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沙門氏菌H抗原 多價(jià)相2 (1,2,5,6,7)血清
廣州健侖生物科技有限公司
我司長(zhǎng)期供應(yīng)尼古丁(可替寧)檢測(cè)試劑盒,違禁品檢測(cè)試劑盒,單卡檢測(cè),3聯(lián)卡到12聯(lián)卡,可以自由組合,根據(jù)您的需求自由組合,*,性價(jià)比高,產(chǎn)品質(zhì)量很好。
保存要求:除了有特殊說明,免疫檢測(cè)產(chǎn)品應(yīng)保存在2-8°C
產(chǎn)品規(guī)格:2ml/瓶
保質(zhì)期:2年
本試劑盒主要用于對(duì)病菌細(xì)菌進(jìn)行檢測(cè),利用快速玻片凝集檢測(cè)技術(shù)
利用快速玻片凝集和對(duì)流免疫電泳(CIE)鑒定流感嗜血桿菌
沙門氏菌屬血清2ml規(guī)格
沙門氏菌屬血清2ml規(guī)格
多群沙門氏菌診斷血清價(jià)格
多群沙門氏菌診斷血清價(jià)格
沙門氏菌血清H抗原診斷血清
沙門氏菌血清H抗原診斷血清
沙門氏血清Salmonella 多價(jià)相1和2診斷血清
沙門氏血清Salmonella 多價(jià)相1和2診斷血清
沙門氏菌H抗原 多價(jià)相2 (1,2,5,6,7)血清
沙門氏菌H抗原 多價(jià)相2 (1,2,5,6,7)血清
我司還有很多種血清學(xué)診斷血清、血液檢測(cè)、免疫檢測(cè)產(chǎn)品、毒素檢測(cè)、凝集檢測(cè)、酶免檢測(cè)、層析檢測(cè)、免疫熒光檢測(cè)產(chǎn)品,。
( MOB:楊永漢)
我司還提供其它進(jìn)口或國(guó)產(chǎn)試劑盒:登革熱、瘧疾、流感、A鏈球菌、合胞病毒、腮病毒、乙腦、寨卡、黃熱病、基孔肯雅熱、克錐蟲病、違禁品濫用、肺炎球菌、軍團(tuán)菌、化妝品檢測(cè)、食品安全檢測(cè)等試劑盒以及日本生研細(xì)菌分型診斷血清、德國(guó)SiFin診斷血清、丹麥SSI診斷血清等產(chǎn)品。
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【公司名稱】 廣州健侖生物科技有限公司
【市場(chǎng)部】 楊永漢
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【騰訊 】
【公司地址】 廣州清華科技園創(chuàng)新基地番禺石樓鎮(zhèn)創(chuàng)啟路63號(hào)二期2幢101-103
后切除三分子葡萄糖和一分子甘露糖→進(jìn)入高爾基體Cis面膜囊→N-乙酰葡糖胺磷酸轉(zhuǎn)移酶識(shí)別溶酶體水解酶的信號(hào)斑→將N-乙酰葡糖胺磷酸轉(zhuǎn)移在~個(gè)甘露糖殘基上→在中間膜囊由N-乙酰葡萄糖苷酶切去N-乙酰葡糖胺形成M配體→與trans膜囊上的受體結(jié)合→選擇性地包裝成初級(jí)溶酶體。溶酶體與疾病編輯矽肺二氧化硅塵粒(矽[xī]塵)吸入肺泡后被巨噬細(xì)胞吞噬,含有矽塵的吞噬小體與溶酶體合并成為次級(jí)溶酶體。二氧化硅的羥基與溶酶體膜的磷脂或蛋白形成氫鍵,導(dǎo)致吞噬細(xì)胞溶酶體崩解,細(xì)胞本身也被破壞,矽塵釋出,后又被其他巨噬細(xì)胞吞噬,如此反復(fù)進(jìn)行。受損或已破壞的巨噬細(xì)胞釋放“致纖維化因子”,并激活成纖維細(xì)胞,導(dǎo)致膠原纖維沉積,肺組織纖維化。肺結(jié)核結(jié)核桿菌不產(chǎn)生內(nèi)、外毒素,也無莢膜和侵襲性酶。但是菌體成分硫酸腦苷脂能抵抗胞內(nèi)的溶菌殺傷作用,使結(jié)核桿菌在肺泡內(nèi)大量生長(zhǎng)繁殖,導(dǎo)致巨噬細(xì)胞裂解,釋放出的結(jié)核桿菌再被吞噬而重復(fù)上述過程,zui終引起肺組織鈣化和纖維化。各類溶酶體貯積癥溶酶體貯積癥(Lysosome Storage Diseases 簡(jiǎn)稱:LSDs)是由于遺傳缺陷引起的,由于溶酶體的酶發(fā)生變異,功能喪失,導(dǎo)致底物在溶酶體中大量貯積,進(jìn)而影響細(xì)胞功能,常見的貯積癥主要有以下幾類:臺(tái)-薩氏綜合征(Tay-Sachs diesease):要叫黑蒙性家族癡呆癥,溶酶體缺少氨基已糖酯酶A(β-N-hexosaminidase),導(dǎo)致神經(jīng)節(jié)甘脂GM積累(圖-),影響細(xì)胞功能,造成精神癡呆,~歲死亡。
After the removal of three molecules of glucose and a molecule of mannose → into the Golgi body Cis mask capsule → N-acetylglucosamine phosphotransferase recognition of lysosomal hydrolase signal spot → transfer of N-acetylglucosamine phosphate in ~ a nectar On the sugar residues → the N-acetylglucosidase is used to cleave N-acetylglucosamine in the intermediate membrane vesicle to form an M ligand → bind to the receptor on the trans-sac vesicle → selectively packaged into primary lysosomes. Lysosomal and disease editing Silica fume silica dust (矽[xī] dust) is inhaled by macrophages after inhalation of alveoli, and phagosomes containing haze are combined with lysosomes to form secondary lysosomes. The hydroxyl group of silica forms a hydrogen bond with the phospholipid or protein of the lysosomal membrane, which results in disintegration of the lysosome of the phagocytic cells, destruction of the cells themselves, release of dust and subsequent phagocytosis by other macrophages, and so on. . Damaged or destroyed macrophages release "fibrogenic factors" and activate fibroblasts, leading to the deposition of collagen fibers and pulmonary fibrosis. Mycobacterium tuberculosis does not produce internal and external toxins, and there are no decidua and invasive enzymes. However, the bacterial component sulfatide can resist intracellular bactericidal killing, causing the growth and reproduction of Mycobacterium tuberculosis in the alveoli, resulting in the lysis of macrophages. The released Mycobacterium tuberculosis is then phagocytosed and the above process is repeated, eventually causing lung tissue. Calcification and fibrosis. Lysosome Storage Diseases (LDDs) are caused by genetic defects. Due to the mutation and loss of function of the lysosomes, many substrates are found in lysosomes. Storage, and then affect cell function, common storage diseases are mainly the following categories: Tai-Sachs diesease: to be called Alzheimer's disease, lysosomes lack of aminohexose esterase A (β-N-hexosaminidase) causes ganglioside GM accumulation (Figure -), affects cell function, causes mental dementia, and dies at ~ year old.