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通过不同途径注射的放射性标记人树突状细胞的生物分布。

Biodistribution of radiolabelled human dendritic cells injected by various routes.

作者信息

Quillien Véronique, Moisan Annick, Carsin Andre, Lesimple Thierry, Lefeuvre Claudia, Adamski Henri, Bertho Nicolas, Devillers Anne, Leberre Claudine, Toujas Louis

机构信息

Centre Régional de Lutte Contre le Cancer, Rennes, France.

出版信息

Eur J Nucl Med Mol Imaging. 2005 Jul;32(7):731-41. doi: 10.1007/s00259-005-1825-9.

Abstract

PURPOSE

The purpose of this study was to investigate the biodistribution of mature dendritic cells (DCs) injected by various routes, during a cell therapy protocol.

METHODS

In the context of a vaccine therapy protocol for melanoma, DCs matured with Ribomunyl and interferon-gamma were labelled with( 111)In-oxine and injected into eight patients along various routes: afferent lymphatic vessel (IL) (4 times), lymph node (IN) (5 times) and intradermally (ID) (6 times).

RESULTS

Scintigraphic investigations showed that the IL route allowed localisation of 80% of injected radioactivity in eight to ten nodes. In three cases of IN injection, the entire radioactivity stagnated in the injected nodes, while in two cases, migration to adjacent nodes was observed. This migration was detected rapidly after injection, as with IL injections, suggesting that passive transport occurred along the physiological lymphatic pathways. In two of the six ID injections, 1-2% of injected radioactivity reached a proximal lymph node. Migration was detectable in the first hour, but increased considerably after 24 h, suggesting an active migration mechanism. In both of the aforementioned cases, DCs were strongly CCR7-positive, but this feature was not a sufficient condition for effective migration. In comparison with DCs matured with TNF-alpha, IL-1beta, IL-6 and PGE2, our DCs showed a weaker in vitro migratory response to CCL21, despite comparable CCR7 expression, and higher allostimulatory and TH1 polarisation capacities.

CONCLUSION

The IL route allowed reproducible administration of specified numbers of DCs. The IN route sometimes yielded fairly similar results, but not reproducibly. Lastly, we showed that DCs matured without PGE2 that have in vitro TH1 polarisation capacities can migrate to lymph nodes after ID injection.

摘要

目的

本研究旨在探讨在细胞治疗方案中,通过不同途径注射成熟树突状细胞(DCs)后的生物分布情况。

方法

在黑色素瘤疫苗治疗方案的背景下,用Ribomunyl和干扰素-γ使其成熟的DCs用(111)铟-奥曲肽标记,并通过不同途径注射入8例患者体内:输入淋巴管(IL)(4次)、淋巴结(IN)(5次)和皮内(ID)(6次)。

结果

闪烁扫描研究表明,IL途径可使80%的注射放射性定位于8至10个淋巴结。在3例IN注射中,全部放射性停滞于注射的淋巴结内,而在2例中,观察到放射性迁移至相邻淋巴结。与IL注射一样,注射后很快检测到这种迁移,提示被动转运沿生理性淋巴途径发生。在6例ID注射中的2例中,1%-2%的注射放射性到达近端淋巴结。迁移在第1小时即可检测到,但在24小时后显著增加,提示存在主动迁移机制。在上述2例中,DCs均为CCR7强阳性,但该特征并非有效迁移的充分条件。与用肿瘤坏死因子-α、白细胞介素-1β、白细胞介素-6和前列腺素E2使其成熟的DCs相比,我们的DCs尽管CCR7表达相当,但对CCL21的体外迁移反应较弱,且具有更高的同种异体刺激和TH1极化能力。

结论

IL途径可重复给予特定数量的DCs。IN途径有时产生相当相似的结果,但不可重复。最后,我们表明,在体外具有TH1极化能力且未用前列腺素E2成熟的DCs在ID注射后可迁移至淋巴结。

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