詳細介紹
表面活性蛋白(Surfactant)
廣州健侖生物科技有限公司
肺部表面活性蛋白是一種由Ⅱ型肺泡細胞分泌的磷脂和蛋白組成的復合物,可在肺泡氣液界面降低表面張力,提供肺泡穩定所需的正常空氣流通。從肺部表面蛋白復合物中分離出來的4種蛋白A,B,C和D。 SP-A(28-36kDa)和SP-D(43kDa)都是膠原醣類結合蛋白,而SP-B(8-9kDa)和SP-C(4kDa)是非膠原的疏水蛋白。SP-B會在肺腺癌中腺泡、乳頭狀突起、細支氣管肺泡穩定增長表達。肺鱗癌、大細胞肺癌和非肺腺癌都不表達SP-B。因此此抗體在肺腺癌的研究中有意義。
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表面活性蛋白(Surfactant)
【產品介紹】
細胞定位:細胞漿
克隆號:1B9
同型:IgG
適用組織:石蠟/冰凍
陽性對照:肺腺癌
抗原修復:熱修復(EDTA)
抗體孵育時間:60min
| 產品編號 | 抗體名稱 | 克隆型別 |
| OB217 | PTEN (10號染色體缺失磷酸酶及張力蛋白同源基因) | polyclonal |
| OB218 | PTH試劑(甲狀旁腺素) | MRQ-31 |
| OB219 | PU.1(Ets蛋白轉錄因子) | EPR3158Y |
| OB220 | RCC(Renal Cell Carcinoma Marker)(腎細胞癌標記) | 66.4.C2 |
| OB221 | S100P(S100P蛋白) | 16/f5 |
| OB222 | S-100(S-100蛋白) | 4C4.9 |
| OB223 | SALL4(SALL4蛋白) | 6E3 |
| OB224 | Smoothelin(平滑肌細胞特異性抗原) | R4A |
| OB225 | SOX-10試劑(Sry相關HMG-Box基因10) | EP268 |
| OB226 | SOX-11(Sry相關HMG-Box基因11) | MRQ-58 |
| OB227 | SOX-2試劑(Sry相關HMG-Box基因2) | SP76 |
| OB228 | Stathmin試劑(微管解聚蛋白) | SP49 |
| OB229 | Surfactant(表面活性蛋白)或SP-B(Surfactant Protein B) | 1B9 |
| OB230 | Survivin(存活蛋白) | EP119 |
| OB231 | Synaptophysin(突觸素) | MRQ-40 |
| OB232 | TAG-72(腫瘤相關糖蛋白) | B72.3 |
| OB233 | Tau試劑(Tau蛋白) | polyclonal |
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【公司名稱】 廣州健侖生物科技有限公司
【市場部】 歐
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【騰訊 】
【公司地址】 廣州清華科技園創新基地番禺石樓鎮創啟路63號二期2幢101-103室



由中科院上海生命科學院/上海交大醫學院健康科學研究所金穎教授帶隊的關于“基于誘導多能干細胞技術的若干重大疾病模型與機理研究”的“973”科技部重大科學研究項目,就是希望能找到誘導iPS細胞的方法。
研究團隊首先建立了從尿液細胞、羊水細胞誘導iPS的技術平臺,中國醫學科學院血液學研究所程濤教授研究組建立了外周血細胞無基因插入的episomal方法誘導iPS的技術平臺,北京大學鄧宏魁教授研究組在世界上*在小鼠建立了*利用小分析化合物誘導iPS的技術平臺。這些技術使得建立人誘導全能干細胞更方便、更安全,為今后的臨床應用打下了重要基礎。
同時,課題組建立了多個的疾病ips細胞模型,如帕金森氏疾病、老年癡呆癥、血友病及白血病等疾病iPS細胞模型,并進行了疾病發生發展的研究,為今后的細胞治療、基因治療提供了可靠的科學依據。例如,課題組在小鼠上做了初步嘗試,iPS細胞可以成功分化為視網膜底干細胞,并且移植獲得成功。血友病的基因矯正實驗研究也正在血研所開展。
Pulmonary surfactant protein is a complex of phospholipids and proteins secreted by type II alveolar cells, which reduces surface tension at the alveolar gas-liquid interface and provides the normal air circulation required for stabilization of the alveoli. Four proteins A, B, C and D isolated from the pulmonary surface protein complex. Both SP-A (28-36 kDa) and SP-D (43 kDa) are collagen-carbohydrate binding proteins whereas SP-B (8-9 kDa) and SP-C (4 kDa) are non-collagenous hydrophobins. SP-B lung adenocarcinoma in the acinar, papillary, bronchial alveolar expression of stable growth. Lung squamous cell carcinoma, large cell lung cancer and non-lung adenocarcinoma do not express SP-B. Therefore, this antibody is of great significance in the study of lung adenocarcinoma.
"973" major scientific research project of Ministry of Science and Technology led by Professor Jin Ying of Shanghai Institutes for Biological Sciences / Shanghai Jiaotong University School of Medicine and Institute of Health Sciences, Chinese Academy of Sciences on the "Research on Several Major Disease Models and Mechanisms Based on Induced Pluripotent Stem Cell Technology" Find ways to induce iPS cells.
The research team first established a technology platform for inducing iPS from urine cells and amniotic fluid cells. The research team of professor Cheng Tao of Institute of Hematology, Chinese Academy of Medical Sciences established a technology platform for induction of iPS by episomal method of peripheral blood cell gene-free insertion. Professor Deng Hongkui of Peking University The research team is the first in the world to set up a technology platform for fully utilizing small analytical compounds to induce iPS in mice. These techniques make it more convenient and safer to establish human-induced totipotent stem cells and lay an important foundation for future clinical applications.
At the same time, the research group established a number of ips cell models of diseases, such as Parkinson's disease, Alzheimer's disease, hemophilia and leukemia and other diseases iPS cell model, and carried out the development of disease research for future cell therapy, Gene therapy provides a reliable scientific basis. For example, the group made a preliminary attempt in mice, iPS cells can be successfully differentiated into stem cells of the retina, and the transplant was successful. Hemophilia gene correction experiments are also carried out by the Institute of Blood.
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