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  • 產(chǎn)品詳情
    • 產(chǎn)品名稱(chēng):甩尾測痛儀

    • 產(chǎn)品型號:37360
    • 產(chǎn)品廠(chǎng)商:疼痛、炎癥
    • 產(chǎn)品價(jià)格:0
    • 折扣價(jià)格:0
    • 產(chǎn)品文檔:
    你添加了1件商品 查看購物車(chē)
    簡(jiǎn)單介紹:
    甩尾測痛儀主要是用于測量大、小鼠尾巴部受紅外熱刺激的痛覺(jué)閾值。實(shí)驗時(shí),當動(dòng)物感覺(jué)疼痛,尾巴會(huì )輕敲臺面,內置傳感器會(huì )立刻檢測到,停止計時(shí)和關(guān)閉光源,即儀器自動(dòng)記錄反應時(shí)間和光源強度。數據可通過(guò)U盤(pán)、USB數據線(xiàn)等導出。
    詳情介紹:

    甩尾測痛儀主要是用于測量大、小鼠尾巴部受紅外熱刺激的痛覺(jué)閾值。實(shí)驗時(shí),當動(dòng)物感覺(jué)疼痛,尾巴會(huì )輕敲臺面,內置傳感器會(huì )立刻檢測到,停止計時(shí)和關(guān)閉光源,即儀器自動(dòng)記錄反應時(shí)間和光源強度。數據可通過(guò)U盤(pán)、USB數據線(xiàn)等導出。


    甩尾測痛儀中有一可調強度的紅外光源,其紅外光主要是通過(guò)一拋物面反射鏡聚焦在實(shí)驗動(dòng)物的尾巴上。實(shí)驗時(shí),操作人員將實(shí)驗動(dòng)物置于儀器上,把動(dòng)物的尾巴放在紅外光源處,接受刺激。

    特征

    • 儀器自動(dòng)記錄實(shí)驗數據

    • 精度高,避免人為因素引起的誤差

    • 包含U盤(pán)和軟件


    優(yōu)點(diǎn)


    • 可獨立工作,也可連接電腦使用

    • 儀器工作臺表面無(wú)突出和遮擋物件

    • 操作方便,實(shí)驗重復性好



    規格:

    命令:軟鍵和腳踏板
    連接電腦:DELTA 9-pin連接頭,USB連線(xiàn)
    數據讀?。阂壕э@示
    電源:universal mains 85-264 VAC, 50-60Hz 
     

    打?。何⑿蜔崦舸蛴C(需另外購買(mǎi))
    工作溫度:15° - 30° C
    開(kāi)始:紅外開(kāi)關(guān)
    聲級:< 70 dB
    紅外強度:10-99級間可調
    反應時(shí)間:液晶屏顯示,分辨率為0.1s
    校準:紅外熱輻射計(需另外購買(mǎi))
    截止時(shí)間:預置,15 - 60 s間
     
     
    文獻

    關(guān)于方法
      
    - F.E. D’Amour & D.L. Smith: "A Method for Determining Loss of Pain Sensation." J. Pharmacol. Exp. Therap. 72: 74-79, 1941.
    - D.C. Yeomans & H.K. Proudfit: “Characterization of the Foot Withdrawal Response to Noxious Radiant Heat in the Rat”P(pán)ain 59: 85-97, 1994.
     
      
    涉及疼痛甩尾
     
    - C. Dawson et alia: “ Dexmedetomidine Enhances Analgesic Action of Nitrous Oxide” Anesthesiology 100 (4): 894?904, 2004
    - P. Tolu et alia: “ Effects of Long-Term Acetyl-L-carnitine Administation in Rats: I. Increased Dopamine Output in Mesocorticolimbic Areas and Protection Toward Acute Stress Exposure” Neuropsychopharmacol. 27 (3): 410-420, 2002 
    - R. Nadeson et alia: “ Potentiation by Ketamine of Fentanyl Antinociception. I. An Experimental Study in Rats Showing that Ketamine Administered by Non-Spinal Routes Targets Spinal Cord Antinociceptive Systems” Br. J. Anaesthesia 88 (5): 685?691, 2002
    - L. Jasmin et alia: “ The NK1 Receptor mediates Both the Hyperalgesia and the Resistance to Morphine in Mice Lacking Noradrenaline” PNAS 99 (2): 1029?1034, 2002
    - G.L. Fraser et alia: “ Antihyperalgesic Effects of Opioid Agonists in a Rat Model of Chronic Inflammation” Br. J. Pharmacol. 129: 1668?1672, 2000
    - M. Xu et alia: “ Effects of Radolmidine, a Novel α2- Adrenergic Agonist Compared with Dexmedetomidine in Different Pain Models in the Rat” Anesthesiology 93 (2): 473?481, 2000
    -  A. K?ster et alia: “Targeted Disruption of the Orphanin Fq/Nociceptin Gene Increases Stress Susceptibility and Impairs Stress Adaptation In Mice” Neurobiology 96 (18): 10444-10449, 1999
     
    - I. Sora et alia: “Opiate Receptor Knockout Mice Define μ Receptor Roles in Endogenous Nociceptive Responses and Morphine-Induced Analgesia” Neurobiology 94: 1544-1549, 1997
    - C.T. Dourish et alia: "The Selective CCK-B Receptor Antagonist L-365,260 Enhances Morphine Analgesia and Prevents Morphine Tolerance in the Rat" Europ. J. Pharmacol. 176: 35-44, 1990
    - P.W. Nance & J. Sawinok: "Substance P-Induced Long-Term Blockade of Spinal Adrenergic Analgesia: Reversal by Morphine and Naloxone" J. Pharmacol. Exp. Therap. Vol. 240, No. 3: 972-977,
     

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