rhIL-8对外周血中性粒细胞功能的影响

目的 探究rhIL 8在体外对外周血中性粒细胞 (PMN)吞噬功能的影响。方法 不同浓度的rhIL 8( 1、10、10 0、10 0 0 μg/L)与受照或未受照的PMN在不同的温度条件下共同培养 ,研究PMN对细菌的吞噬功能。 结果 各种浓度的rhIL 8对PMN的吞噬功能均有增强作用 ,以 10 0 μg/L时最强 ;PMN受到 1.2Gy 6MV X线照射后吞噬功能较正常PMN无明显改变 ,rhIL 8仍能增强其吞噬功能。rhIL 8对PMN的作用 ,在温度条件为 4℃时 ,受到完全抑制 ,在 37℃时比较充分。结论 rhIL 8能显著增强外周血PMN的吞噬功能 ,在人体的温度条件下可以充分发挥其生物学功能。

可溶性噻唑盐WST-8用于重组人白细胞介素-2的生物学活性测定

运用新型测定活细胞个数的化学物质,建立一种快速测定重组人白细胞介素-2生物学活性的方法.活细胞代谢过程中,胞内的可溶性噻唑盐WST-8在电子载体1-Methoxy PMS存在时被还原成可溶性甲臢染料,甲臢染料可在A45Onm处产生吸收值,根据其吸收值的大小间接检测活细胞个数从而测定待检测样品中IL-2的浓度水平.相关性实验结果证明,在细胞浓度1250～160000个/孔范围内,CTLL-2活细胞个数与A45O值之间呈线性相关;用此种新方法检测的白细胞介素-2(IL-2)生物学活性结果与MTT法及XTT法结果基本一致,相关系数分别为r=0.9602和r=0.9511.因此, WST-8法适用于悬浮依赖型细胞CTLL-2为基础的IL-2生物学活性检测,且具有经济、实用、简便、易行的特点,有较好的实际应用价值.

白介素8和兔心肌缺血/再灌注损伤研究

目的 探讨白介素8(rhIL-8)参与兔心肌缺血/再灌注损伤的机制,为减轻再灌注损伤探索新的治疗途径。方法 结扎兔冠状动脉左前降支(left anterior descending coronary artery,LAD)造成缺血1小时,再灌注3.5小时。实验分两组:缺血/再灌注组(MI/R,n=8)和假结扎组(Sham MI/R,n=8)。结果 MI/R组发生严重的心肌损伤,包括受累心肌髓过氧化物酶(myeloperoxidase,MPO)活性增大和血清肌酸磷酸激酶-MB同工酶(CPK-MB)、异构前列腺素(eoi-PGF_(2α))水平增高(均P<0.01)。血清IL-8浓度逐渐升高,免疫组化示受损心肌区血管内皮基底膜呈IL-8阳性染色。结论 血管内皮细胞释放的IL-8是吸引中性粒细胞浸润于缺血区心肌,造成缺血/再灌注损伤的因素之一。

The Hematopoietic and Immunomodulatory Effect of rhIL-12 for Liver Cancer

Purpose: To explore the effect of rhIL-12 on the number of the blood cells and CD4/8+ T, CD45+ leukocytes, and CD56+ NK cells in liver cancer patients following radiation therapy. Methods: We selected forty liver cancer patients who carried out by cyber knife (the patients were given 5 Gy every time for 5 times continuously) to observe the size of the tumor. After thirty hours, rhIL-12 was injected into the liver cancer patients via subcutaneous at the concentration of 50 ng/kg, 100 ng/kg, 200 ng/kg and 300 ng/kg in different patients, respectively. And there were ten patients in the four groups, respectively. The twenty patients who were selected from the hospital without rhIL-12 treatment were used as controls. All the blood cells were collected from different groups on day 0, hour 12, day 7, day 14, day 21 and day 28 after rhIL-12 treatment, respectively. The full number of blood cells in every group was analyzed by ELISA. The number of CD4/8+ T, CD45+ leukocytes, and CD56+ NK cells were detected by Flow Cytometry. After one month with rhIL-12 treatment, ECOG and WHO were used to evaluate the prognosis of liver cancer. Results: In present study, we found that the number of blood cells was significantly decreased on day 0 - day 3, while recovered from day 7 - day 14 and down-regulated on day 21 after rhIL-12 treatment. The number of CD4/8+ T, CD45+ leukocytes, and CD56+ NK cells was elevated with any concentration of rhIL-12. Furthermore, results showed that number of white blood cells was obviously higher than in patients without rhIL-12 treatment (P < 0.05). However, there was no significant difference of erythrocyte and platelet, between groups treated with rhIL-12 and control groups. In addition, the immune cells including CD4/8+ T, CD45+ leukocytes, and CD56+ NK cells were reduced on day 0 - day 3, recovered from day 7, and then decreased from day 21 in rhIL-12 treatment groups related to control groups (P < 0.05). Furthermore, studies showed that five patients developed symptoms of fever, bilirubin increased and liver dysfunction with the dose of 300 ng/kg. So we found that the safe and well-tolerated human dose of 200 ng/kg is within this efficacious range based on exposure parameters through the research. Higher ECOG and WHO scores were observed in rhIL-12 treatment groups compared to control groups (P = 0.025, P = 0.044, respectively). Conclusion: Our results suggested that rhIL-12 could recover the liver cancer induced aberrant blood cell number and CD4/8+ T, CD45+ leukocytes, and CD56+ NK cells , which may be an effective method to alleviate the progress of liver cancer and played an important role in treating liver cancer.