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免疫调节与持续释放丁丙诺啡在卵清蛋白挑战的雌性 CD1 小鼠相关联。

Immunomodulation Associated with Sustained-release Buprenorphine in Female CD1 Mice Challenged with Ovalbumin.

机构信息

Department of Microbiology, Immunology, and Pathology, College of Veterinary Medicine and Biomedical Sciences, Colorado State University, Fort Collins, Colorado.

Department of Microbiology, Immunology, and Pathology, College of Veterinary Medicine and Biomedical Sciences, Colorado State University, Fort Collins, Colorado;, Email:

出版信息

J Am Assoc Lab Anim Sci. 2019 Sep 1;58(5):577-582. doi: 10.30802/AALAS-JAALAS-18-000135. Epub 2019 Jul 18.

DOI:10.30802/AALAS-JAALAS-18-000135
PMID:31319903
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC6774459/
Abstract

Opioid analgesics have immunomodulatory properties, which often result in immunosuppression. Sustained-release buprenorphine (SR-Bup) has recently become available as an analgesic for pain management in mice, and little is known regarding potential effects of SR-Bup on the murine immune response. To this end, we immunized female CD1 mice with ovalbumin in complete Freud adjuvant and then treated them with either saline, SR-Bup, Bup-HCl, or SR-vehicle (SR-Veh) for 18 d. Splenocytes were isolated for culture and stimulation to assess cytokine responses, and blood was collected to determine serum antibody responses to ovalbumin. In all treatment groups, levels of IL10, TNFα, and IFNγ increased in ovalbumin-stimulated splenocytes compared with unstimulated splenocytes. Cytokine responses after stimulation did not differ between treatment groups except for IL10, which was significantly higher in SR-Bup-treated mice compared with those given saline or Bup-HCl. The antibody response was significantly increased after immunization but did not differ across treatment groups, except that the response to SR-Veh was lower. These results suggest that the immunomodulatory effects of prolonged treatment with SR-Bup on innate and adaptive immunity are negligible.

摘要

阿片类镇痛药具有免疫调节特性,通常导致免疫抑制。 缓释丁丙诺啡(SR-Bup)最近已作为一种用于治疗小鼠疼痛的镇痛药上市,而关于 SR-Bup 对小鼠免疫反应的潜在影响知之甚少。 为此,我们用完全弗氏佐剂中的卵清蛋白免疫 CD1 雌性小鼠,然后用生理盐水、SR-Bup、丁丙诺啡盐酸盐或 SR-载体(SR-Veh)处理它们 18 天。 分离脾细胞进行培养和刺激,以评估细胞因子反应,并采集血液以确定血清对卵清蛋白的抗体反应。 在所有治疗组中,与未刺激的脾细胞相比,卵清蛋白刺激的脾细胞中 IL10、TNFα 和 IFNγ 的水平增加。 刺激后的细胞因子反应除了 IL10 之外,在治疗组之间没有差异,SR-Bup 治疗的小鼠中的 IL10 明显高于给予生理盐水或丁丙诺啡盐酸盐的小鼠。 免疫后抗体反应显著增加,但在治疗组之间没有差异,只是 SR-Veh 的反应较低。 这些结果表明,SR-Bup 延长治疗对先天和适应性免疫的免疫调节作用可以忽略不计。

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Cationic Liposome-Oligonucleotide Complex as an Alternative Adjuvant for Polyclonal Antibody Production in New Zealand White Rabbits ().阳离子脂质体 - 寡核苷酸复合物作为新西兰白兔多克隆抗体制备的替代佐剂()
Comp Med. 2017 Dec 1;67(6):498-503.
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To Treat or Not to Treat: The Effects of Pain on Experimental Parameters.治疗还是不治疗:疼痛对实验参数的影响。
Comp Med. 2017 Dec 1;67(6):469-482.
3
In contrast to morphine, buprenorphine enhances macrophage-induced humoral immunity and, as oxycodone, slightly suppresses the effector phase of cell-mediated immune response in mice.与吗啡相反,丁丙诺啡增强了巨噬细胞诱导的体液免疫,而羟考酮则像吗啡一样,轻微抑制了小鼠细胞介导免疫反应的效应期。
Int Immunopharmacol. 2018 Jan;54:344-353. doi: 10.1016/j.intimp.2017.11.039. Epub 2017 Dec 1.
4
Effects of buprenorphine in the adrenal, thyroid, and cytokine intra-operative responses in a rat model (): a preliminary study.丁丙诺啡对大鼠模型肾上腺、甲状腺及细胞因子术中反应的影响():一项初步研究。
Iran J Basic Med Sci. 2017 Apr;20(4):368-379. doi: 10.22038/IJBMS.2017.8576.
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Sustained-Release Buprenorphine Improves Postsurgical Clinical Condition but Does Not Alter Survival or Cytokine Levels in a Murine Model of Polymicrobial Sepsis.缓释丁丙诺啡改善术后临床状况,但不改变多微生物脓毒症小鼠模型的生存率或细胞因子水平。
Comp Med. 2016 Dec 1;66(6):455-462.
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Opioid System Modulates the Immune Function: A Review.阿片类系统对免疫功能的调节:综述
Transl Perioper Pain Med. 2016;1(1):5-13.
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Efficacy of Sustained-Release Buprenorphine in an Experimental Laparotomy Model in Female Mice.缓释丁丙诺啡在雌性小鼠实验性剖腹手术模型中的疗效
J Am Assoc Lab Anim Sci. 2016 Jan;55(1):66-73.
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Analgesia in mice with experimental meningitis reduces pain without altering immune parameters.
ALTEX. 2015;32(3):183-9. doi: 10.14573/altex.1502021. Epub 2015 Mar 24.
9
Morphine and buprenorphine do not alter leukocyte cytokine production capacity, early apoptosis, or neutrophil phagocytic function in healthy dogs.吗啡和丁丙诺啡不会改变健康犬的白细胞细胞因子产生能力、早期凋亡或中性粒细胞吞噬功能。
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