Bio-inspired Ice-controlling Materials for Cryopreservation of Cells and Tissues

doi:10.6023/A21020043

Acta Chimica Sinica ›› 2021, Vol. 79 ›› Issue (6): 729-741.DOI: 10.6023/A21020043 Previous Articles Next Articles

Review

仿生控冰材料用于细胞及组织的冷冻保存

郑夏^a^,^b, 刘建亭^a, 刘樟^a, 王健君^a^,^b^,^*()

a 中国科学院化学研究所北京 100190
b 中国科学院大学北京 101407

投稿日期:2021-02-03 发布日期:2021-03-19
通讯作者: 王健君

作者简介:

郑夏, 中国科学院大学未来技术学院2019级直博生, 现于中国科学院化学研究所绿色印刷实验室攻读博士学位. 目前的研究方向为抗冻(糖)蛋白在复杂生物环境中的作用机理及低温生物样品冷冻保存.

刘建亭, 2020年毕业于中国科学院化学研究所, 获得博士学位. 现于中国科学院化学研究所从事博士后研究工作, 主要研究方向为组织、器官冷冻保存研究.

刘樟, 中国科学院化学研究所博士后. 2016年毕业于中国科学院化学研究所, 获得博士学位. 2016~2018年于以色列威兹曼研究所从事博士后研究. 2018年加入中国科学院化学研究所从事博士后研究. 研究方向为抗冻(糖)蛋白在仿生拥挤环境中的低温保护机制及其在细胞、组织冷冻保存领域的应用.

王健君, 中国科学院化学研究所研究员, 博士生导师, 国家杰出青年科学基金获得者. 1999年获华东理工大学学士学位; 2002年获华东理工大学硕士学位; 2006年获德国美因茨大学博士学位; 2007年5月担任德国马普高分子所课题组长; 2010年2月在中国科学院化学研究所工作, 任研究员/课题组长. 主要从事揭示冰晶形成分子机制、创制新型控冰材料并应用于细胞、组织和器官的冷冻保存等.

基金资助:
国家自然科学基金(51925307); 国家自然科学基金(21733010); 国家重点研发计划项目(2018YFA0208502); 中国科学院前沿科学重点研究项目(ZDBS-LYSLH031)

Bio-inspired Ice-controlling Materials for Cryopreservation of Cells and Tissues

Xia Zheng^a^,^b, Jianting Liu^a, Zhang Liu^a, Jianjun Wang^a^,^b()

a Institute of Chemistry, Chinese Academy of Sciences, Beijing 100190, China
b University of Chinese Academy of Sciences, Beijing 101407, China

Received:2021-02-03 Published:2021-03-19
Contact: Jianjun Wang
Supported by:
National Natural Science Foundation of China(51925307); National Natural Science Foundation of China(21733010); National Key R&D Program of China(2018YFA0208502); Key Research Program of Frontier Sciences, CAS(ZDBS-LYSLH031)

Cryopreservation is a science and technology of using ultra-low temperatures for the long-term storage of cells, tissues, or organs; also it ensures a recovery in function after thawing. Cryopreservation is currently the only effective method to realize long-term storage of biological samples, and it plays a critical role in areas of biomedicine such as cell therapy, regenerative medicine and organ transplantation. As the water content of cells and tissues can be as high as 70%~90%, ice formation inevitably occurs both intracellularly and extracellularly, which can be lethal because of the mechanical damage, the osmotic shock and excessive solute accumulations. Therefore, the scientific challenge of cryopreservation is to inhibit or control ice formation in the freezing/thawing processes. Traditional cryopreservation strategies use large amounts of small molecules, such as dimethyl sulfoxide (DMSO), as cryoprotectant (CPA) to permeate into the cells and prevent intracellular ice formation; which to some extends are successful in the cryopreservation of cells. However, these molecules are chemically and epigenetically toxic to cells. Meanwhile, these strategies have proved refractory for the cryopreservation of tissues and organs. Therefore, great efforts have been made for effective ice-controlling materials to regulate the ice formation during cryopreservation. In nature, many cold-acclimated species can avoid cold damage and survive in the subzero environment due to the existence of ice-regulating proteins, i.e., ice nucleating proteins (INPs) and antifreeze (glyco) proteins (AF(G)Ps). Inspired by these proteins, intensive investigations have been made to reveal the protection mechanism of the ice-regulating proteins in order to develop their mimics. It has been reported that the bio-inspired ice-controlling materials are more effective and safer CPA in cryopreservation in comparison to small organic molecules. Therefore, the present review will briefly summarize the history of cryopreservation for cells and tissues, and focus on the development of bio-inspired ice-controlling materials and their application in the cryopreservation of cells and tissues. At last, the challenges and possible directions of bio-inspired ice-controlling materials as cryoprotective agents will be briefed.

Key words: biomimetic ice-controlling material, biological sample, cryopreservation, ice-controlling protein, complex biological system

Cite this article

Xia Zheng, Jianting Liu, Zhang Liu, Jianjun Wang. Bio-inspired Ice-controlling Materials for Cryopreservation of Cells and Tissues[J]. Acta Chimica Sinica, 2021, 79(6): 729-741.

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Fig. & Tab. 8

Figure 1. Research progress of cryopreservation

Figure 2. Cryoinjury of cells during freezing and thawing in the traditional cryopreservation, mainly including the solution effect (leading to osmotic shock) and intracellular ice formation (leading to breakdown of intracellular structures)

Figure 3. (A) Relationship between the concentration of strong hydration molecules and glass transition temperature of the system. (B) During cryopreservation, the damage effect of CPA to genomes[79], Copyright 2013, FASEB; proteins[78], Copyright 2016, American Chemical Society; organelles[55], Copyright 2020, American Chemical Society; cytoskeleton[73], Copyright 2014, Elsevier; and intercellular matrix [84], Copyright 2019, Public Library of Science, etc.

Figure 4. Representative creatures living in cold regions of nature. (A) Alaska wood frog (Rana sylvatica)[93](Photo by Janet Storey). (B) Beetle[129], Copyright 2016, National Academy of Sciences. (C) Polar fish[42] (Photo by Paul Dayton). (D) Snow fleas[99] (Photo by Peter L. Davies)

Figure 5. The mechanism of AFPs controlling the growth of ice crystal. (A) The ice-binding face (IBF) and non-ice-binding face (NIBF) of AFPs were fixed selectively for the investigation of the surface property[129]. Copyright 2016, National Academy of Sciences. (B) Schematic illustration of the fully spreading of AFPs at the ice/water interface to maximize the efficacy in controlling ice crystal growth[131]. Copyright 2018, American Chemical Society.

Figure 6. Probing the critical nucleus size for ice formation with graphene oxide nanosheets[133]. Copyright 2019, Springer Nature. (A) Schematic representation of antifreeze protein and ice nucleation protein, both have similar lattice characteristics with that of ice crystal, but have obvious difference in size. (B) a, Illustration of GO nanosheets. Carbon, grey; oxygen, red; hydrogen, white. b~f, TEM images of various-sized GOs. All the scale bars are 20 nm. The insets in b~f are the corresponding size distributions of the GOs. (C) The free-energy barrier is compared with the one obtained from the CNT calculation with typical assumptions of GO characteristics. Data show the abrupt change in TIN in the free-energy barrier of ice nucleation on GO nanosheets at LΔT≈200 nm?K, which corresponding to the nucleation size on the water/substrate interface. (D) Mechanism diagram of critical ice nucleus detected by GO nanosheets

Figure 7. The unique ice-control properties of biomimetic two-dimen- sional graphene oxide[54,146]. Copyright 2017, Wiley-VCH Verlag GmbH & Co. KGaA; Copyright 2020, Royal Society of Chemistry. (A) Highly active TmAFP, its ice binding sites correspond to methyl and hydroxyl groups, of which C is light blue, H is white, O is red and the main chain of protein is cyan band. (B) The top and side views of the biomimetic graphene oxide structure, where C is light blue and H is white, O is red. (C) GOs modify the morphology of ice crystals and has a thermal hysteresis value. (D) GOs lower the freezing point and generate thermal hysteresis (TH)

Figure 8. Recent development of biomimetic ice-controlling materials for the cryopreservation of biological cells. (A) Structure of diblock copolymer worms. (B) RBC recovery post freeze/thaw as judged by haemolysis assay. Worms 5% (w/w), HES 20% (w/w), PVA 1 mg?mL–1[157]; Copyright 2016, Wiley-VCH Verlag GmbH & Co. KGaA. (C) The structural formula of L-proline oligomers and its distribution after FITC labeling during oocytes cryopreservation. (D) Survival rates of mouse oocyte CP with VM, Cm-P, Cm-P3, Cm-P8, and Cm-P15, as the CPA respectively[55]; Copyright 2020, American Chemical Society. (E) GO nanosheets are adsorbed on the ice crystal surface due to the lattice matching through hydrogen bonds to produce curvatures on ice surface, inhibiting the growth of ice crystals. (F) The motility of cryopreserved horse sperm with different cryoprotectants[54]. Copyright 2017, Wiley-VCH Verlag GmbH & Co. KGaA.

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	(闫琳, 任永硕, 王雪靖, 穆韡, 韩晓军, 化学学报, 2020, 78, 1150.) doi: 10.6023/A20060253

仿生控冰材料用于细胞及组织的冷冻保存

Bio-inspired Ice-controlling Materials for Cryopreservation of Cells and Tissues

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