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小肠黏膜下层不会促进Lobund-Wistar大鼠的PAIII肿瘤生长。

Small intestinal submucosa does not promote PAIII tumor growth in Lobund-Wistar rats.

作者信息

Hodde Jason P, Suckow Mark A, Wolter William R, Hiles Michael C

机构信息

Cook Biotech Incorporated, 3055 Kent Avenue, West Lafayette, Indiana, USA.

出版信息

J Surg Res. 2004 Aug;120(2):189-94. doi: 10.1016/j.jss.2003.10.022.

Abstract

BACKGROUND

Site-specific remodeling and angiogenesis are two observations associated with the use of small intestinal submucosa (SIS) as a tissue repair graft. Its angiogenic capacity has raised questions concerning its effect on tumor growth and metastasis in clinical tumor resection cases. The effect of SIS on the ability of neoplastic (prostate adenocarcinoma) cells to establish, grow, and metastasize was examined in Lobund-Wistar (L-W) rats.

MATERIALS AND METHODS

In one study, SIS, expanded polytetrafluoroethylene (ePTFE), or human cadaveric dermis was placed in a subcutaneous pocket on the flank of L-W rats and immediately inoculated with PA-III cell suspension. Tumors were allowed to establish and metastasize for 5 weeks prior to sacrifice. Rate of tumor growth, tumor weight, and frequency of lung metastases were assessed. In a second study, SIS was placed in a resected tumor bed and tumors were allowed to recur. Rate of tumor growth, tumor weight, and frequency of lung metastases were assessed after 3 weeks.

RESULTS

ePTFE hastened the rate of formation of palpable tumors compared to controls and other materials; cadaveric dermis and SIS did not. No differences between materials were noted in final tumor weight nor in the frequency of metastasis to the lungs. Following surgical tumor resection, residual tumor cells led to recurrence of same-site tumors in all animals, but in the defects augmented with SIS, the tumors were significantly smaller than those which regrew in the resected, unaugmented group.

CONCLUSIONS

This study demonstrates that SIS does not enhance tumor establishment, growth, or metastasis in de novo tumors. Furthermore, SIS appears to reduce the rate of tumor growth, but not metastasis, when applied in direct contact with a residual tumor bed in a rat model of prostate-related tumors.

摘要

背景

位点特异性重塑和血管生成是与使用小肠黏膜下层(SIS)作为组织修复移植物相关的两个现象。其血管生成能力引发了关于其在临床肿瘤切除病例中对肿瘤生长和转移影响的疑问。在Lobund-Wistar(L-W)大鼠中研究了SIS对肿瘤(前列腺腺癌)细胞建立、生长和转移能力的影响。

材料与方法

在一项研究中,将SIS、膨化聚四氟乙烯(ePTFE)或人尸体真皮置于L-W大鼠胁腹的皮下袋中,并立即接种PA-III细胞悬液。在处死前让肿瘤建立并转移5周。评估肿瘤生长速率、肿瘤重量和肺转移频率。在第二项研究中,将SIS置于切除的肿瘤床中,让肿瘤复发。3周后评估肿瘤生长速率、肿瘤重量和肺转移频率。

结果

与对照组和其他材料相比,ePTFE加速了可触及肿瘤的形成速率;尸体真皮和SIS则没有。在最终肿瘤重量或肺转移频率方面,未观察到材料之间的差异。手术切除肿瘤后,所有动物的残留肿瘤细胞均导致同部位肿瘤复发,但在填充SIS的缺损处,肿瘤明显小于未填充的切除组中复发的肿瘤。

结论

本研究表明,SIS不会增强原发性肿瘤的建立、生长或转移。此外,在前列腺相关肿瘤大鼠模型中,当SIS直接与残留肿瘤床接触应用时,似乎会降低肿瘤生长速率,但不会降低转移速率。

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