末治脾肾,能起沉疴--单纯中药治疗乙肝相关性肝癌1例

探讨中药审因论治对乙肝相关性肝癌的治疗作用。应用调补脾肾、搜邪泄浊法 ,对一例乙肝相关性肝癌患者进行单纯中药治疗。结果 :经过 12个月治疗 ,AFP由最高 10 0 0 0 μg/L降至正常 (<2 0 μg/L) ,AFP异质体同步转阴 ,B超、MRI显示肝部实质性肿块消散 ,肝功能好转。提示本治法对肝癌具有较好的治疗作用。     

RFDD-PCR技术用于构建证的相关基因表达谱初探

目的　运用限制性酶切片段差异显示 (RFDD -PCR)技术初步筛选支气管哮喘肾虚证的相关基因 ,以冀探讨构建中医证的相关基因表达谱的一种研究方法。方法　应用RFDD -PCR技术 ,收集支气管哮喘肾虚证患者治疗前后外周血 ,分离其总RNA ,进行DNaseI处理、合成双链cDNA、TaqI限切酶酶切、在其两端连上接头、特异配对于接头的引物来降落PCR扩增、变性聚丙烯酰胺凝胶电泳、AgNO3 染色、回收差异条带并重新PCR扩增、反向斑点杂交、测序、生物信息学分析。结果　共找到 36条差异条带 ,其中 2 5条能用斑点杂交验证 ,选取 3条测序 ,结果与基因库比较未发现同源序列。结论　 3条基因片段可能是与支气管哮喘肾虚证相关的新基因 ;RFDD -PCR技术不失为构建中医证的相关基因表达谱的一种好方法。     

榛子叶化学成分研究(Π)

目的　对榛子叶中的鞣质成分进行了研究 ,开发利用黑龙江省榛子叶资源。方法　利用 1 H- NMR,1 3C- NMR,FAB- MS,CD谱及 1 H- 1 HCOSY二维谱与化学方法鉴定。结果　从中得到 4个化学成分 :榛叶素 B(heterophylliin B, ) ,tellimagrandin ( ) ,casuarictin ( ) ,casuarinin ( )。结论　榛叶素 B是一个新的鞣花二聚体成分     

HPLC研究川芎-赤芍配伍的化学成分变化

中药复方配伍理论是中药方剂的精华。中药配伍后多化学成分的变化研究尚未见报道。本文首次应用HPLC-DAD研究川芎-赤芍配伍的多化学成分变化。由于中药成分复杂,需要建立稳定、重复、可靠的液相色谱分析方法;然后用液相色谱的统一方法分离样品和数据处理;通过比较合煎液和单煎液中各成分的保留时间和紫外光谱确定合煎液中各峰的归属;并可研究配伍后化学成分含量的变化。实验结果表明,川芎-赤芍配伍后少数化学成分含量发生变化,但没有发现新峰的产生。     

Inhibition of hyperacute transplant rejection by soluble proteins with the functional domains of CD46 and FcgammaRII

BACKGROUND: Recombinant soluble forms of complement regulatory molecules, including the human complement regulatory protein CD46 (rsCD46), have been shown to inhibit hyperacute transplant rejection (HAR) and protect against complement-mediated inflammatory tissue damage. Similarly, recombinant soluble forms of the immunoglobulin receptor FcgammaRII (rsFcgammaRII) can attenuate antibody-mediated inflammatory responses. We have produced and tested the function of novel recombinant chimeric proteins that incorporate the functional domains of both CD46 (membrane cofactor protein, MCP) and the low affinity human IgG receptor FcgammaRII (CD32). METHODS: Two recombinant soluble chimeric proteins (CD46:FcR and FcR:CD46) were designed and produced using a human cell expression system. Their ability to protect cells against complement-mediated lysis (through the CD46 domain) and bind human IgG (through the Fc receptor domain) was assessed in vitro. They were also tested in vivo in the rat reverse passive Arthus reaction and a murine model of hyperacute cardiac transplant rejection. RESULTS: In vitro, the functional domains of the chimeric proteins each retained their activity. In vivo, the serum half-life of the recombinant chimeric proteins in mice was more than either rsCD46 or rsFcgammaRII. In the rat reverse passive Arthus reaction, intradermal injection of each recombinant protein substantially reduced inflammatory skin edema (>50%) and polymorphonuclear neutrophil infiltration (>90%). In the hyperacute rejection model, i.v. treatment with FcR:CD46 prevented complement-mediated rejection, macroscopic bruising, edema, and thrombosis more effectively than rsCD46. CONCLUSIONS: CD46/FcgammaRII bifunctional proteins have an improved ability to control complement-mediated hyperacute graft rejection and have therapeutic potential in other conditions involving antibody-mediated inflammation.     

胃粘膜瓣成型预防食管胃吻合术后反流的观察

目的:介绍胃粘膜瓣成型预防食管胃吻合术后反流的临床应用.方法:食管、贲门癌50例,行部分食管部分胃切除,用吻合器作食管胃吻合后行胃粘膜瓣成型.结果:成型组术后无反流症状,上消化道造影及放射性核素显像表明该手术方法抗反流作用明显.食管镜检查示胃粘膜瓣成型组吻合口粘膜充血、水肿、糜烂、溃疡较常规手术组明显减轻.结论:胃粘膜瓣成型术可有效预防食管胃吻合术后胃食管反流.     

Approval summary: Docetaxel in combination with prednisone for the treatment of androgen-independent hormone-refractory prostate cancer.

PURPOSE: Docetaxel, a taxane previously approved for the treatment of breast cancer and non-small cell lung cancer, was approved by the United States Food and Drug Administration on May 19, 2004 for use in combination with prednisone for the treatment of metastatic androgen-independent (hormone-refractory) prostate cancer. The purpose of this summary is to review the database supporting this approval. EXPERIMENTAL DESIGN: In a randomized, global study enrolling 1,006 patients, two schedules of docetaxel were compared with mitoxantrone + prednisone as follows: MTZ q 3w, mitoxantrone 12 mg/m2 every 21 days + prednisone 5 mg twice a day for a total of 10 cycles; TXT q 3w, docetaxel 75 mg/m2 every 21 days + prednisone 5 mg twice a day for a total of 10 cycles; and TXT qw, docetaxel 30 mg/m2 days 1, 8, 15, 22, and 29 every 6 weeks + prednisone 5 mg twice a day for a total of 5 cycles. RESULTS: There was a statistically significant overall survival advantage shown for the TXT q 3w arm over MTZ q 3w (median survival 18.9 months versus 16.5 months, P = 0.0094). No overall survival advantage was shown for TXT qw compared with MTZ q 3w. The most commonly occurring adverse events included anemia, neutropenia, infection, nausea, sensory neuropathy, fluid retention, alopecia, nail changes, diarrhea, and fatigue. CONCLUSIONS: This report describes the Food and Drug Administration review supporting this first approval of a combination therapy for hormone-refractory prostate cancer based on demonstration of a survival benefit.     

红细胞在抗肿瘤治疗中的作用

红细胞不仅可以运送氧、二氧化碳和清除循环免疫复合物，还能够识别、黏附、提呈肿瘤抗原，此外红细胞能够促进免疫细胞吞噬和杀伤肿瘤细胞的能力，因此红细胞在机体抗肿瘤免疫发挥重要作用。近年来，红细胞也可以开发作为药物载体治疗肿瘤，这与红细胞自身具有生物相容性和半透膜的特性有关。药物可以倍助渗透压梯度的不同、抗生素提高膜通透性，膜受体介导连接，以及交联介导连接等方法载入。已载入红细胞的药物半衰期延长，缓慢释放，受体液中酶等具有生物活性的物质降解，并且可以减轻药物毒副作用。缺点在于其靶向性单一。