日本国产在线专区,日欧一片内射VA在线影院,免费v在线视频在线观看,天天欢夜夜爽视频精品,久久综合综合久久久,亚洲精品国产综合野狼,国产破外女视频全集在线观看

歡迎光臨上海懋康生物科技有限公司
主頁 > 產品中心 > 蛋白質研究 > 蛋白純化與分離 > MP5436-5MGMBP (68–86)髓鞘堿性蛋白 蛋白純化
產品中心
MBP (68–86)髓鞘堿性蛋白 蛋白純化

MBP (68–86)髓鞘堿性蛋白 蛋白純化

簡要描述:

MBP (68–86)髓鞘堿性蛋白 蛋白純化 MBP,英文全名Myelin Basic Protein,中文名髓鞘堿性蛋白或髓磷脂堿性蛋白,是構成中樞神經系統(tǒng)(CNS)髓磷脂的重要成分,由少突膠質細胞和施萬細胞(Schwann cells)合成,可用作這兩種細胞的標記物。MBP是一條單鏈多肽,分子量約18.5kDa,位于致密的髓鞘和髓核中。

產品時間:2024-06-13

打印當前頁

分享到:

MBP (68–86)髓鞘堿性蛋白(68–86)


產品關鍵詞:

MBP (68–86) ;MBP (87-99) ;MOG (35-55)髓鞘少突膠質細胞糖蛋白(35-55);中樞神經系統(tǒng)(CNS);Multiple Sclerosis (MS)多發(fā)性硬化癥;實驗性自身免疫性腦脊髓炎(EAE);PLP (178-191); 


產品信息

產品名稱

產品編號

規(guī)格

價格(元)

MBP (68–86)髓鞘堿性蛋白(68–86)

MP5436-5MG

5mg

1280

MBP (68–86)髓鞘堿性蛋白(68–86)

MP5436-10MG

10mg

2180

MBP (68–86)髓鞘堿性蛋白(68–86)

MP5436-25MG

25mg

3480


產品描述

MBP,英文全名Myelin Basic Protein,中文名髓鞘堿性蛋白或髓磷脂堿性蛋白,是構成中樞神經系統(tǒng)(CNS)髓磷脂的重要成分,由少突膠質細胞和施萬細胞(Schwann cells)合成,可用作這兩種細胞的標記物。MBP是一條單鏈多肽,分子量約18.5kDa,位于致密的髓鞘和髓核中。是一種有潛力的靶向抗原,能夠誘發(fā)動物產生實驗性過敏性腦脊髓炎(EAE)。MBP的致腦炎肽隨敏感品系不同而有差異,且與MHC Class II基因型有關。


產品特性

1) 同義名:Myelin Basic Protein peptide (68–86); 髓鞘堿性蛋白肽段(68-86);

2) 分子式:C81H129N25O30

3) 分子量:1933.1

4) 純度:≥95%(HPLC)

5) 外觀:白色至類白色凍干粉

6) 溶解性:溶于水(1 mg/ml)

7) 單字母序列:YGSLPQKSQRSQDENPV

8) 三字母序列:Tyr-Gly-Ser-Leu-Pro-Gln-Lys-Ser-Gln-Arg-Ser-Gln-Asp-Glu-Asn-Pro-Val


保存與運輸方法

保存:-20 °C干燥保存,一年有效。

運輸:冰袋運輸。


注意事項

1) 本品以凍干粉形式提供,可能因量少不易觀察到。請直接加溶劑到瓶子內,低速漩渦震蕩以確保充分溶解;制備好的儲存液,根據單次用量分裝,置于-20°C避光凍存,避免反復凍融。

2) 本品的抗衡離子是三氟乙suan(TFA);

3) 為了您的安全和健康,請穿實驗服并戴一次性手套操作。


應用示例(來自文獻,僅做參考)

1)文獻來源:Liu Y, Wang H, Wang X, Mu L, Kong Q, Wang D, et al. (2013) The Mechanism of Effective Electroacupuncture on T Cell Response in Rats with Experimental Autoimmune Encephalomyelitis. PLoS ONE 8(1): e51573.    doi.org/10.1371/journal.pone.0051573


EAE模型建立:Myelin basic protein (MBP68–86) (YGSLPQKSQRSQDENPV) peptide 

Animals were divided into 4 treatment groups: (1) CFA emulsified in phosphate buffered saline (PBS) (CFA contained M. tuberculosis strain R37RA at a concentration of 20 mg/ml), (2) the EAE group consisted of rats immunized subcutaneously in the tail with 0.2 ml of 0.025 mg MBP68–86 emulsified in CFA, (3) the Zusanli acupoint (EA) immunization group that was immunized as group 2 but treated with EA, and (4) the NAL group that consisted of animals injected with naloxone (0.4 mg/kg) intravenously after electroacupuncture in 30 min. Prior to delivery, naloxone was diluted in sterile saline so that a 100 µl injection contained 250 µg of the drug. The Zusanli acupoint (ST36) is located 5 mm ventral and lateral to the anterior tubercle of the tibia. EA stimulation was applied for 30 min, started on the day of immunization, and repeated each day for a period of 21 days. Rats were scored for EAE as follows: 0, no disease; 1, piloerection; 2, loss in tail tonicity; 3, hind leg paralysis; 4, paraplegia, and 5, moribund or dead. Mean clinical scores at separate days and mean maximal scores were calculated by adding scores of individual rats and dividing by number of rats in each group.


2)文獻來源:Xiao BG, Huang YM, Yang JS, Xu LY, Link H. Bone marrow-derived dendritic cells from experimental allergic encephalomyelitis induce immune tolerance to EAE in Lewis rats. Clin Exp Immunol. 2001 Aug;125(2):300-9. doi: 10.1046/j.1365-2249.2001.01573.x. PMID: 11529923; PMCID: PMC1906114.

 

EAE模型建立:Guinea pig MBP 68–86 (YGSLPQKSQRSQDENPV) 

EAE was induced for two purposes: (i) to incite pulsing of DC in vivo with autoantigen and (ii) to observe the effects of EAE-DC-induced tolerance to EAE. Lewis rats were immunized in both hind footpads with 200 µl of inoculum containing 25 µg of MBP 68–86, 2 mg Mycobacterium tuberculosis (strain H37RA; Difco, Detroit, MI), 100 µl saline and 100 µl Freund's incomplete adjuvant (Difco). On day 7 post-immunization (p.i.), BM DC representing ‘in vivo pulsed DC’ were prepared.

For the clinical evaluation of EAE and DC-induced tolerance to EAE, clinical scores of EAE were graded as follows: 0, asymptomatic; 1, loss of distal half of tail tonicity; 2, loss of entire tail tonicity; 3, hindlimb paresis; 4, hindlimb paralysis; 5, tetraplegia. Clinical observations of EAE were made blind by at least two investigators. All immunized animals injected with PBS (group I) developed clinical signs of EAE, with maximum symptoms around day 14 p.i., followed by clinical improvement and recovery on day 20 p.i. (Fig. 2a).

 


 — —Written/Edited by V. Shallan【版權歸MKBio懋康所有】


 

 

上海懋康生物科技有限公司是一家涉足于生命科學和生物技術領域研究的試劑、儀器和實驗室消耗品與實驗服務工作,主要從事細胞生物學、植物學、分子生物學、免疫學、生物化學、蛋白組學。生物制藥與診斷試劑研發(fā)生產等領域。 本公司秉承“以人為本,以誠為信、合同守信"的經營理念。堅持"品質保障"的原則為廣大客戶提供優(yōu)質產品。

MBP (68–86)髓鞘堿性蛋白 蛋白純化MBP (68–86)髓鞘堿性蛋白 蛋白純化

留言框

  • 產品:

  • 您的單位:

  • 您的姓名:

  • 聯系電話:

  • 常用郵箱:

  • 省份:

  • 詳細地址:

  • 補充說明:

  • 驗證碼:

    請輸入計算結果(填寫阿拉伯數字),如:三加四=7
  • © 2019 上海懋康生物科技有限公司 版權所有 技術支持:環(huán)保在線
  • 電 話:18616957973 傳 真:86-021-54736159 QQ號碼:1563822900 郵 箱:2971634497@qq.com 地 址:上海市閔行區(qū)虹梅南路2588號綠亮科創(chuàng)園1幢A棟321室
  • 備案號:滬ICP備16016464號-3 總訪問量:528070
在線客服 聯系方式

服務熱線

18616957973

<tt id="qhynb"></tt>

<tt id="qhynb"></tt>
<var id="qhynb"></var>
<menuitem id="qhynb"></menuitem>

    <tt id="qhynb"><form id="qhynb"><listing id="qhynb"></listing></form></tt>
    <sup id="qhynb"><li id="qhynb"></li></sup><samp id="qhynb"></samp>
      <sup id="qhynb"></sup>

      1. 日本国产在线专区,日欧一片内射VA在线影院,免费v在线视频在线观看,天天欢夜夜爽视频精品,久久综合综合久久久,亚洲精品国产综合野狼,国产破外女视频全集在线观看 思思99热在线观看 免费只有精品久久 97一期涩涩97片久久久久久久 男人的资源无码专区 天天cao视频一区 99高清国产自产拍 麻豆精品久久精品色综合