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从实验室到临床:基因和细胞治疗的回顾及缓慢进入 3 期临床试验,重点关注 Aastrom 的 Ixmyelocel-T。

From bench to bedside: review of gene and cell-based therapies and the slow advancement into phase 3 clinical trials, with a focus on Aastrom's Ixmyelocel-T.

出版信息

Stem Cell Rev Rep. 2013 Jun;9(3):373-83. doi: 10.1007/s12015-013-9431-x.

Abstract

There is a large body of preclinical research demonstrating the efficacy of gene and cellular therapy for the potential treatment of severe (limb-threatening) peripheral arterial disease (PAD), including evidence for growth and transcription factors, monocytes, and mesenchymal stem cells. While preclinical research has advanced into early phase clinical trials in patients, few late-phase clinical trials have been conducted. The reasons for the slow progression of these therapies from bench to bedside are as complicated as the fields of gene and cellular therapies. The variety of tissue sources of stem cells (embryonic, adult bone marrow, umbilical cord, placenta, adipose tissue, etc.); autologous versus allogeneic donation; types of cells (hematopoietic, mesenchymal stromal, progenitor, and mixed populations); confusion and stigmatism by the public and patients regarding gene, protein, and stem cell therapy; scaling of manufacturing; and the changing regulatory environment all contribute to the small number of late phase (Phase 3) clinical trials and the lack of Food and Drug Administration (FDA) approvals. This review article provides an overview of the progression of research from gene therapy to the cellular therapy field as it applies to peripheral arterial disease, as well as the position of Aastrom's cellular therapy, ixmyelocel-T, within this field.

摘要

有大量的临床前研究证明基因和细胞疗法对于严重(肢体威胁性)外周动脉疾病(PAD)的潜在治疗效果,包括生长和转录因子、单核细胞和间充质干细胞的证据。虽然临床前研究已经在患者中推进到早期临床试验阶段,但很少进行后期临床试验。这些疗法从实验室到临床的进展缓慢的原因与基因和细胞疗法领域一样复杂。干细胞的组织来源多种多样(胚胎、成人骨髓、脐带、胎盘、脂肪组织等);自体与异体捐献;细胞类型(造血、间充质基质、祖细胞和混合群体);公众和患者对基因、蛋白质和干细胞治疗的混淆和污名化;制造规模的扩大;以及不断变化的监管环境,所有这些都导致了后期(第 3 阶段)临床试验的数量较少,以及食品和药物管理局(FDA)的批准不足。这篇综述文章概述了基因治疗向细胞治疗领域的研究进展,以及 Aastrom 的细胞疗法 ixmyelocel-T 在该领域的地位。

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