ATP和脂多糖诱导人单核细胞释放白细胞介素-1β的药理学特性

Pharmacological characterization of ATP- and LPS-induced IL-1beta release in human monocytes.

作者信息

Grahames C B, Michel A D, Chessell I P, Humphrey P P

机构信息

Glaxo Institute of Applied Pharmacology, Department of Pharmacology, University of Cambridge, Tennis Court Rd, Cambridge CB2 1QJ.

出版信息

Br J Pharmacol. 1999 Aug;127(8):1915-21. doi: 10.1038/sj.bjp.0702732.

DOI:10.1038/sj.bjp.0702732

PMID:10482924

原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC1566177/

Abstract

We have utilized the human monocytic cell line, THP-1, and freshly isolated adherent human monocytes with the compounds pyridoxalphosphate-6-azophenyl-2',4'-disuphonic acid (PPADS), oxidized ATP, and 1-(N, O-bis[5-isoquinolinesufonyll]-N-methyl-L-tyrosyl)-4-phenylpiper azi ne (KN-62) to pharmacologically characterize the P2 receptor involved in ATP-induced release of interleukin 1beta (IL-1beta). We have also investigated the involvement of P2 receptors in lipopolysaccharide (LPS)-induced IL-1beta release from both cell types. 2. ATP caused release of IL-1beta from LPS primed THP-1 cells in both a time- and concentration-dependent manner, with a minimal effective ATP concentration of 1 mM. Stimulation of cells with 5 mM ATP resulted in detectable concentrations of IL-1beta in cell supernatants within 30 min. 3. The ATP analogue benzoylbenzoyl ATP (DBATP), a P2X7 receptor agonist, was approximately 10 fold more potent than ATP at eliciting IL-1beta release. 4. KN-62 (1 micro M), PPADS (100 microM) or oxidized ATP (100 uM) significantly inhibited 5 mM ATP-induced IL-1beta release by 81, 90 and 66% respectively, but failed to significantly inhibit LPS-induced IL-1beta release in both THP-1 cells and in freshly isolated human monocytes. 5. In both THP-1 cells and freshly isolated human monocytes, addition of the ATP degrading enzyme apyrase (0.4 U ml(-1)) to cell supernatants prior to LPS activation failed to significantly inhibit the LPS-induced IL-1beta release. In addition there was no correlation between extracellular ATP concentrations and IL-1beta release in THP-1 cells when studied over a 6 h time period. 6. In conclusion our data confirm the involvement of P2X7 receptors in ATP-induced IL-1beta release in human monocytes. However no evidence was obtained which would support the involvement of either endogenous ATP release or P2X7 receptor activation as the mechanism by which LPS-induces IL-1beta release in either the THP-1 cell line or in freshly isolated human monocytes.

摘要

我们利用人单核细胞系THP-1以及新鲜分离的贴壁人单核细胞，使用化合物磷酸吡哆醛-6-偶氮苯-2',4'-二磺酸（PPADS）、氧化ATP和1-(N,O-双[5-异喹啉磺酰基]-N-甲基-L-酪氨酰)-4-苯基哌嗪（KN-62），从药理学角度对参与ATP诱导白细胞介素1β（IL-1β）释放的P2受体进行表征。我们还研究了P2受体在脂多糖（LPS）诱导这两种细胞类型释放IL-1β过程中的作用。2. ATP以时间和浓度依赖性方式促使LPS预处理的THP-1细胞释放IL-1β，ATP的最小有效浓度为1 mM。用5 mM ATP刺激细胞30分钟内，细胞上清液中即可检测到IL-1β的浓度。3. ATP类似物苯甲酰苯甲酰ATP（DBATP）是一种P2X7受体激动剂，在引发IL-1β释放方面的效力比ATP高约10倍。4. KN-62（1 μM）、PPADS（100 μM）或氧化ATP（100 μM）分别显著抑制5 mM ATP诱导的IL-1β释放达81%、90%和66%，但未能显著抑制THP-1细胞和新鲜分离的人单核细胞中LPS诱导的IL-1β释放。5. 在THP-1细胞和新鲜分离的人单核细胞中，在LPS激活前向细胞上清液中添加ATP降解酶腺苷三磷酸双磷酸酶（0.4 U ml(-1)）未能显著抑制LPS诱导的IL-1β释放。此外，在6小时的研究时间段内，THP-1细胞中细胞外ATP浓度与IL-1β释放之间没有相关性。6. 总之，我们的数据证实P2X7受体参与人单核细胞中ATP诱导的IL-1β释放。然而，没有获得证据支持内源性ATP释放或P2X7受体激活作为LPS在THP-1细胞系或新鲜分离的人单核细胞中诱导IL-1β释放的机制。

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ATP和脂多糖诱导人单核细胞释放白细胞介素-1β的药理学特性

Pharmacological characterization of ATP- and LPS-induced IL-1beta release in human monocytes.

作者信息

Grahames C B, Michel A D, Chessell I P, Humphrey P P

机构信息

Glaxo Institute of Applied Pharmacology, Department of Pharmacology, University of Cambridge, Tennis Court Rd, Cambridge CB2 1QJ.

出版信息

Br J Pharmacol. 1999 Aug;127(8):1915-21. doi: 10.1038/sj.bjp.0702732.

DOI:10.1038/sj.bjp.0702732

PMID:10482924

原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC1566177/

Abstract

We have utilized the human monocytic cell line, THP-1, and freshly isolated adherent human monocytes with the compounds pyridoxalphosphate-6-azophenyl-2',4'-disuphonic acid (PPADS), oxidized ATP, and 1-(N, O-bis[5-isoquinolinesufonyll]-N-methyl-L-tyrosyl)-4-phenylpiper azi ne (KN-62) to pharmacologically characterize the P2 receptor involved in ATP-induced release of interleukin 1beta (IL-1beta). We have also investigated the involvement of P2 receptors in lipopolysaccharide (LPS)-induced IL-1beta release from both cell types. 2. ATP caused release of IL-1beta from LPS primed THP-1 cells in both a time- and concentration-dependent manner, with a minimal effective ATP concentration of 1 mM. Stimulation of cells with 5 mM ATP resulted in detectable concentrations of IL-1beta in cell supernatants within 30 min. 3. The ATP analogue benzoylbenzoyl ATP (DBATP), a P2X7 receptor agonist, was approximately 10 fold more potent than ATP at eliciting IL-1beta release. 4. KN-62 (1 micro M), PPADS (100 microM) or oxidized ATP (100 uM) significantly inhibited 5 mM ATP-induced IL-1beta release by 81, 90 and 66% respectively, but failed to significantly inhibit LPS-induced IL-1beta release in both THP-1 cells and in freshly isolated human monocytes. 5. In both THP-1 cells and freshly isolated human monocytes, addition of the ATP degrading enzyme apyrase (0.4 U ml(-1)) to cell supernatants prior to LPS activation failed to significantly inhibit the LPS-induced IL-1beta release. In addition there was no correlation between extracellular ATP concentrations and IL-1beta release in THP-1 cells when studied over a 6 h time period. 6. In conclusion our data confirm the involvement of P2X7 receptors in ATP-induced IL-1beta release in human monocytes. However no evidence was obtained which would support the involvement of either endogenous ATP release or P2X7 receptor activation as the mechanism by which LPS-induces IL-1beta release in either the THP-1 cell line or in freshly isolated human monocytes.

摘要

我们利用人单核细胞系THP-1以及新鲜分离的贴壁人单核细胞，使用化合物磷酸吡哆醛-6-偶氮苯-2',4'-二磺酸（PPADS）、氧化ATP和1-(N,O-双[5-异喹啉磺酰基]-N-甲基-L-酪氨酰)-4-苯基哌嗪（KN-62），从药理学角度对参与ATP诱导白细胞介素1β（IL-1β）释放的P2受体进行表征。我们还研究了P2受体在脂多糖（LPS）诱导这两种细胞类型释放IL-1β过程中的作用。2. ATP以时间和浓度依赖性方式促使LPS预处理的THP-1细胞释放IL-1β，ATP的最小有效浓度为1 mM。用5 mM ATP刺激细胞30分钟内，细胞上清液中即可检测到IL-1β的浓度。3. ATP类似物苯甲酰苯甲酰ATP（DBATP）是一种P2X7受体激动剂，在引发IL-1β释放方面的效力比ATP高约10倍。4. KN-62（1 μM）、PPADS（100 μM）或氧化ATP（100 μM）分别显著抑制5 mM ATP诱导的IL-1β释放达81%、90%和66%，但未能显著抑制THP-1细胞和新鲜分离的人单核细胞中LPS诱导的IL-1β释放。5. 在THP-1细胞和新鲜分离的人单核细胞中，在LPS激活前向细胞上清液中添加ATP降解酶腺苷三磷酸双磷酸酶（0.4 U ml(-1)）未能显著抑制LPS诱导的IL-1β释放。此外，在6小时的研究时间段内，THP-1细胞中细胞外ATP浓度与IL-1β释放之间没有相关性。6. 总之，我们的数据证实P2X7受体参与人单核细胞中ATP诱导的IL-1β释放。然而，没有获得证据支持内源性ATP释放或P2X7受体激活作为LPS在THP-1细胞系或新鲜分离的人单核细胞中诱导IL-1β释放的机制。

ATP和脂多糖诱导人单核细胞释放白细胞介素-1β的药理学特性

Pharmacological characterization of ATP- and LPS-induced IL-1beta release in human monocytes.

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ATP和脂多糖诱导人单核细胞释放白细胞介素-1β的药理学特性

Pharmacological characterization of ATP- and LPS-induced IL-1beta release in human monocytes.

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机构信息

出版信息