. Long-term in vivo clearance of gadolinium-based aguix nanoparticles and their biocompatibility after systemic injection[J]. ACS Nano, 2015, 9(3): 2477-2488.

44、 OGAWA S, OTA Z, SHIKATA K, et al. High-resolution ultrastructural comparison of renal glomerular and tubular basement membranes[J]. Am J Nephrol, 1999, 19(6): 686-693.

45、 KANWAR Y S, FARQUHAR M G. Presence of heparan sulfate in the glomerular basement membrane[J]. P Natl Acad Sci USA, 1979, 76(3), 1303-1307.

46、 SUH J H, MINER J H. The glomerular basement membrane as a barrier to albumin[J]. Nat Rev Nephrol, 2013, 9(8): 470-477.

47、 CURRY F E, ADAMSON R H. Endothelial glycocalyx: permeability barrier and mechanosensor[J]. Ann Biomed Eng, 2012, 40(4): 828-839.

48、 SATCHELL S C, BRAET F. Glomerular endothelial cell fenestrations: an integral component of the glomerular filtration barrier[J]. Am J Physiol Renal, 2009, 296(5): F947-F956.

49、 WIGHT T N, POTTER-PERIGO S. The extracellular matrix: an active or passive player in fibrosis?[J] Am J Physiol Gastr L, 2011, 301(6): G950-955.

50、 BOOR P, OSTENDORF T, FLOEGE J. Renal fibrosis: novel insights into mechanisms and therapeutic targets[J]. Nat Rev Nephrol, 2010, 6(11): 643-656.

51、 WOO K-T, CHOONG H L, WONG K-S, et al. The contribution of chronic kidney disease to the global burden of major noncommunicable diseases[J]. Kidney Int, 2012, 81(10): 1044-1045.

52、 FALKE L L, GHOLIZADEH S, GOLDSCHMEDING R, et al. Diverse origins of the myofibroblast-implications for kidney fibrosis[J]. Nat Rev Nephrol, 2015, 11(4): 233-244.

53、 STATER E P, SONAY A Y, HART C, et al. The ancillary effects of nanoparticles and their implications for nanomedicine[J]. Nat Nanotechnol, 2021, 16(11): 1180-1194.

54、 KAMALY N, HE J C, AUSIELLO D A, et al. Nanomedicines for renal disease: current status and future applications[J]. Nat Rev Nephrol, 2016, 12(12): 738-753.

55、 HUANG L, YANG J, WANG T, GAO J, et al. Engineering of small-molecule lipidic prodrugs as novel nanomedicines for enhanced drug delivery[J]. J Nanobiotechnol, 2022, 20(1): 49.

56、 ROBERTS T C, LANGER R, WOOD M J A. Advances in oligonucleotide drug delivery[J]. Nat Rev Drug Discov, 2020, 19(10): 673-694.

57、 CHEN T K, KNICELY D H, GRAMS M E. Chronic kidney disease diagnosis and management: a review[J]. J Am Med Assoc, 2019, 322(13): 1294-1304.

58、 UMPHREYS B D. Mechanisms of renal fibrosis[J]. Annu Rev Physiol, 2018(80): 309-326.

59、 FOREMAN K J, MARQUEZ N, DOLGERT A, et al. Forecasting life expectancy, years of life lost, and all-cause and cause-specific mortality for 250 causes of death: reference and alternative scenarios for 2016-40 for 195 countries and territories[J]. Lancet, 2018, 392(10159): 2052-2090.

60、 DENG Y, LI N, WU Y, et al. Global, regional, and national burden of diabetes-related chronic kidney disease from 1990 to 2019[J]. Front endocrinol, 2021(12): 672350.

61、 RUIZ-ORTEGA M, RAYEGO-MATEOS S, LAMAS S, et al. Targeting the progression of chronic kidney disease[J]. Nat Rev Nephrol, 2020, 16(5): 269-288.