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在运输过程中用聚乙二醇和谷胱甘肽控制冷冻保存静脉移植物中的移植血管病变。

Controlling transplant vasculopathy in cryopreserved vein grafts with polyethylene glycol and glutathione during transport.

作者信息

Davies M G, Huynh T T, Fulton G J, Svendsen E, Brockbank F G, Hagen P O

机构信息

Vascular Biology and Atherosclerosis Research Laboratory, Department of Surgery, Durham, North Carolina 27710, USA.

出版信息

Eur J Vasc Endovasc Surg. 1999 Jun;17(6):493-500. doi: 10.1053/ejvs.1999.0793.

Abstract

BACKGROUND

the biological characteristics of cryopreserved allografts are poorly understood, although many factors are known to influence their outcome. This study examines the development of transplant vasculopathy in both fresh and cryopreserved vein allografts and specifically assesses the efficacy of a transport solution containing 10% polyethylene glycol and 10 microM glutathione (PEG/GSH).

METHODS

jugular veins were harvested from control donor rabbits and transplanted as interposition carotid bypass grafts in 30 New Zealand White (NZW) rabbits. Ten received the fresh jugular veins (fresh). Ten animals received jugular veins which had been harvested, transported in a physiological solution, cryopreserved and stored in a standard fashion (cryopreserved). Ten animals received jugular veins which had been harvested, transported in the same solution with the addition of PEG/GSH, cryopreserved and stored in a standard fashion (PEG/GSH). Cryopreserved jugular veins were stored for 6 weeks before transplantation. All animals were sacrificed 28 days postoperatively. Vein grafts were perfusion-fixed and wall dimensions were determined by planimetry.

RESULTS

all transplanted grafts were patent at harvest. The control cryopreserved vein grafts showed a 54% increase in mean intimal thickness (63+/-10 micron vs. 41+/-3 micron p<0.05) but no change in mean medial thickness (125+/-9 micron vs. 119+/-13 micron; p = N.S. ) compared to the fresh allograft. Transport of the grafts in PEG/GSH solution resulted in the abolition of the increase in intimal thickness (41+/-4 micron; p <0.01) associated with cryopreservation without a change in medial thickness (140+/-15 micron; p = N.S.) compared to the cryopreserved allograft.

CONCLUSION

cryopreserved vein grafts develop significant intimal hyperplasia compared to freshly transplanted grafts. The use of PEG/GSH in the transport solution significantly reduces this transplant graft intimal hyperplasia to that which develops in fresh grafts and may lead to improvements in the clinical use of cryopreserved veins.

摘要

背景

尽管已知许多因素会影响冷冻异体移植物的结果,但其生物学特性仍了解不足。本研究考察了新鲜和冷冻保存的静脉异体移植物中移植血管病变的发展情况,并特别评估了含有10%聚乙二醇和10微摩尔谷胱甘肽(PEG/GSH)的运输溶液的效果。

方法

从对照供体兔获取颈静脉,并作为颈总动脉间置旁路移植物移植到30只新西兰白兔(NZW)体内。10只接受新鲜颈静脉(新鲜组)。10只动物接受已获取、在生理溶液中运输、冷冻保存并以标准方式储存的颈静脉(冷冻保存组)。10只动物接受已获取、在添加了PEG/GSH的相同溶液中运输、冷冻保存并以标准方式储存的颈静脉(PEG/GSH组)。冷冻保存的颈静脉在移植前储存6周。所有动物在术后28天处死。静脉移植物进行灌注固定,并通过平面测量法确定血管壁尺寸。

结果

所有移植的移植物在取材时均通畅。与新鲜异体移植物相比,对照冷冻保存静脉移植物的平均内膜厚度增加了54%(63±10微米对41±3微米,p<0.05),但平均中膜厚度无变化(125±9微米对119±13微米;p =无显著性差异)。与冷冻保存的异体移植物相比,移植物在PEG/GSH溶液中运输可消除与冷冻保存相关的内膜厚度增加(41±4微米;p<0.01),而中膜厚度无变化(140±15微米;p =无显著性差异)。

结论

与新鲜移植的移植物相比,冷冻保存的静脉移植物会发生显著的内膜增生。在运输溶液中使用PEG/GSH可显著将这种移植移植物内膜增生减少至新鲜移植物中出现的水平,并可能改善冷冻保存静脉在临床中的应用。

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