首页> 外文期刊>Transplantation: Official Journal of the Transplantation Society >Xenotransplantation of cells using biodegradable microcapsules.
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Xenotransplantation of cells using biodegradable microcapsules.

机译:使用可生物降解的微胶囊对细胞进行异种移植。

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摘要

BACKGROUND: The use of immunoisolation to protect transplanted cells from the immune system of the host has broad application to the treatment of major diseases such as diabetes and a wide range of other disorders resulting from functional defects of native cell systems. In most cases, limitations in functional cell longevity will necessitate periodic replenishment of the cells. We describe a hydrogel-based microcapsule that breaks down at a rate that can be adjusted to correspond to the functional longevity of the encapsulated cells. These injectable capsules can be engineered to degrade over several weeks to months for short-term drug delivery, or to remain intact and immunoprotective for more extended periods. When the supply of cells needs to be replenished, no surgery will be required to localize and remove the old capsules. METHODS: Porcine and bovine islets were immobilized in "composite" microcapsules fabricated from alginate and low-relative molecular mass (Mr) poly (L-lysine[PLL]) (Mr exclusion <120 Kd) and implanted into the peritoneum of normal and streptozotocin-induced diabetic rats. In addition to demonstrating long-term islet viability and function, a series of in vitro studies were carried out to determine the permeability and biodegradability of the microcapsules used in the present system. RESULTS: Xenogeneic islets implanted in nonimmunosuppressed rats remained in excellent condition indefinitely (>40 weeks)(viability was comparable to that of preimplant control specimens). In contrast, no islets survived in uncoated alginate spheres after 2 weeks postimplantation. By changing the concentration of the alginate, it was possible to vary the rate of capsule breakdown in rats from mechanically unstable (outer matrix <0.5-0.75% alginate) to stable for >1 year (> or =1.5% alginate). In addition to in vivo breakdown studies, the biodegradability of the capsular components was verified in vitro using a mixture of tritosomes (enzymes isolated from animal cells). CONCLUSIONS: We have designed a microcapsule system with controllable biodegradability which allows breakdown and absorption of implants when the cells die or become functionally inactive. These results may have application to other alginate-PLL encapsulation systems. The ability to cross species lines using these biodegradable microcapsules has the potential to expand dramatically the number of patients and the scope of diseases that can be successfully treated with cellular therapy.
机译:背景:使用免疫隔离保护移植的细胞免受宿主免疫系统的侵害,已广泛应用于治疗主要疾病,例如糖尿病和由天然细胞系统功能缺陷引起的其他多种疾病。在大多数情况下,功能性细胞寿命的限制将需要定期补充细胞。我们描述了一种基于水凝胶的微胶囊,该微胶囊的分解速率可以调节以对应于被囊封细胞的功能寿命。这些可注射的胶囊可经过工程改造,可在数周至数月内降解,以进行短期药物输送,或在更长的时间内保持完好无损和免疫保护。当需要补充细胞供应时,无需进行手术来定位和取出旧的胶囊。方法:将猪和牛的胰岛固定在由藻酸盐和低相对分子质量(Mr)聚(Lr-赖氨酸[PLL])(Mr排除率<120 Kd)制造的“复合”微胶囊中,并植入正常和链脲佐菌素的腹膜中诱导的糖尿病大鼠。除了证明胰岛的长期生存能力和功能外,还进行了一系列体外研究,以确定本系统中使用的微胶囊的渗透性和生物降解性。结果:植入非免疫抑制大鼠的异种胰岛无限期(> 40周)保持良好状态(生存力可与植入前对照样本媲美)。相反,在植入后2周,没有胰岛在未涂覆的藻酸盐球中存活。通过改变藻酸盐的浓度,可以将大鼠的胶囊破裂速率从机械不稳定(外部基质<0.5-0.75%海藻酸盐)改变为稳定超过1年(>或= 1.5%海藻酸盐)。除了体内分解研究外,还使用Tritosome(从动物细胞中分离的酶)的混合物在体外验证了荚膜成分的生物降解性。结论:我们设计了一种具有可控制的生物降解能力的微胶囊系统,当细胞死亡或功能失活时,它可以分解和吸收植入物。这些结果可能适用于其他藻酸盐PLL封装系统。使用这些可生物降解的微囊跨越种系的能力具有极大地扩大可以通过细胞疗法成功治疗的患者人数和疾病范围的潜力。

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