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SDF-1α - 壳聚糖硫酸葡聚糖纳米粒子的制备与表征

Published: January 22, 2015
doi:
10.3791/52323
, , , , ,
1Department of Medicine,Brigham and Women’s Hospital and Harvard Medical School, 2Laboratory for Biomaterials and Drug Delivery, Department of Anesthesiology, Division of Critical Care,Boston Children’s Hospital

Summary

The objective of this protocol is to incorporate SDF-1α, a stem cell homing factor, into dextran sulfate-chitosan nanoparticles. The resultant particles are measured for their size and zeta potential, as well as the content, activity, and in vitro release rate of SDF-1α from the nanoparticles.

Abstract

Chitosan (CS) and dextran sulfate (DS) are charged polysaccharides (glycans), which form polyelectrolyte complex-based nanoparticles when mixed under appropriate conditions. The glycan nanoparticles are useful carriers for protein factors, which facilitate the in vivo delivery of the proteins and sustain their retention in the targeted tissue. The glycan polyelectrolyte complexes are also ideal for protein delivery, as the incorporation is carried out in aqueous solution, which reduces the likelihood of inactivation of the proteins. Proteins with a heparin-binding site adhere to dextran sulfate readily, and are, in turn, stabilized by the binding. These particles are also less inflammatory and toxic when delivered in vivo. In the protocol described below, SDF-1α (Stromal cell-derived factor-1α), a stem cell homing factor, is first mixed and incubated with dextran sulfate. Chitosan is added to the mixture to form polyelectrolyte complexes, followed by zinc sulfate to stabilize the complexes with zinc bridges. The resultant SDF-1α-DS-CS particles are measured for size (diameter) and surface charge (zeta potential). The amount of the incorporated SDF-1α is determined, followed by measurements of its in vitro release rate and its chemotactic activity in a particle-bound form.

Introduction

硫酸葡聚糖(DS)和脱乙酰壳多糖(CS)与多个取代带负电荷的硫酸基(在DS)的多糖,或带正电荷的胺基(脱乙酰CS)。当在水溶液中混合时,两种多糖形成通过静电相互作用的聚电解质复合物。所得复合物可以形成大的聚集体将相分离的水溶液(沉淀),或小颗粒是水可分散的(胶体)。有助于这些成果的具体条件已被广泛研究,并进行了总结,并详细示出在最近的评论1。在这些条件下,用于生产水可分散的颗粒的两个基本要求是相反电荷的聚合物必须1)有显著不同摩尔质量;和2)被混合在一个非化学计量比。这些条件将允许由电荷产生的电荷中性络合聚合物链段中和,以分隔并形成颗粒的核,和过量的聚合物,以形成外壳1。在这个协议中所描述的聚糖颗粒旨在用于肺部递送,并且被设计成净负电荷,和纳米尺寸。的负的表面电荷降低了蜂窝颗粒2,3的吸收的可能性。纳米尺寸的颗粒有利于通过远端气道的通道。为了实现这一目标,DS在这一制备中所用的量是过量的CS(重量比3:1);和高分子量的DS(重均分子量50万)和低分子量的CS(分子量范围50-190 kDa的,75-85%脱乙酰化)被使用。

SDF-1α是干细胞归巢因子,其发挥通过其趋化活性的归巢功能。 SDF-1α起着寻和维护的造血干细胞在骨髓中的重要作用,并在招募PROGE的NITOR细胞的损伤修复4,5外围组织。 SDF-1α具有肝素结合位点在其蛋白序列,其允许蛋白结合到肝素/硫酸乙酰肝素,形式二聚体,被保护免受蛋白酶(CD26 / DPPIV)失活,并通过细胞表面受体与靶细胞相互作用6-8。 DS也有类似的结构性质肝素/硫酸乙酰肝素;因此,SDF-1α对DS中的结合将是类似于其天然的聚合物配位体。

在下面的协议中,我们描述了SDF-1α-DS-CS纳米颗粒的制备。该程序表示先前已经研究了9所述的制剂中的一个。该协议最初是改编自VEGF-DS-CS纳米粒子10进行调查。一个小规模的制备进行了说明,可以很容易地按比例放大以相同储备溶液和制备条件。制备后,该颗粒的特征在于BÝ检查其尺寸,zeta电位,SDF-1α结合的程度, 在体外释放时间,以及掺入的SDF-1α活性。

Protocol

1.准备SDF-1α聚糖纳米粒子由于在体内递送的目的,消毒的所有容器,移液管,并在制备中使用的提示。 制备下列储备溶液在超纯水:1%硫酸葡聚糖; 1 M氢氧化钠(无菌过滤用PES膜);在0.2%的冰醋酸0.1%的壳聚糖(过滤器通过0.8和0.22微米的过滤器,并连续调节pH值至5.5,用NaOH之后); 0.1M的硫酸锌; 15%甘露醇;和0.92毫克/毫升,SDF-1α(在80℃下以等分试样?…

Representative Results

所制备的SDF-1α-DS-CS粒子的大小和ζ电位均用颗粒分析仪确定的。 图1示出了尺寸测量的分析。从来自四个重复测量得到的累积的结果,所述SDF-1α-DS-CS颗粒的平均流体动力学直径是661±8.2(nm),而多分散性是0.23±0.02。 zeta电位的测量结果示于图2中 。在5次重复测量中,SDF-1α-DS-CS粒子的ζ电位为-24.8±0.5毫伏。如上所述,在SDF-1α-DS-CS粒子悬浮液的5%甘露糖醇的存在是为在一?…

Discussion

如上所述,在DS-CS纳米颗粒通过电荷中和聚阴离子(DS)和聚阳离子(CS)的分子之间形成。由于电荷相互作用的分子碰撞时容易发生时,聚合物溶液和搅拌速度的混合期间的浓度是对所产生的粒子的大小是至关重要的。一个总的趋势是,越来越稀释DS和CS的解决方案15和更高的搅拌速度导致更小的粒子。

所述SDF-1α聚糖纳米颗粒的制剂可以改变。例如,SDF-1α/ DS / CS在这?…

Divulgaciones

The authors have nothing to disclose.

Acknowledgements

HL671795,HL048743和HL108630:这项工作是由美国国立卫生研究院资助。

Materials

Name Company Catalog number
Dextran sulfate Fisher BP1585-100
Chitosan, low molecular weight  Sigma 448869
Zinc sulfate heptahydrate Sigma 204986
D-Mannitol Sigma M9546
UltraPure water  Invitrogen  10977-023
SDF-1α Prepared according to reference 8.
Syringe filter, PES membrane 0.22 um.    Millipore SLGP033RS
Magnetic Micro Stirring Bars (2 x 7 mm) Fisher  14-513-63
Glass vial Kit; SUN-SRi Fisher  14-823-182
Delsa Nano C Particle Analyzer  Backman Coulter
Eppendorf UVette Cuvets Eppendorf 952010069
4–20% Mini-PROTEAN TGX Gel Bio-Rad 456-1096
GelCode Blue Safe Protein Stain Fisher  PI-24592
Molecular Imager VersaDoc MP 4000 System BioRad 170-8640
Corning Transwell Permeable Supports Corning 3421
Accuri C6 Flow Cytometer BD Biosciences
Dulbecco’s phosphate buffered saline  Sigma D8537
Pyrogent plus kit Fisher NC9753738
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Referencias

  1. Delair, T. Colloidal polyelectrolyte complexes of chitosan and dextran sulfate towards versatile nanocarriers of bioactive molecules. Eur J Pharm Biopharm. 78 (1), 10-18 (2011).
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  3. Yue, Z. G., et al. Surface charge affects cellular uptake and intracellular trafficking of chitosan-based nanoparticles. Biomacromolecules. 12 (7), 2440-2446 (2011).
  4. Ghadge, S. K., Muhlstedt, S., Ozcelik, C., Bader, M. SDF-1alpha as a therapeutic stem cell homing factor in myocardial infarction. Pharmacol Ther. 129 (1), 97-108 (2011).
  5. Sharma, M., Afrin, F., Satija, N., Tripathi, R. P., Gangenahalli, G. U. Stromal-derived factor-1/CXCR4 signaling: indispensable role in homing and engraftment of hematopoietic stem cells in bone marrow. Stem Cells Dev. 20 (6), 933-946 (2011).
  6. Sadir, R., Baleux, F., Grosdidier, A., Imberty, A., Lortat-Jacob, H. Characterization of the stromal cell-derived factor-1alpha-heparin complex. J Biol Chem. 276 (11), 8288-8296 (2001).
  7. Amara, A., et al. Stromal cell-derived factor-1alpha associates with heparan sulfates through the first beta-strand of the chemokine. J Biol Chem. 274 (34), 23916-23925 (1999).
  8. Sadir, R., Imberty, A., Baleux, F., Lortat-Jacob, H. Heparan sulfate/heparin oligosaccharides protect stromal cell-derived factor-1 (SDF-1)/CXCL12 against proteolysis induced by CD26/dipeptidyl peptidase IV. J Biol Chem. 279 (42), 43854-43860 (1074).
  9. Yin, T., et al. SDF-1alpha in glycan nanoparticles exhibits full activity and reduces pulmonary hypertension in rats. Biomacromolecules. 14 (11), 4009-4020 (2013).
  10. Huang, M., Vitharana, S. N., Peek, L. J., Coop, T., Berkland, C. Polyelectrolyte complexes stabilize and controllably release vascular endothelial growth factor. Biomacromolecules. 8 (5), 1607-1614 (2007).
  11. McCall, R. L., Sirianni, R. W. PLGA nanoparticles formed by single- or double-emulsion with vitamin E-TPGS. J Vis Exp. (82), 51015 (2013).
  12. Carrillo-Conde, B. R., Roychoudhury, R., Chavez-Santoscoy, A. V., Narasimhan, B., Pohl, N. L. High-throughput synthesis of carbohydrates and functionalization of polyanhydride nanoparticles. J Vis Exp. (65), 3967 (2012).
  13. Xu, J., Amiji, M. Therapeutic gene delivery and transfection in human pancreatic cancer cells using epidermal growth factor receptor-targeted gelatin nanoparticles. J Vis Exp. (59), e3612 (2012).
  14. Lauten, E. H., et al. Nanoglycan complex formulation extends VEGF retention time in the lung. Biomacromolecules. 11 (7), 1863-1872 (2010).
  15. Schatz, C., Domard, A., Viton, C., Pichot, C., Delair, T. Versatile and efficient formation of colloids of biopolymer-based polyelectrolyte complexes. Biomacromolecules. 5 (5), 1882-1892 (2004).

Tags

SDF-1αChitosanDextran SulfateNanoparticlesPolyelectrolyte ComplexesProtein DeliveryStem Cell Homing

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Bader, A. R., Li, T., Wang, W., Kohane, D. S., Loscalzo, J., Zhang, Y. Preparation and Characterization of SDF-1α-Chitosan-Dextran Sulfate Nanoparticles. J. Vis. Exp. (95), e52323, doi:10.3791/52323 (2015).
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