CN116679047A - 偶联物的制备方法 - Google Patents
偶联物的制备方法 Download PDFInfo
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- CN116679047A CN116679047A CN202310554774.8A CN202310554774A CN116679047A CN 116679047 A CN116679047 A CN 116679047A CN 202310554774 A CN202310554774 A CN 202310554774A CN 116679047 A CN116679047 A CN 116679047A
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- glucose
- phosphate dehydrogenase
- cyclosporine
- mutant
- conjugate
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- 229960000604 valproic acid Drugs 0.000 description 1
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Abstract
本申请涉及偶联物的制备方法。具体而言,本申请的6‑磷酸葡萄糖脱氢酶突变体相较于野生型6‑磷酸葡萄糖脱氢酶包含选自以下的一个突变或其组合:D306C、D375C、G426C。使用本申请的6‑磷酸葡萄糖脱氢酶突变体所制备的检测试剂盒,其特异性强、灵敏度高、操作方便、检测时间短、定量准确,适合高通量检测。
Description
本申请是2020年1月7日提交的申请号为2020100131747《6-磷酸葡萄糖脱氢酶突变体及其在制备环孢霉素A检测试剂中的用途》的分案申请。
技术领域
本申请涉及生物检测领域,特别是涉及一种突变的酶6-磷酸葡萄糖脱氢酶(简称G6PDH)及其在环孢霉素A检测试剂盒中的应用。
背景技术
半抗原,某些小分子物质(分子量小于4000Da),其单独不能诱导免疫应答,即不具备免疫原性,但当其与大分子蛋白质或非抗原性的多聚赖氨酸等载体交联或结合后可获得免疫原性,诱导免疫应答。这些小分子物质可与应答效应产物结合,具备抗原性,它只有免疫反应性,不具免疫原性,又称不完全抗原。
半抗原能与对应抗体结合出现抗原-抗体反应,又不能单独激发人或动物体产生抗体的抗原。它只有免疫反应性,不具免疫原性,又称不完全抗原。大多数多糖、类脂、激素、小分子药物都属于半抗原。如果用化学方法把半抗原与某种蛋白分子(载体)结合,会获得新的免疫原性,并能刺激动物产生相应的抗体。
小分子抗原或半抗原因缺乏可作夹心法的两个以上的位点,因此不能用双抗体夹心法进行测定,多采用竞争模式。原理是标本中的抗原和一定量的酶标抗原竞争与固相抗体结合。标本中抗原量含量愈多,结合在固相上的酶标抗原愈少,显色愈浅。小分子激素、药物等ELISA测定多用此法。
环孢霉素A(Cyclosporine A,CsA)结构式如下所示:
环孢霉素A是由真菌(多孢木霉菌或柱孢木霉菌)分泌的多种氨基酸组成的脂溶性环形肽。CsA作为具有高选择性和超低骨髓毒性的免疫抑制剂,可选择性抑制T辅助淋巴细胞的增殖和释放,同时该药物具有抗真菌活性,可有效降低患者感染情况。环孢霉素A在器官和组织移植、血液病和眼科疾病等方面具有重要临床应用价值,在器官和组织移植方面,可预防同种异体肾、肝、心、骨髓等器官或组织移植所发生的排斥反应,也可预防及治疗骨髓移植时发生的移植物抗宿主反应;在血液病方面,可应用于再生障碍性贫血、红细胞再生障碍性贫血、骨髓增生异常综合征、自身免疫性溶血性贫血等疾病;在眼科疾病方面,主要用于白塞氏综合征、干眼症、巩膜炎、过敏性结膜炎等疾病。
环孢霉素A作为钙调磷酸酶抑制剂常用药物,已成为很多难治性肾病治疗和器官移植的重要选择之一,主要分布在除大脑外的人体组织中,在血液中主要分布在红细胞和血浆中。环孢霉素A主要由肝脏代谢,已知代谢产物15种,消除半衰期10-27小时左右,代谢物主要由胆汁经粪便排泄,尿中仅0.1%以原药形式排出。
然而,由于该药物安全范围窄、代谢影响因素复杂,在药动学和药效学上存在着明显的个体差异,且血药浓度与给药量间相关性不佳,给临床治疗增加了难度,易产生肾毒性、多毛症、牙龈增生等不良反应以及不良反应个体化差异严重等问题。
基于上述原因,在治疗过程中需及时进行环孢霉素A血药浓度监测,是辅助临床治疗、改善治疗效果、降低毒性风险的有效方式。
目前已知的环孢霉素A检测方法主要有:高效液相色谱法(HPLC)、发光免疫、酶联免疫吸附剂测定(ELISA)等方法。HPLC法需要复杂的样品前处理,操作复杂周期长且成本昂贵;发光免疫法试剂成本昂贵,不适合常规治疗药物检测,更不利于大范围推广。
现有的均相酶免疫测定法、胶乳凝集比浊法常常因制备工艺复杂、批间差大,应用受到一定限制。
现有技术CN107782889A描述了一种环孢霉素A检测试剂盒,其中公开了6-磷酸葡萄糖脱氢酶和环孢霉素A偶联物的制备方法:
准确称取240mg环孢霉素A,50mg 4-苯甲酰苯甲酸,装入石英比色皿中,加入10mL叔丁醇,超声溶解;
紫外光照射3小时,反应充分,室温静置成冻干粉末;
准确称取4.5mg 6-磷酸葡萄糖脱氢酶溶于0.5mL 10mM的PBS溶液中(pH 7.4),取上述粉末(CsA-BBa)15mg溶于0.7mL的二甲基甲酰胺(DMF)溶液中,恒温25℃搅拌下将CsA-BBa逐滴加入到溶有GDH的PBS溶液中;
调节溶液pH保持在6.0-8.0,再逐滴加入0.5%的碳化二亚胺(EDC)120μL,4℃搅拌过夜;
通过G-25凝胶层析柱纯化,得到6-磷酸葡萄糖脱氢酶-环孢霉素A偶联物,于2-8℃下储存。
然而,现有技术的方法依赖于对小分子药物(环孢霉素A)自身所带反应基团进行的激活,之后再与酶进行反应。这样的偶联方法会出现同一葡萄糖六磷酸脱氢酶上链接有多个环孢霉素A的情况,且偶联位点难以确保一致性,难以保证小分子药物和酶之间的定向1:1反应,而导致批间差异大。
发明内容
鉴于本领域的需求,本申请提供了一种新型的6-磷酸葡萄糖脱氢酶突变体、及其在制备环孢霉素A检测试剂盒中的用途。
根据一些实施方案,提供了一种6-磷酸葡萄糖脱氢酶突变体。区别于已有发表的专利US006090567A(Homogeneous immunoassays using mutant glucose-6-phosphatedehydrogenases)的6磷酸葡萄糖脱氢酶的突变体,本申请的6-磷酸葡萄糖脱氢酶突变体,其包含选自以下的突变:D306C、D375C、G426C。
根据一些实施方案,提供了一种6-磷酸葡萄糖脱氢酶突变体,所述6-磷酸葡萄糖脱氢酶突变体是选自以下的序列所示:SEQ ID No.2、SEQ ID No.3、SEQ ID No.4。
根据一些实施方案,提供了一种多核苷酸,其编码本申请的6-磷酸葡萄糖脱氢酶突变体。
根据一些实施方案,提供了一种表达载体,其包含本申请的多核苷酸。
根据一些实施方案,提供了一种宿主细胞,其包含本申请的表达载体。宿主细胞可以是原核(如细菌)或真核(如酵母)。
根据一些实施方案,提供了一种偶联物,其是本申请的6-磷酸葡萄糖脱氢酶突变体与半抗原按照摩尔比1:x偶联而成。在一些实施方案中,x是1至10,例如,1、2、3、4、5、6、7、8、9、10。在一些具体的实施方案中,本申请的6-磷酸葡萄糖脱氢酶突变体与半抗原按照摩尔比优选为1:1。
在一些具体的实施方案中,半抗原的分子量为100Da至4000Da,例如:100、150、200、250、300、350、400、410、420、430、440、450、460、470、480、490、500、520、550、570、600、620、650、700、750、800、850、900、950、1000、1100、1200、1300、1400、1500、1600、1700、1800、1900、2000、2100、2200、2300、2400、2500、2600、2700、2800、2900、3000、3100、3200、3300、3400、3500、3600、3700、3800、3900、4000。
根据本申请,技术人员将理解,“半抗原”还包含其衍生物的形式。为了便于和6-磷酸葡萄糖脱氢酶进行偶联,对于那些自身不带有偶联基团(例如,与巯基反应的基团)的半抗原(例如环孢霉素A),可以经改造而带有接头,以便和巯基共价结合。因此,在本申请中,半抗原衍生物是指,经改造而带有巯基反应基团的半抗原。
半抗原选自:小分子药物(如抗生素、精神药物)、激素、代谢物、糖、脂质、氨基酸。
半抗原例如但不限于:万古霉素、茶碱、苯妥英、维生素D、25羟维生素D、1,25双羟维生素D、叶酸、强心甙(包括地高辛、洋地黄毒苷)、酶酚酸、雷帕明、环孢霉素A、乙胺碘复酮、甲胺喋呤、他克莫司、血清氨基酸、胆汁酸、甘胆酸、苯丙氨酸、乙醇、尿尼柯丁代谢产物柯替宁、尿吗啡、尿单羟酚衍生物、神经肽酪氨酸、血浆甘丙素、多胺、组织胺、促甲状腺激素、泌乳素、胎盘泌乳素、生长激素、促卵泡刺激素、促黄体生成素、促肾上腺皮质激素、抗利尿激素、降钙素、降钙素原、甲状旁腺激素、甲状腺素、三碘甲状原氨酸、反三碘甲状原氨酸、游离甲状腺素、游离三碘甲状原氨酸、皮质醇、尿17-羟皮质类固醇、尿17-酮类固醇、脱氢表雄酮及硫酸酯、醛固酮、尿香草苦杏仁酸、血浆肾素、血管紧张素、促红细胞生成素、睾酮、双氢睾酮、雄烯二酮、17α羟孕酮、雌酮、雌三醇、雌二醇、孕酮、人绒毛膜促性腺激素、胰岛素、胰岛素原、C肽、胃泌素、血浆前列腺素、血浆6-酮前列腺素F1α、前列环素、肾上腺素、儿茶酚胺、去甲肾上腺素、胆囊收缩素、纳素、环磷酸腺苷、环磷酸鸟苷、血管活性肽、生长抑素、促胰液素、P-物质、神经降压素、血栓素A2、血栓素B2、5羟色胺、神经肽Y、骨钙素。
在具体的实施方案中,半抗原是环孢霉素A或其衍生物。
在具体的实施方案中,半抗原是环孢霉素A衍生物,其带有巯基反应基团,例如来酰亚胺、溴乙酰基、乙烯基砜或氮丙啶。
在具体的实施方案中,半抗原是环孢霉素A衍生物,如式I所示:
其中,CsA是所示。
在一些实施方案中,m为1至10的整数,优选1至3的整数,例如1、2、3。
在具体的实施方案中,环孢霉素A衍生物如式III所示:
其中,CsA是所示;。
根据一些实施方案,提供了一种试剂,其包含本申请的偶联物。
根据一些实施方案,提供了本申请的6-磷酸葡萄糖脱氢酶突变体在制备环孢霉素A检测试剂中的用途。
根据一些实施方案,提供了本申请的偶联物在制备环孢霉素A检测试剂中的用途。
在具体的实施方案中,所述的检测试剂选自:酶联免疫法检测试剂、化学发光免疫法检测试剂、均相酶免疫法检测试剂、胶乳增强免疫比浊法检测试剂。
在具体的实施方案中,所述的检测试剂优选是基于竞争法检测的试剂。
根据一些实施方案,提供了本申请的偶联物在制备环孢霉素A检测装置中的用途。
在具体的实施方案中,所述的检测装置可以制备成孔板(例如96-孔板)的形式,比如板上包被根据本申请的试剂。
在具体的实施方案中,所述的检测装置可以制备成颗粒(例如胶乳、磁珠)的形式,比如颗粒上包被根据本申请的试剂。
根据一些实施方案,提供了一种环孢霉素A检测试剂盒,其包含:
-第一试剂,所述第一试剂包含底物、缓冲液和环孢霉素A抗体;所述底物是6-磷酸葡萄糖脱氢酶的底物;
-第二试剂,所述第二试剂包含本申请的偶联物和缓冲液;
-任选地,校准品,所述校准品包含10mM至500mM缓冲液、0ng/ml至1500ng/ml环孢霉素A;以及
-任选地,质控品,所述质控品包含10mM至500mM缓冲液、20ng/ml至1400ng/ml环孢霉素A。
根据一个实施方案,提供了一种环孢霉素A检测试剂盒,其包含:
第一试剂,其包含:
10mM至500mM缓冲液、
5mM至50mM底物、
0.1μg/ml至10μg/ml环孢霉素A抗体、
0.05%至0.5%w/v稳定剂、
0.05%至0.5%w/v表面活性剂、
0.05%至0.5%w/v防腐剂;
第二试剂,其包含:
10mM至500mM缓冲液、
0.01μg/ml至1μg/ml根据本申请的偶联物、
0.05%至0.5%w/v稳定剂、
0.05%至0.5%w/v表面活性剂、
0.05%至0.5%w/v防腐剂;
在一些实施方案中,所述缓冲液选自以下的一种或组合:TAPS、氨基丁三醇缓冲液、磷酸盐缓冲液、Tris-HCl缓冲液、柠檬酸-柠檬酸钠缓冲液、巴比妥缓冲液、甘氨酸缓冲液、硼酸盐缓冲液、三羟甲基甲烷缓冲液;优选地,磷酸盐缓冲液;所述缓冲液的浓度为10mmol/L至500mmol/L,优选50至100mM;所述缓冲液的pH为7至8.4。
在一些实施方案中,所述稳定剂选自以下的一种或组合:牛血清白蛋白、海藻糖、甘油、蔗糖、甘露醇、甘氨酸、精氨酸、聚乙二醇6000、聚乙二醇8000;优选牛血清白蛋白。
在一些实施方案中,所述表面活性剂选自以下的一种或组合:Brij23、Brij35、Triton X-100、Triton X-405、Tween20、Tween30、Tween80、椰子油脂肪酸二乙醇酰胺、AEO7,优选Tween80。
在一些实施方案中,所述的防腐剂选自以下的一种或组合:叠氮化物、MIT、生物防腐剂PC(如PC300)、硫柳汞;所述叠氮化物选自:叠氮钠、叠氮锂。
在一些实施方案中,所述底物包含:6-磷酸葡糖糖、β-烟酰胺腺嘌呤二核苷酸。
在一些具体的实施方案中,所述环孢霉素A抗体源自:小鼠、大鼠、猫、犬、灵长类、牛、马、羊、骆驼科、禽、人。
在一些具体的实施方案中,所述环孢霉素A抗体选自:单抗、多抗、重组抗体、嵌合抗体、抗原结合片段。
根据一些实施方案,提供了一种偶联物的制备方法,包括步骤:
1)提供根据本申请的环孢霉素A衍生物,尤其是在非质子性溶剂(例如但不限于乙腈、二甲基甲酰胺、二甲基亚砜)中提供根据本申请的环孢霉素A衍生物;
2)提供6-磷酸葡萄糖脱氢酶突变体,优选在缓冲液(其提供反应环境,例如但不限于PBS、Tris、TAPS、TAPSO,所述缓冲液pH为6.0至8.0)中提供6-磷酸葡萄糖脱氢酶突变体;
3)在18℃至28℃,将所述环孢霉素A衍生物和所述6-磷酸葡萄糖脱氢酶突变体按照摩尔比n:1接触1小时至4小时(优选2小时至3小时)使得所述环孢霉素A衍生物和所述6-磷酸葡萄糖脱氢酶突变体发生偶联,得到所述种偶联物;
4)根据需要,任选对所述种偶联物进行纯化,例如脱盐处理等。
在一些实施方案中,反应体系中酶和半抗原的接触摩尔比1:n,其中n是1至500,例如,1、2、3、4、5、6、7、8、9、10、11、12、13、14、15、16、17、18、19、20、21、22、23、24、25、26、27、28、29、30、31、32、33、34、35、36、37、38、39、40、41、42、43、44、45、46、47、48、49、50、100、200、300、400、500及其任意上述数值之间的范围;优选n是20至60。
在一些具体的实施方案中,步骤1)和2)可互换或并行。
在一些具体的实施方案中,在偶联之前,所述6-磷酸葡萄糖脱氢酶包含一个或多个游离的巯基,从而允许和环孢霉素A实现定向反应。
野生型6-磷酸葡萄糖脱氢酶不含游离的巯基,因此在一些具体的实施方案中,6-磷酸葡萄糖脱氢酶是经过基因工程改造的,使其在特定位点(306、375或426位)上的氨基酸突变为半胱氨酸,从而带有一个游离巯基。
附图说明
图1.G6PDH(野生型)氨基酸序列(SEQ ID No.1);源自假肠膜明串珠菌Leuconostoc pseudomesenteroides。
图2.G6PDH(D306C)氨基酸序列(SEQ ID No.2)。
图3.G6PDH(D375C)氨基酸序列(SEQ ID No.3)。
图4.G6PDH(G426C)氨基酸序列(SEQ ID No.4)。
具体实施方式
实施例
实施例1.环孢霉素A衍生物的合成
1.化合物2的合成
向圆底烧瓶中加入环孢霉素A(100mg,0.08mmol),溶于干燥的二氯甲烷(5mL)中,向反应体系中加入三乙胺(25mg,0.25mmol),搅拌至全部溶解。
向反应体系中加入草酰氯(52.8mg,0.42mmol),室温搅拌,TLC检测,室温(18-28℃,优选20至25℃)反应约1小时,原料基本消失,减压除去溶剂,使用DCM反复(2-3次)带出多余的草酰氯,不经纯化直接用于下一步。
2.环孢霉素A衍生物的合成
将化合物2和化合物3(10mg,0.05mmol)溶于干燥的二氯甲烷(5mL)中,向其中滴加三乙胺(12.4mg,0.12mmol),室温(18-28℃,优选20至25℃)搅拌,TLC检测。反应完毕直接用制备板纯化(MeOH/DCM=1:20),得到式III所示环孢霉素A衍生物(45mg,产率38%)。
3.按常规方法确认产物结构。本实施例使得环孢霉素A带有一个可以和酶结合的基团。
实施例2.环孢霉素A衍生物与G6PDH分子的偶联
一、本申请的偶联方法
根据本申请的G6PDH-环孢霉素A偶联物,按照以下方式进行偶联:环孢霉素A衍生物分子上的巯基反应性基团(如但不限于马来酰亚胺基团)与G6PDH分子上的巯基共价结合。
1.将实施例1制备的环孢霉素A衍生物溶于N,N-二甲基甲酰胺中(10mg/ml);
2.G6PDH溶液:G6PDH(本申请的突变体或现有技术突变体)溶于0.2M磷酸盐缓冲液,pH 8.0(2.5mg/ml酶);
3.将300μl葡萄糖6磷酸脱氢酶突变体溶液加入50μl环孢霉素A衍生物溶液;
4.上述混合溶液,在室温(18-28℃,优选20至25℃)下充分震荡2-3小时,分子筛层析处理,所得产物即G6PDH-环孢霉素A偶联物(浓度0.1mg/mL-2.5mg/mL)。
二、对照偶联方法
参照CN107782889A实施例中公开的方法制备G6PDH-环孢霉素A偶联物。
实施例3.试剂盒的制备
制备以下检测环孢霉素A的试剂盒,其包含:
试剂R1,包含:
Tris缓冲液100mM,pH7.4
20mM 6-磷酸葡萄糖
20mMβ-烟酰胺腺嘌呤二核苷酸
1μg/ml环孢霉素A抗体(市售抗体)
0.5%w/v牛血清白蛋白
0.1%w/v Tween80
0.1%w/v PC300;
试剂R2,包括:
Tris缓冲液100mM,pH8.2
0.05μg/ml G6PDH-环孢霉素A偶联物
0.5%w/v牛血清白蛋白
0.1%w/v Tween 80
0.1%w/v PC300;
样本萃取液:硫酸锌50mM、Tris缓冲液50mM、PC300 0.1%w/v、甲醇50%w/v;
校准品:全血基质、以及0ng/ml、50ng/ml、300ng/ml、600ng/ml、900ng/ml、1500ng/ml环孢霉素A(或按需加入);
质控品:全血基质、以及100ng/ml、750ng/ml、1300ng/ml环孢霉素A(或按需加入)。
将上述试剂(任选包含质控品、校准品),组装成检测试剂盒。
上述所述校准品、质控品以及待测样本为生理样本,例如血清、血浆、全血等。优选,上述所述校准品、质控品以及待测样本均为全血基质,测试前需用样本萃取液进行前处理。
检测例
本发明试剂盒采用酶放大免疫测定EMIT原理,即样本中游离的CsA,与酶-CsA偶联物竞争性结合CsA抗体。样本中游离的CsA越多,结合的抗体越多,游离的偶联物就越多。游离出来的偶联物催化β-烟酰胺腺嘌呤二核苷酸氧化型(NAD+)转化为β-烟酰胺腺嘌呤二核苷酸还原型(NADH),样本中的CsA浓度与NADH的生成量成正比,通过340nm吸光值的变化即可计算出CsA的含量。
表1.全自动生化仪参数
检测例1.本申请试剂盒的性能
1.定标吸光度
表2.定标吸光度
2.精密度实验
利用如上建立起的定标曲线,测定高、中、低质控品、临床样本。
表3.总不精密度
3.重复性
测低、中、高值质控品各20次进行重复性实验。如下表所示,样本测试重复20次,CV均在2.35%以内。
表4.试剂盒的重复性
4.回收
表5.回收
5.检测试剂盒的线性
表6.线性
6.37℃试剂加速稳定性
表7.37℃试剂加速稳定性
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7.药物干扰实验
选取以下干扰物,在环孢霉素A浓度为200-1000ng/ml时,以下物质产生的系统偏差小于10%。
表8.药物干扰实验
| 药物 | 测试浓度(μg/mL) |
| 阿普唑仓 | 0.57 |
| 地高辛 | 0.015 |
| 卡马西平 | 100 |
| 庆大霉素 | 150 |
| 雷帕霉素 | 0.25 |
| 他克莫司 | 0.25 |
| 水杨酸 | 400 |
| 茶碱 | 200 |
| 丙戊酸 | 600 |
| 万古霉素 | 500 |
| 免疫球蛋白 | 8500 |
| 盐酸异丙肾上腺素 | 0.4 |
| 苯巴比妥 | 200 |
| 氨苯碟啶 | 5.0 |
| 沙丁胺醇 | 0.15 |
| 胃复安 | 4 |
| 硝酸甘油 | 3.5 |
检测例2.抗体抑制率
1.抗体抑制率的检测原理
当抗体与G6PDH-环孢霉素A偶联物结合时,由于空间位阻导致G6PDH酶活性受到影响,从而使得其催化NAD转化为NADH的效率降低,通过检测NADH量的变化,从而比较加入抗体与未加入抗体的实验组的差异,这种差异即体现为抗体对G6PDH的抑制能力。
2.反应体系
表9.抗体抑制率的检测试剂制备
3.结果
比较加入抗体与未加入抗体时,分别检测G6PDH-环孢霉素A偶联物吸光度测值,即可得到抗体对G6PDH的抑制情况。
相对于已发表的突变位点(A45C、K55C)所制备的偶联物相比,本申请的突变体在抗体抑制率上有明显提高,能达到44%以上(G426C:44%;D375C:50%),最高达63%(D306C)。而之前已发表的突变位点(例如A45C、K55C)的抑制率为40%至43%。
虽然不限于具体理论,但是可以部分地解释为:和现有技术中的G6PDH突变体(A45C、K55C)相比,本申请酶突变体中突变位点(即引入游离巯基的位点)是和半抗原(比如激素、小分子药物等)发生偶联的位置所在。半抗原在这个位置上与半抗原特异性抗体结合时,所构成的空间位阻对G6PDH酶的活性影响最大,同时在引入突变后,还不能实质上影响分子的空间折叠。因此,这个突变位点的位置非常重要,需要同时兼顾G6PDH酶的活性、偶联分子的空间折叠、以及半抗原表位的充分暴露。
由于酶的突变体在抗体抑制率上有明显的提高。将酶的突变体与环孢霉素A偶联后的偶联物配制成试剂盒后,试剂在批间变异系数、线性、特异性等性能方面有明显的性能提升。
Claims (2)
1.一种偶联物的制备方法,其包括步骤:
1)提供环孢霉素A衍生物;
2)提供6-磷酸葡萄糖脱氢酶突变体;
3)所述6-磷酸葡萄糖脱氢酶突变体与所述环孢霉素A衍生物发生偶联;
所述环孢霉素A衍生物是式I所示:
其中,
CsA是所示;
m为1至10的整数,优选1至3的整数;
所述6-磷酸葡萄糖脱氢酶突变体,相较于野生型6-磷酸葡萄糖脱氢酶,包含选自以下任一个突变:D306C、D375C、G426C;
所述6-磷酸葡萄糖脱氢酶突变体是选自以下任一序列所示:SEQ ID No.2、SEQ IDNo.3、SEQ ID No.4。
2.根据权利要求1所述的偶联物的制备方法,其包括步骤:
1)提供环孢霉素A衍生物,优选在非质子性溶剂中提供环孢霉素A衍生物;
2)提供6-磷酸葡萄糖脱氢酶突变体,优选在缓冲液中提供所述6-磷酸葡萄糖脱氢酶突变体;
3)在18℃至28℃,优选20℃至25℃,将所述6-磷酸葡萄糖脱氢酶突变体和所述环孢霉素A衍生物接触1小时至4小时,优选2小时至3小时,使得所述环孢霉素A衍生物和所述6-磷酸葡萄糖脱氢酶突变体发生偶联,得到所述偶联物;
4)任选,对所述偶联物进行纯化,优选对所述偶联物进行脱盐纯化;
步骤1)和步骤2)能够互换或并行;
所述缓冲液选自以下一种或组合:PBS、Tris、TAPS、TAPSO,
所述缓冲液的pH为6.0至8.0;
所述非质子性溶剂选自以下一种或组合:乙腈、二甲基甲酰胺、二甲基亚砜;
在步骤3)之前,所述6-磷酸葡萄糖脱氢酶突变体在第306、375或426位有游离巯基。
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| CN113046335B (zh) * | 2019-12-27 | 2023-05-26 | 中国科学院天津工业生物技术研究所 | 一种仿生辅酶偏好性的葡萄糖6-磷酸脱氢酶突变体及其应用 |
| CN115856278A (zh) * | 2020-01-07 | 2023-03-28 | 北京九强生物技术股份有限公司 | 妥布霉素检测试剂盒 |
| CN112114127A (zh) * | 2020-09-09 | 2020-12-22 | 武汉生之源生物科技股份有限公司 | 一种甘胆酸均相酶免疫测定试剂盒及其制备方法和应用 |
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