کد مقاله | کد نشریه | سال انتشار | مقاله انگلیسی | نسخه تمام متن |
---|---|---|---|---|
5756164 | 1622544 | 2017 | 13 صفحه PDF | دانلود رایگان |
عنوان انگلیسی مقاله ISI
Imbalanced immune responses involving inflammatory molecules and immune-related pathways in the lung of acute and subchronic arsenic-exposed mice
ترجمه فارسی عنوان
پاسخ های ایمنی ناسازگار شامل مولکول های التهابی و مسیرهای مربوط به ایمنی در ریه موش های آرسنیک حاد و زیر سیکل
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کلمات کلیدی
Nrf2−/−CATNrf2GSHHO-1MMP-9PVDFBCALSDOVAHClMMADMAIL-1βJnkNF-κBT helper type 1MDATBARAHRHeme oxygenase-1TregTh1PBSTIMP-1BSA - BSAc-Jun N-terminal kinases - C-Jun N-terminal kinasesMPO - DFOERK1/2 - ERK1 / 2GSH-Px - GSH-PXH&E - H & EMAPKs - MAPK هاROS - ROSγ-glutamyl cysteine synthetase - γ-گلوتامیل سیتستین سنتتازArsenic - آرسنیکbicinchoninic acid assay - آزمون اسید بیستینکونینیکbovine serum albumin - آلبومین سرم گاوdimethylarsinic acid - اسید دی متیلارسینیکmonomethylarsonic acid - اسید مونومیتیلارسونیکhydrochloric acid - اسید هیدروکلریک یا اسید کلریدریک یا جوهر نمک Ovalbumin - اوبلبومینInterleukin-1β - اینترلوکین-1βBALF - بافتCOPD - بیماری مزمن انسدادی ریهChronic obstructive pulmonary disease - بیماری مزمن انسدادی ریهANOVA - تحلیل واریانس Analysis of varianceEnzyme-linked immunosorbent assay - تست الیزاELISA - تست الیزاOxidative stress - تنش اکسیداتیوtumor necrosis factor-α - تومور نکروز عامل αLung - ریهNF-E2-related factor 2 - عامل NF-E2 2TNF-α - فاکتور نکروز توموری آلفاnuclear factor kappa B - فاکتور هسته ای کاپا BPhosphate buffered saline - فسفات بافر شورlactate dehydrogenase - لاکتات دهیدروژناز LDH - لاکتات دهیدروژناز به صورت مختصر شده LDH matrix metalloproteinase - ماتریکس متالوپروتئینازmalondialdehyde - مالون دی آلدهیدbroncho-alveolar lavage fluid - مایع شستشوی برونکو-آلوئولارlimit of detection - محدودیت تشخیصRegulatory T - مقررات TTissue inhibitor of metalloproteinase - مهار کننده های متالوپروتئیناز بافتmyeloperoxidase - میلوپراکسیداز hematoxylin-eosin - هماتوکسیلین ائوزینImmune responses - پاسخ های ایمنیPolyvinylidene fluoride - پلی وینیلیدین فلورایدCatalase - کاتالازTotal arsenic - کل آرسنیکGlutathione - گلوتاتیونglutathione reductase - گلوتاتیون ردوکتازglutathione peroxidase - گلوتاتیون پراکسیدازReactive oxygen species - گونههای فعال اکسیژن
موضوعات مرتبط
علوم زیستی و بیوفناوری
علوم محیط زیست
بهداشت، سم شناسی و جهش زایی
چکیده انگلیسی
Inorganic arsenic has been claimed to increase the risk of pulmonary diseases through ingestion, as opposed to inhalation, which makes it a unique and intriguing environmental toxicant. However, the immunotoxic effects of lung, one of the targets of arsenic exposure, have not been extensively investigated in vivo. In the present study, we first confirmed that 2.5, 5 and 10 mg/kg NaAsO2 orally for 24 h dose-dependently triggered the infiltration of neutrophils, lymphocytes and macrophages in BALF. Not only the transcription activity, but also the secretion of proinflammatory cytokines IL-1β, IL-6 and TNF-α were consistently raised in the lung and BALF of acute arsenic-exposed mice. Acute oral administration of NaAsO2 also raised pulmonary MPO activity and mRNA levels of chemokine Mip-2 and Mcp-1. Meanwhile, obvious histopathological damages with inflammatory cells infiltration and erythrocyte aggregation around the capillaries were verified in the lung of mice drank arsenic-rich water freely for 3 months. Furthermore, we affirmed notable disturbance of CD4+ T-cell differentiation in the lung of acute arsenic-exposed mice, as demonstrated by up-regulated mRNA levels of regulator Gata3 and cytokine Il-4 of Th2, enhanced Foxp3 and Il-10 of Treg, down-regulated T-bet and Ifn-γ of Th1, as well as lessened Ror-γt and Il-23 of Th17. However, impressive elevation of cytokine Ifn-γ and Il-23, as well as moderate enhancement of Il-4 and Il-10 were found in the lung by subchronic arsenic administration. Finally, our present study demonstrated that both a single and sustained arsenic exposure prominently increased the expression of immune-related p38, JNK, ERK1/2 and NF-κB proteins in the lung tissue. While disrupting the pulmonary redox homeostasis by increasing MDA levels, exhausting GSH and impaired enzyme activities of CAT and GSH-Px, antioxidant regulator NRF2 and its downstream targets HO-1 and GSTO1/2 were also up-regulated by both acute and subchronic arsenic treatment. Conclusively, our present study demonstrated both acute and subchronic oral administration of arsenic triggers multiple pulmonary immune responses involving inflammatory molecules and T-cell differentiation, which might be closely associated with the imbalanced redox status and activation of immune-related MAPKs, NF-κB and anti-inflammatory NRF2 pathways.
ناشر
Database: Elsevier - ScienceDirect (ساینس دایرکت)
Journal: Environmental Research - Volume 159, November 2017, Pages 381-393
Journal: Environmental Research - Volume 159, November 2017, Pages 381-393
نویسندگان
Jinlong Li, Lu Zhao, Yang Zhang, Wei Li, Xiaoxu Duan, Jinli Chen, Yuanyuan Guo, Shan Yang, Guifan Sun, Bing Li,