CN110462024A - 用于癌症免疫疗法的mr1限制性t细胞受体 - Google Patents
用于癌症免疫疗法的mr1限制性t细胞受体 Download PDFInfo
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Abstract
本发明涉及分离可表达T细胞受体的T细胞的方法,该T细胞受体能够特异性结合通过与MR分子相关联的癌细胞呈递的抗原。该方法包括以下步骤:(a)提供T细胞制剂;(b)使制剂与表达MR1蛋白的癌细胞接触;(c)分离与所述癌细胞产生特异反应的T细胞。本发明进一步涉及一种制备T细胞制剂的方法,该T细胞制剂在转基因表达载体上表达选择性识别MR1的T细胞受体,该T细胞制剂在癌症治疗中的应用,以及编码响应MR1的T细胞受体的核酸和细胞的集合。
Description
本发明涉及限于非多态性抗原呈递分子MR1的肿瘤反应性人T细胞抗原受体(TCR)的鉴别。从代表新型的人T细胞群(由发明人发现并称为MR1T的细胞)的克隆中分离功能性TCR转录序列,该人T细胞群在没有添加任何外来抗原的情况下并以MR1依赖性的方式与表达MR1的肿瘤细胞反应。本发明还涉及MR1限制性肿瘤反应性TCR基因序列在癌症治疗中的使用。
背景技术
T淋巴细胞可以检测多种不同的由非多态性细胞表面分子呈递的非肽抗原,包括脂质和磷酸化类异戊二烯。这些T细胞的多样性表型和功能特性起到保护宿主免受感染、自身免疫和癌症的特殊作用。针对非肽抗原的T细胞库最近增加并包含粘膜相关的恒定T(MAIT)细胞,这些细胞对众多酵母和细菌产生的小核黄素前体作出反应,并由MHC I类相关蛋白MR1呈递。MAIT细胞在人血液、肾脏和肠道中很常见,并且包含大部分驻留在肝脏中的T细胞。活化后,MAIT细胞释放出一系列促炎和免疫调节细胞因子,并可介导直接杀伤被微生物感染的细胞。尚不清楚MR1除了将微生物代谢产物向MAIT细胞呈递之外是否还有其他作用。
MR1为非多态性MHC I类蛋白,其在许多细胞类型的表面上以低水平表达。MR1在多个菌种中高度保守,人和小鼠MR1在蛋白质水平上具有>90%的序列同源性。
发明人提出了存在可识别由MR1呈递的肿瘤相关抗原的人T细胞。这些新型T细胞可能参与肿瘤免疫监视,因此代表了癌症免疫疗法的新工具。用供体或源于患者的T细胞的过继性疗法(其设计成表达选定的肿瘤相关抗原的TCR)代表了在癌症患者中诱导临床相关的抗肿瘤免疫应答的一种有保证且安全的策略。然而,迄今为止已鉴别出的大多数肿瘤相关抗原是由多态性MHC分子呈递的肽。MHC基因的极端多态性限制了该方法在表达独特MHC等位基因的患者中的应用。靶向与非多态性抗原呈递分子(诸如MR1)结合的肿瘤抗原可以克服该限制,并且原则上适用于患有表达MR1的肿瘤的所有患者。使用识别MR1呈递的抗原的肿瘤反应性T细胞受体也可能具有补充由MHC呈递的肽抗原介导的抗肿瘤反应的优点,这排除了肿瘤抗原与相同类型的呈递分子结合所产生的交叉竞争。此外,该策略可提供在相同肿瘤细胞上靶向不同性质的抗原的可能性,从而最大限度地减少在选定性免疫压力下肿瘤逃逸变体的潜在发生。因此,鉴别MR1呈递的肿瘤相关抗原以及识别这些抗原的MR1限制性TCR的表征可能对癌症免疫疗法具有重要意义。
基于本领域的上述状态,本发明的目的是提供治疗癌症的新型手段和方法。该目的通过独立权利要求的主题实现,并且通过本文公开的从属权利要求、示例和附图提供了进一步有利的解决方案。
定义
在本说明书的上下文中,术语MR1是指MR1基因(Entrez 3140)或MR1基因产物(Uniprot Q95460)。
在本说明书的上下文中,术语MR1T细胞是指表达能够与癌细胞呈递的MR1分子特异性结合的T细胞受体的T细胞。
在本说明书的上下文中,术语MR1T细胞受体是指能够特异性结合由与MR1分子相关的癌细胞呈递的抗原的T细胞受体。
在本说明书中,术语阳性当在上下文中用于标记物表达时,是指通过荧光标记的抗体测定的抗原的表达,其中该荧光的中值荧光强度与用同型匹配的抗体染色后得到的荧光强度相比,至少高30%(≥30%),特别是≥50%或≥80%,所述同型匹配的抗体不与相同的靶细胞特异性结合。这样的标记物表达由该标记物的名称后面的上标“加号”(+)表示,例如CD4+。
在本说明书中,当在上下文中用于标记物表达时,术语阴性是指由荧光标记的抗体测定的抗原的表达,其中该荧光的中值荧光强度不高于用同型匹配的抗体染色后得到的荧光强度的130%,特别是不高于115%,所述同型匹配的抗体不与相同的靶细胞特异性结合。这样的标记物表达由标记物名称后面的上标减号(-)表示,例如CD127-。
术语抗体是指完整抗体,包括但不限于免疫球蛋白G型(IgG)、A型(IgA)、D型(IgD)、E型(IgE)或M型(IgM),以及任何与抗原结合的所述抗体的片段或单链和相关或衍生的构建体。该术语涵盖所谓的纳米抗体或单结构域抗体,即由单个单体可变抗体结构域组成的抗体片段。
发明内容
在最广泛的意义上,本发明涉及治疗癌症的方法,其中从与表达MR1的癌细胞具有反应性的T细胞(MR1T细胞)中分离的TCR序列在患者的T细胞群中基因转移后表达。这些外源性、转基因表达的TCR序列用于将对表达MR1的癌细胞特异性识别能力赋予T细胞,作为对患者肿瘤的治疗。
本发明类似地涉及T细胞和T细胞制剂,所述T细胞制剂包含用MR1T细胞特异性TCR基因转导的多个T细胞。在某些实施方案中,用MR1T细胞TCR基因转导的T细胞可以与其他治疗干预组合用于过继性细胞免疫疗法。
本发明还涉及一种促进鉴别从与表达MR1的癌细胞具有反应性的T细胞(MR1T细胞)中分离的TCR序列的研究方法。这涵盖分离识别肿瘤相关抗原的MR1限制性T细胞的方法。用与患者体内相同类型肿瘤的肿瘤细胞系刺激来自正常供体或来自癌症患者的外周血的T细胞。用MR1基因转染这些肿瘤细胞系,从而在其质膜上表达大量的MR1蛋白。对活化的T细胞进行分选以表达活化标记物(例如CD137、或CD150、或CD69、或ICOS),并根据公开文件(De Libero,Methods for the generation of T cell clones and epithelial celllines fromexcised human biopsies or needle aspirates.In MHC 123-140(IRL,Oxford;1997))。测试各个克隆的以MR1限制性方式识别肿瘤细胞、杀伤肿瘤细胞和释放炎性细胞因子的能力。对MR1限制性和肿瘤特异性T细胞克隆的TCR基因进行测序和识别。
本发明还涉及根据我们先前建立的方案(De Libero,同上)从相同的癌组织活检中制备肿瘤浸润性T细胞的方法。针对表达MR1蛋白的肿瘤细胞系测试各个T细胞克隆。研究了反应性最强的T细胞克隆的MR1限制性、肿瘤杀伤力和炎性细胞因子的释放。对所选T细胞克隆的TCR基因进行测序。
具体实施方式
本发明的第一方面涉及一种方法,
该方法识别和分离表达T细胞受体的T细胞,所述T细胞受体能够特异性结合特定癌细胞抗原,该特定癌细胞抗原由与非多态性MHC I相关的MR1抗原呈递分子关联的癌细胞呈递。所述方法包含以下步骤:
a.提供从患者或健康供体分离的T细胞制剂,然后
b.在接触步骤中,在没有外源微生物衍生抗原的情况下,将该分离的T细胞制剂与表达MR1蛋白的癌细胞
接触,特别是共培养,然后
c.在分离步骤中以MR1依赖的方式将与所述癌细胞特异反应的T细胞分离。
在非肿瘤患者的生理环境中,MR1呈递细菌核黄素副产物(以上称为“外源微生物衍生抗原”),并将其呈递给粘膜恒定的T细胞。
在某些实施方案中,接触步骤包括扩增步骤,其中分离的T细胞制剂在表达MR1的癌细胞存在下扩增。在某些特定实施方案中,照射癌细胞以便在与T细胞接触之前阻止其生长。如果要将两种细胞共培养较长的时间并且要避免癌细胞令该培养过度生长,这一处理是有益处的。
在其他环境中,特别是在临床使用(见下文)中,当培养时间短的时候,癌细胞可以在没有照射的情况下使用。
在某些实施方案中,扩增步骤在IL-2、IL-7和IL-15的存在下进行。
在某些实施方案中,分离步骤包括用一种或多种配体染色,特别是对选自CD3、CD69、CD137、CD150和/或ICOS的细胞表面标记物具有特异性的一种或多种(单克隆)抗体。在特别优选的实施方案中,分离步骤包括选定CD3+CD137+、和/或CD3+CD69+、和/或CD3+CD150+、和/或CD3+ICOS+T细胞,然后进行流式细胞分析和细胞分选,特别是使用FACS或磁分离(MACS)进行细胞分选。此处标记物的阳性表达(+)意指与用同型匹配的抗体染色相比,其中值荧光强度增加至少30%,该同型匹配的抗体不与相同的细胞特异性结合。换句话说,使用FACS或MACS分离表达CD3和CD137、和/或CD3和CD69、和/或CD3和CD150、和/或CD3和ICOS的T细胞。本领域技术人员知晓,在经由FACS分离细胞的情况下,可以在单个步骤中分离对两种(或更多种)不同标记物的表达呈阳性的细胞。如果使用磁分离,则必须进行两个单独的步骤以分离对于两种不同标记物的表达呈阳性的细胞。
分离步骤包括选定显示MR1限制性活性的T细胞。换句话说,该步骤包括分离由MR1呈递的抗原活化的T细胞。
在某些实施方案中,分离步骤包括选定T细胞,当用表达MR1的细胞刺激时,与用不表达MR1的细胞刺激相比,其从选自IFN-γ和/或GM-CSF的细胞因子释放两倍的表达量。
本领域技术人员知晓表达MR1的癌细胞在MR1呈递特定的癌抗原或许多特定的癌抗原。
在某些实施方案中,分离步骤包括选定T细胞,当用表达MR1的肿瘤细胞刺激时,其与用不表达MR1的肿瘤细胞(相同来源或相同细胞系)刺激相比,其从选自IFN-γ和/或GM-CSF的细胞因子释放两倍的表达量。
反应性细胞对与表达MR1的癌细胞(以MR1限制性方式呈递癌抗原)的接触产生响应时,其会上调活化标记物(特别是前述段落中记载的标记物),释放细胞因子并开始增殖。
换句话说,显示MR1限制性活性的T细胞是可以由MR1显示的肿瘤相关的抗原激活的T细胞。
这些细胞可以在对标记物具有特异性的经适当荧光标记的抗体染色后通过荧光激活细胞分选(FACS)进行分选,或者通过用适当抗体标记的磁珠进行分选(这是临床环境中常用的分选方法)。
在某些实施方案中,分离步骤包括扩增根据其活化状态的函数分选后的细胞的各个克隆,然后选定显示MR1限制性活性的T细胞克隆,特别是这样一种T细胞克隆,当用表达MR1的细胞刺激时,与用不表达MR1的细胞刺激相比,选自IFN-γ和/或GM-CSF的细胞因子具有两倍的表达量。
在某些实施方案中,该方法还包括确定编码在分离步骤中分离的T细胞的T细胞受体的核酸序列。在某些实施方案中,该方法包括确定编码在分离步骤中分离的T细胞的T细胞受体的两条链的两个核酸序列。
本发明的另一方面涉及一种在不存在外源抗原时产生与MR1反应的转基因MR1T细胞制剂的方法。该方法首先涵盖确定哪些T细胞受体最可能对患者中特定的表达MR1的癌症具有反应性,然后从转移到细胞中的表达构建体制备表达这些特异性T细胞受体基因的T细胞群,以及将这些设计好的T细胞给患者施用。
该方法包括以下步骤:
a.提供从患者获得的肿瘤样品;
b.将所述肿瘤样品与多个对MR1反应的MR1T细胞受体分子接触,并且
-在多个T细胞克隆上呈递,其中每个T细胞克隆的特征在于具有与MR1反应的MR1T细胞受体分子;或
-作为经过标记的可溶性MR1T细胞受体分子,以非细胞依赖性方式进行识别;
c.识别对所述肿瘤样品特异性反应的多个T细胞克隆;
d.提供T细胞制剂,特别是从同一患者获得的T细胞制剂;
e.将一核酸表达构建体引入所述T细胞制剂从而产生转基因T细胞制剂,所述核酸构建体编码在所述T细胞克隆上表达的MR1反应性T细胞受体分子,其在步骤c中被识别出与所述肿瘤样品特异性反应。
因此可以将患者的转基因T细胞制剂施用给患者。
在某些实施方案中,所述T细胞制剂从同一患者获得(自体过继性T细胞疗法)。该方法具有避免不良反应风险的优点,特别是由设计的T细胞制剂的内源性T细胞受体驱动的同种免疫反应。
在某些实施方案中,所述T细胞制剂从另一个受试者获得,特别是与HLA匹配的受试者(同种异体过继性T细胞疗法)。取决于HLA匹配的质量,同种免疫的风险可能会很大,但与定制的患者个体疗法高得多的成本和监管障碍相比,大量选定预先制备的TC制剂的后勤和程序优势可能有助于该疗法在更大的患者群体中进行。
将MR1T细胞受体表达构建体引入T细胞制剂中可以通过慢病毒转导实现,发明人在MR1T细胞的工作中经常使用慢病毒转导,或通过DNA表达载体(质粒)或RNA转染的标准方法实现。本领域技术人员知晓相关的方案和程序。
任选地,转基因T细胞制剂可以在施用于患者之前保持培养一段时间以扩增其数量,并且再次任选地,进一步刺激其分化成特别期望的T细胞亚组。
在某些实施方案中,从所述患者获得的T细胞制剂获自患者的外周血,特别是其中所述T细胞制剂通过选定外周血单核细胞(PBMC)以表达CD4、CD8、CD27、CD45RA和CD57中的一种或多种T细胞标记物而获得的。
在某些实施方案中,从所述患者获得的T细胞制剂是从肿瘤活检中获得的,随后相继在体外扩增。在某些实施方案中,在植物凝集素、IL-2、IL-7和IL-15的存在下,T细胞扩增。增殖T细胞通过磁分选分离并用于T细胞受体设计或用于克隆和分离肿瘤特异性MR1限制性T细胞。分离的MR1T细胞用于TCR基因克隆。
多个MR1特异性T细胞克隆可以在上述程序之前制备,并且以库或组的形式保存,以便在需要快速表征出现肿瘤时进行临时使用。该步骤基本上是鉴别可识别特定肿瘤实体的MR1特异性T细胞受体分子。
或者,可以产生可溶性MR1T TCR并使其多聚化(参见Subbramanian et al.NatureBiotechnology,22,1429,(2004))。TCR多聚体将用荧光染料标记并用于染色从肿瘤活检分离的肿瘤细胞。可溶性MR1T TCR多聚体的结合将指示MR1T TCR识别肿瘤细胞的能力,因此将有助于选定适合该患者的基因疗法的MR1T TCR。
本发明的另一方面涉及表达载体,其包含编码功能性T细胞受体异二聚体的核酸序列并使其转录,或能够与T细胞受体β链一起形成功能性T细胞受体异二聚体的T细胞受体α链,和/或能够与T细胞受体α链一起形成功能性T细胞受体异二聚体的T细胞受体β链。值得注意的是,发明人也发现了MR1特异性γ-δ异二聚体,因此上述限定同样适用于这些链。
在表达载体包含编码T细胞受体α链或T细胞受体β链(或γ或δ链)的核酸序列的实施方案中,必须将两种不同的表达载体(一种编码α链(γ链)和一种编码β链(δ链))引入细胞中,以使所述细胞能够表达功能性T细胞受体异二聚体。T细胞受体异二聚体特异性结合MR1分子,其中所述MR1分子在肿瘤细胞上表达并呈递肿瘤相关抗原。
上述核酸序列的表达由可在哺乳动物细胞,特别是人T细胞中运作的启动子序列控制。在某些实施方案中,启动子是组成型活化的启动子,例如通常用于分子生物学的CMV即刻早期启动子。在某些其他实施方案中,所述启动子是诱导型启动子。
在本发明该方面的某些实施方案中,表达载体中包含的核酸序列是或包含选自SEQ ID NO.027至038的核酸序列,和/或编码选自SEQ ID NO.001至012(α链)的氨基酸序列。
在本发明该方面的某些实施方案中,表达载体中包含的核酸序列是或包含选自SEQ ID NO.039至050的核酸序列,和/或编码选自SEQ ID NO.013刚至024(β链)的氨基酸序列。
在某些实施方案中,核酸序列编码由SEQ ID NO.051编码的T细胞受体γ链或编码由SEQ ID NO.025指定的T细胞受体γ链。
在某些实施方案中,核酸序列编码由SEQ ID NO.052编码的T细胞受体δ链或编码由SEQ ID NO.026指定的T细胞受体δ链。
本发明的另一方面涉及一种编码功能性T细胞受体异二聚体的核酸序列。T细胞受体异二聚体特异性地结合在呈递肿瘤相关抗原的肿瘤细胞上表达的非多态性MHC I相关(MR1)的抗原呈递分子。
在某些实施方案中,核酸序列编码T细胞受体α链并且选自SEQ ID NO.027至038,或编码与选自SEQ IDNO.001至012的氨基酸序列对应的T细胞受体α链。
在某些实施方案中,核酸序列编码T细胞受体β链并且选自SEQ ID NO.039至050或编码与选自SEQ IDNO.013至024的氨基酸序列对应的T细胞受体β链。
在某些实施方案中,MR1T细胞受体由本文公开的一条α链和一条β链构成。发明人出人意料地发现α和β链可以组合以产生能够识别MR1的功能性TCR分子。
在某些实施方案中,MR1T细胞受体由一个α链和一个β链构成,与以下列表的序列所对应:
a.SEQ ID NO.001和SEQ ID NO.023;
b.SEQ ID NO.002和SEQ ID NO.022;
c.SEQ ID NO.003和SEQ ID NO.021;
d.SEQ ID NO.004和SEQ ID NO.020;
e.SEQ ID NO.005和SEQ ID NO.019;
f.SEQ ID NO.006和SEQ ID NO.017;
g.SEQ ID NO.007和SEQ ID NO.018;
h.SEQ ID NO.008和SEQ ID NO.016;
i.SEQ ID NO.009和SEQ ID NO.015;
j.SEQ ID NO.010和SEQ ID NO.014;
k.SEQ ID NO.011和SEQ ID NO.013;
l.SEQ ID NO.012和SEQ ID NO.024;或
m.SEQ ID NO.025和SEQ ID NO.026;
本发明的另一方面涉及一种与非多态性MHC I相关的MR1抗原呈递分子结合的T细胞受体蛋白。MR1分子在肿瘤细胞上表达并呈递肿瘤相关抗原。在某些实施方案中,通过根据本发明第一方面的方法鉴别结合非多态性MHC I相关MR1抗原呈递分子的T细胞受体蛋白。
在某些实施方案中,T细胞受体蛋白包含T细胞受体α链,其特征在于选自SEQ IDNO.001至012的氨基酸序列,以及T细胞受体β链,其特征在于选自SEQ ID NO.013至024的氨基酸序列。
在某些实施方案中,T细胞受体蛋白包含T细胞受体γ链,其特征在于氨基酸序列SEQ ID NO.25,和T细胞受体δ链,其特征在于氨基酸序列SEQ ID NO.26。
本发明的另一方面涉及一种重组细胞,其包含如前述段落所述的根据本发明的表达载体和/或根据本发明的T细胞受体多肽。本领域技术人员知道,在表达载体仅包含编码T细胞受体α链(或γ链)或T细胞受体β链(或δ链)的核酸序列,而不是两者都包含的情况下,必须将两种不同的表达载体(一种编码α/γ链,以及一种编码β/δ链)引入重组细胞中,以便使所述细胞能够表达功能性T细胞受体异二聚体。在某些实施方案中,重组细胞源于外周血的T细胞。在某些实施方案中,重组细胞源于肿瘤浸润淋巴细胞。
本发明的另一个方面涉及根据本发明前述方面的重组细胞在癌症冶疗或预防方法中的使用。该方法包括施用重组细胞。
在某些实施方案中,所述癌症的特征在于表达MR1。
在某些实施方案中,通过过继性T细胞免疫疗法实现该施用。
本发明进一步涉及一种治疗或预防癌症复发的方法,包括施用根据本发明的重组细胞。在某些实施方案中,所述癌症的特征在于表达MR1。
在某些实施方案中,通过过继性T细胞免疫疗法实现该施用。
本发明还涉及核酸序列的集合,其中该集合的每个序列编码不同的T细胞受体α链、T细胞受体β链、T细胞受体γ链、T细胞受体δ链或T细胞受体α链和β链的组合,或T细胞受体γ链和δ链的组合,其中所述组合能够特异性结合呈递癌症抗原的MR1分子。核酸序列能够促进哺乳动物细胞中T细胞受体α链、β链或α和β链组合的表达。
该集合将用于选定转基因构建体,以转移到从患者收集的T细胞中。在鉴别出最适合在该治疗方法的第一阶段对肿瘤所呈递的一组特定肿瘤抗原发起反应的TCR序列后,医生将需要能够从根据GMP制造的该集合中选定预先产生的表达载体,以快速实现基因转移到患者的T细胞中。
在某些实施方案中,该集合包含选自SEQ ID NO.27至SEQ ID NO.52的序列,和/或该集合包含编码选自SEQ ID NO.1至SEQ ID NO.26的T细胞受体分子(或构成α或β、或γ或δ链的T细胞受体)的序列。
本发明的另一个方面涉及一种重组T细胞集合,其中该集合的每个细胞表达能够与呈递癌抗原的MR1分子特异性结合的T细胞受体作为转基因体。在某些实施方案中,该集合包含这样一种重组T细胞,该重组T细胞包含根据本发明各方面的T细胞受体蛋白异二聚体。
发明人鉴别并分离了一种新型人MR1限制性T细胞群体,该群体以MR1依赖性方式对多种肿瘤细胞产生反应。MR1T细胞克隆通常在不同健康个体的血液中发现,表达不同的TCR基因,并且不识别先前鉴别的MR1微生物或叶酸衍生配体。相反,他们认识到从肿瘤细胞中分离并由MR1呈递的各种不同组的未知抗原。目前正在进行与肿瘤细胞相关的刺激性抗原的鉴别和表征。MR1T细胞克隆识别并杀伤不同类型的肿瘤细胞,因此在体外显示出标记的抗肿瘤活性。此外,他们释放Th1、Th2和Th17细胞因子的不同组合,并显示多种趋化因子受体表达谱、表明表型和功能多样性。重要的是,当从各个的MR1T细胞克隆分离的配对的TCRα和β基因或TCRγ和δ基因转移到TCR缺陷的T细胞中时,受体T细胞获得识别表达MR1的肿瘤细胞的能力,从而表明MR1T细胞TCR基因转移对于该类型的肿瘤识别是足够的,并且可以用于指示选定的T细胞识别表达MR1的肿瘤细胞。
总之,这些发现揭示了一种新型功能多样的肿瘤反应性人T细胞群,其限于非多态性MR1分子,在肿瘤免疫中具有不同的潜在作用,从而为癌症免疫监测和免疫疗法提供新的概念框架。
在本说明书中,使用以下缩写:APC:抗原呈递细胞;β2m:β2微球蛋白;Dc:树突状细胞;GM-CSF:粒细胞-巨噬细胞菌落刺激因子;HPLC:高压液相色谱法;IFN-γ:干扰素-γ;mAb:单克隆抗体;MAIT细胞:粘膜相关的不变T细胞;MHC:主要组织相容性复合体;MR1:MHCI类相关分子;MR1T细胞:MR1限制性T细胞;PBMC:外周血单核细胞;TCR:T细胞受体;TIL:肿瘤浸润淋巴细胞。
通过以下示例和附图进一步说明本发明,从中可以得出进一步的实施方案和优点。这些示例旨在说明本发明,但不限制其范围。
附图说明
图1.MR1T细胞不识别微生物抗原。(A)CCRFSB、THP-1和A375-MR1细胞对MR1的表面表达。灰色直方图表示用同型匹配的对照mAb染色。在不存在(无Ag)或存在大肠杆菌裂解物(大肠杆菌)和/或抗MR1阻断mAb(α-MR1)的情况下,由三种细胞系在A中刺激(B)MR1T细胞克隆DGB129或(C)MAIT细胞克隆SMC3。MAIT克隆SMC3先前从健康供体的PBMC中分离并表达经典的MAIT表型和功能。柱表示IFN-γ释放(平均值±SD)。THP-1细胞刺激(D)DGB129MR1T或(E)SMC3MAIT细胞,结构上表达表面MR1,载有合成的6,7-二甲基-8-D-核糖基嗪(RL-6,7-二聚体)以及具有或不具有抗MR1mAb。柱表示平均IFN-γ释放+SD。数据代表四个(A、B和C),两个(D和E)。*P<0.05(非配对student T检验)。
图2.从外周T细胞中分离MR1T细胞克隆的策略。(A)在不存在外源抗原的情况下与A375-MR1细胞过夜共培养后,用经照射的A375-MR1细胞预先扩增的纯化T细胞的FACS分析。左点图显示活细胞中的CD3和细胞追踪紫色(CTV)染色。右点图显示CD3阳性CTV阴性门控细胞的CD69和CD137表达。箭头表示门控层次结构。数字表示门内细胞的百分比。来自供体A的细胞示出为代表性供体。(B,D)从供体A和B筛选的T细胞克隆的累积结果。如A中所示,从CD3+CTV-CD137+分选的T细胞产生T细胞克隆。图表显示各个克隆(x轴)及其IFN-γ释放(y轴),表示为响应于A375-MR1细胞对A375WT细胞分泌的细胞因子的量之间的比率。每个点代表单个T细胞克隆,在指定的实验条件下同时测试。垂直线表示显示MR1限制性反应性的T细胞克隆的数量(即显示IFN-γ释放率高于任意截止值2的克隆)。结果代表两个独立实验。(C,E)在阻断抗MR1mAb(α-MR1)存在下用A375WT、A375-MR1和A375-MR1刺激后,供体A和来自供体B的11个克隆的14个代表性克隆释放IFN-γ。点代表每个克隆的IFN-γ释放(重复培养物的平均值±SD)。结果代表三个独立实验。*P<0.05(非配对Student T检验)。
图3.MR1T细胞在健康个体的血液中是常见的。(A)在与A375WT或A375-MR1细胞过夜共培养后,来自代表性供体(供体C)的纯化T细胞的流式血细胞术分析。点图显示活CD3+细胞上的CD69和CD137表达。数字表示门中细胞的百分比。(B)与A375WT或A375-MR1细胞过夜共培养后来自5个不同供体的CD69+CD137+T细胞的频率。(C)来自供体C的T细胞克隆刺激测定的累积结果。从CD3+CD69+CD137+分选的T细胞产生T细胞克隆,如右点图所示。该图显示了测试克隆的数量(x轴)和IFN-γ释放(y轴),表示为响应于A375-MR1细胞对A375WT细胞分泌的细胞因子的量之间的比率。每个点代表单个T细胞克隆,在指定的实验条件下同时测试。垂直线表示显示MR1限制性反应性的T细胞克隆的数量(即显示IFN-γ释放率高于任意截止值2的克隆)。结果代表两个独立实验。(D)来自供体C的8个代表性MR1限制性T细胞克隆在没有外源抗原的情况下识别A375-MR1但不识别A375WT细胞。通过阻断抗MR1mAb(α-MR1)抑制T细胞克隆对A375-MR1细胞的反应性。点代表在三个实验条件下测试的每个克隆的IFN-γ释放(重复培养物的平均值±SD)。结果代表三个独立实验。*P<0.05(非配对StudentT检验)。
图4.MR1T TCR基因转移赋予A375细胞MR1限制性识别。分别在大肠杆菌裂解物和抗MR1mAb存在或不存在的情况下,通过表达(A375-MR1)或缺少(A375WT)MR1的A375细胞刺激(A)表达DGB129TCR(SKW3-DGB129)的SKW-3细胞和(B)表达MAIT MRC25TCR(J.RT3-MAIT)的J.RT3-T3.5细胞。在存在或不存在抗MR1mAb的情况下,用A375-MR1或A375WT细胞通过三种单独MR1T细胞克隆(C)DGA4(SKW3-DGA4)、(D)DGB70(SKW3-DGB70)和(E)JMA(SKW3-JMA)刺激表达TCR的SKW-3细胞。示出了转导的T细胞的重复培养物的CD69中值荧光强度(MFI)+SD。还示出了在不存在APC的情况下培养的转导T细胞的CD69MFI。当与A375-MR1或A375WT孵育时,模拟转导的T细胞示出了CD69表达的背景水平(未示出)。数据代表三次独立的实验。*P<0.05(非配对Student T检验)。
图5.MR1T细胞克隆对各种类型肿瘤细胞的鉴别识别。(A)在没有(无Ag)或存在大肠杆菌裂解物(大肠杆菌)的情况下,通过代表性SMC3MAIT细胞克隆识别表达MR1组成型表面水平的四种人细胞系,该裂解物具有或不具有抗MR1阻断mAb(α-MR1)。(B)通过具有或不具有抗MR1mAb(α-MR1)的13个MR1T细胞克隆识别与A中相同的细胞类型。图表显示IFN-γ释放(重复培养物的平均值±SD)。
图6.MR1T细胞克隆不与微生物配体或6-FP反应。(A)在存在或不存在大肠杆菌裂解物的情况下,7个MR1T细胞克隆和一个对照MAIT细胞克隆与表达(A375-MR1)或不表达A375细胞(A375WT)MR1共培养的反应。还示出了由抗-MR1mAb(α-MR1)阻断T细胞克隆反应性。(B)在6-甲酰蝶呤(6-FP)存在下,MR1T细胞克隆对表达WT MR1分子(A375-MR1)或K43A突变的MR1分子(A375-MR1K43A)的A375细胞的响应。(C)用A375-MR1或A375-MR1K43A细胞刺激对照MAIT细胞克隆MRC25或对照TCRVγ9Vδ2克隆G2B9,该细胞预先分别在没有或存在6-FP的情况下与大肠杆菌裂解物或唑来膦酸盐一起孵育。结果表示为在重复培养物中测量的IFN-γ的平均值±SD。结果代表三个独立实验。*P<0.05(非配对Student T检验)。
图7.MR1T细胞克隆不识别Ac-6-FP。(A)在不存在或存在乙酰基-6-甲酰基蝶呤(Ac-6-FP)的情况下通过A375-MR1细胞刺激三个代表性MR1T细胞克隆。(B)在不存在或存在Ac-6-FP的情况下,用大肠杆菌裂解物脉冲的A375-MR1细胞刺激两个MAIT细胞克隆(MRC25和SMC3)。(C)在不存在或存在Ac-6-FP(25μg/ml)的情况下,用唑来膦酸盐(Zol)处理A375-MR1细胞,并用于刺激TCRVγ9-Vδ2细胞克隆(G2B9)。(D)在不存在或存在Ac-6-FP(25μg/ml)的情况下,使用表达K43A突变体MR1分子(A375-MR1K43A)的A375细胞刺激A中示出的三个MR1T细胞克隆。(E)在不存在或存在Ac-6-FP(25μg/ml)的情况下,用大肠杆菌裂解物脉冲的A375-MR1K43A细胞刺激B中使用的两个MAIT细胞克隆。结果表示为在重复培养物中评估的IFN-γ释放的平均值±SD,并且代表三个独立实验。*P<0.05(非配对Student T检验)。
图8.MR1T细胞识别肿瘤细胞中存在的抗原,而不是源自RPMI 1640培养基。通过MR1过表达(A)A375细胞(A375-MR1)和(B)THP-1细胞(THP1-MR1)在RPMI 1640或PBS中生长4天刺激DGB129MR1T细胞克隆,两者都补充有5%的人血清。示出了抗MR1阻断mAb(α-MR1)对T细胞克隆反应性的抑制。DGB129细胞识别载有分离自(C)THP-1细胞裂解物或来自(D)体内生长的小鼠乳腺肿瘤EMT6的APC分离物。分离物E1和E2含有疏水分子;分离物N1至N4含有亲水分子。(E)DGB70MR1T细胞与THP-1裂解物的N3分离物反应。(F)通过加载到塑料结合的重组MR1上的THP-1衍生的分离物N3和N4刺激DGB129和DGB70T细胞。示出了重复培养物的IFN-γ或GM-CSF平均值±SD的T细胞释放(代表三次独立实验)。总细胞因子释放在组A、组B、组F中示出;在组C、组D、组E中示出了背景上的折叠增加。*P<0.05(非配对StudentT检验)。
图9.MR1T细胞显示出不同的抗肿瘤反应。表达MR1的肿瘤细胞系THP-1和A375与MR1T细胞克隆(A)DGB129或(B)DGB70以指定的效应物:靶向(E:T)比率培养过夜。该图示出了在各个实验条件下凋亡靶细胞的百分比,通过使用膜联蛋白V和碘化丙锭染色的流式细胞术评估。通过用抗CD3mAb染色鉴别MR1T细胞并从分析中排除。抗MR1(α-MR1)mAb对MR1T细胞克隆杀伤能力的抑制也以1:1E:T比例示出。(C)通过具有或不具有抗MR1mAb(α-MR1)的13个MR1T细胞克隆从健康个体分离的Mo-DC的识别。图表显示IFN-γ释放(重复培养物的平均值±SD)。(D)在不存在或存在抗MR1(α-MR1)mAb的情况下,由代表性DGB129MR1T细胞克隆识别来自三个供体的Mo-DC。示出上清液中的IFN-γ释放并表示为平均值±SD。(E)与具有或不具有抗MR1mAb(α-MR1)的DGB129MR1T细胞共培养后,Mo-DC上的共刺激分子CD83和CD86的流式细胞术分析。还示出了在不存在T细胞的情况下用LPS(10ng/ml)刺激的Mo-DC组成的对照组。数字表示每个象限中细胞的百分比。(F)在存在或不存在抗MR1mAb(α-MR1)的情况下通过LS 174T和HCT116胃肠道肿瘤细胞系和正常肠上皮细胞(GEC)刺激JMAN MR1T细胞克隆。柱显示IFN-γ释放(重复培养物的平均值±SD)。所有结果均代表至少三次独立实验。*P<0.05(未配对学生的t-检验)。
图10.MR1T细胞克隆的功能多样性。(A)由用A375-MR1细胞刺激的7个选定的MR1T细胞克隆释放的IFN-γ。ELISA结果表示为在重复培养物中测量的IFN-γ释放的平均值±SD。(B)通过对相同上清液进行多重细胞因子测定分析附加的16种细胞因子,其中IFN-γ显示在A中。结果代表两个独立实验。
图11.MR1T细胞克隆显示多种趋化因子受体表达谱。通过七个选定的静息MR1T细胞克隆对CXCR3、CCR4和CCR6表面表达进行流式细胞术分析。图表示出了通过将特定mAb染色的中值荧光强度(MFI)除以相应同型对照的MFI而计算的相对荧光强度。数据代表两个独立实验。
图12.MR1T细胞减少小鼠中人黑素瘤肺结节的数量。向免疫失能的NSG小鼠注射表达MR1(A375-MR1)和MR1T细胞的人黑素瘤A375细胞。在第14天,处死小鼠并在印度墨水灌注后计数肺结节。
P<0.0001(非配对Student T检验)。
表格1.选定MR1反应性T细胞克隆的表型。
表格2.由MR1T细胞识别的肿瘤细胞系列表。
表格3.TCR蛋白质序列列表。
表格4.TCR核苷酸序列列表。
示例
方法
细胞。以下人细胞系获自美国典型培养物保藏中心:A375(黑色素瘤)、THP-1(髓单核细胞白血病)、J.RT3-T3.5(TCRβ缺陷型T细胞白血病)、LS174T(结肠腺癌)、HCT116(结肠癌)、Huh7(肝细胞癌)、HEK293(人胚肾)和CCRF-SB(急性B细胞淋巴母细胞白血病)。SKW-3细胞(TCRα、β、γ和δ基因缺陷的人T细胞白血病)获自莱布尼茨研究所DSMZ-德国微生物和细胞培养物保藏中心。两个代表性的MAIT克隆(MRC25和SMC3)和一个TCRγδ克隆(G2B9)((Gober et al.,The Journal of experimental medicine 197,163-168(2003))在该研究中用作对照细胞,从两个健康供体的血液中产生,并如前所述保持在培养物中(Leporeet al.,Nat Commun 5,3866(2014))。MR1T细胞从健康个体的外周血中分离出来,在采集血液时获得献血者的知情同意,并获得“北西伦理委员会和zentraschweiz/EKNZ(139/13)”的批准。简而言之,通过阴性选定纯化的T细胞(EasySepTM人T细胞富集试剂盒,StemCell)每周用辐射(80灰度)A375-MR1细胞(比例2:1)刺激一次,持续三周。人rIL-2(5U/ml;Hoffmann-La Roche),rIL-7和rIL-15(均为5ng/ml,Peprotech)在每次刺激后第+2和+5天加入。最后一次刺激后12天,洗涤细胞并与A375-MR1细胞共培养过夜(比例2:1)。然后CD3+CD69+CD37+细胞在PHA(1μg/ml,Wellcome Research Laboratories)、人rIL-2(100U/ml,Hoffmann-LaRoche)和辐射PBMC(5x105细胞/ml)存在下通过限制稀释进行分选和克隆。在其他实验中,使用与分选的CD3+CD69+CD137+相同的方案,在用A375-MR1细胞(比例2:1)进行单次过夜刺激时,产生MR1T细胞克隆。按照相同的方案周期性地再刺激T细胞克隆(Lepore等人,同上)。根据制造商的说明书,使用EasySep人CD14和CD19阳性选定试剂盒(StemcellTechnologies)从健康供体的PBMC纯化单核细胞和B细胞(>90%纯度)。如前所述(Lepore等人,同上),通过在GM-CSF和IL-4存在下培养,使Mo-DC与纯化的CD14+单核细胞分化。根据公开的方案(Graves等人,Journal of immunological methods 414,20-31(2014))从无肿瘤个体的肠活组织检查分离人正常肠上皮细胞(GEC)。
表达与β2m共价联接的MR1A基因的细胞的产生。如前所述(Lepore et al.,同上),通过PCR产生经由柔性Gly-Ser接头与β2m联接的人MR1A cDNA构建体。使用以下引物将MR1AcDNA中的K43A取代引入融合构建体:MR1K43A_f 5'-CTCGGCAGGCCGAGCCACGGGC(SEQ IDNO.53)和MR1K43A_r5'GCCCGTGGCTCGGCCTGCCGAG(SEQ ID NO.54)。将得到的WT和突变体构建体克隆到双向慢病毒载体(LV)中(Lepore等人,同上)。根据制造商的说明书,使用Metafectene Pro(Biontex),用单独的LV-MR1A-β2m构建体与慢病毒包装质粒pMD2.G、pMDLg/pRRE和pRSV-REV(Addgene)一起转染HEK 293细胞。在8μg/ml硫酸鱼精蛋白存在下,通过含有病毒颗粒的上清液的自旋感染转导A375和THP-1细胞。通过流式细胞术评估MR1的表面表达,并对阳性细胞进行FACS分选。
可溶性重组β2m-MR1-Fc融合蛋白。使用上述人MR1A-β2m构建体作为模板获得β2m-MR1-Fc融合构建体。使用引物:β2mXhoI_f5'-CTCGAGATGTCTCGCTCCGTGGCCTTA(SEQ ID 55)和MR1-IgG1_r5'-GTGTGAGTTTTGTCGCTAGCCTGGGGGACCTG(SEQ ID 56),通过PCR扩增与β2m-MR1A基因互补的DNA,从而排除MR1跨膜和细胞内结构域。使用以下引物产生与人IgG1重链的铰链区和CH2-CH3结构域互补的DNA:NheI-hinge-f5'-CAGGTCCCCCAGGCTAGCGACAAAACTCACAC(SEQ ID 57)和IgG1NotI_r5'-GCGGCCGCTCATTTACCCGGAGACAGGGAGA(SEQ ID 58)pFUSE-hIgG1-Fc1(InvivoGen)。使用具有重叠延伸PCR的两步剪接将β2m-MR1A和IgG1PCR产物连接在一起,并将得到的构建体亚克隆到BCMGSNeo表达载体的XhoI/NotI位点中。使用Metafectene Pro(Biontex)用最终构建体转染CHO-K1细胞,通过有限稀释克隆并通过ELISA筛选以产生β2m-MR1-Fc融合蛋白。适用于EX-CELL ACF CHO无血清培养基(Sigma)的选定克隆用于蛋白质生产,并且使用Protein-A-Sepharose(Thermo Fisher Scientific)根据制造商说明书纯化β2m-MR1-Fc。使用抗-MR1mAb 25.6(Biolegend)通过SDS-PAGE和蛋白质印记验证蛋白质完整性和纯度。
流式细胞术和抗体。使用标准方案进行细胞表面标记。根据制造商的说明书使用True-NuclearTM转录因子缓冲液组进行细胞内标记。从Biolegend获得以下抗人mAb:CD4-APC(OKT4)、CD8α-PE(TuGh4)、CD161-Alexa Fluor 647(HP-3G10)、CD69-PE(FN50)、CD3-PE/Cy7、亮紫-711、或Alexa-700(UCHT1)、CD137-生物素(n4b4-1)、CXCR3-亮紫421(G025H7)、CD83-生物素(HB15e)、MR1-PE(26.5)和TRAV1-2-PE(10C3)。CD86-FITC(2331)、CCR4-PECy7(1G1)和CCR6-PE(11A9)mAb来自BD Pharmingen。所有这些mAb以5μg/ml使用。用链霉抗生物素蛋白-PE、-荧光基团488或-亮紫421(2μg/ml,Biolegend)显示生物素化的mAb。在LSRFortessa流式细胞仪(Becton Dickinson)上获得样品。使用Influx仪器(BectonDickinson)进行细胞分选实验。基于前向散射面积和宽度/侧向散射和DAPI染色排除死细胞和双峰。使用FlowJo软件(TreeStar)分析所有数据。
MR1T细胞克隆的TCR基因分析。MR1T细胞克隆的TCRα和β或基因TCRγ和δ表达通过使用总cDNA和特异性引物的RT-PCR评估,或通过使用根据制造商说明书或panγδTCR特异性单克隆抗体(B1,Biolegend)的BetaMarkTCRVβRepertoire试剂盒(BeckmanCoulter)的流式细胞术来评估。对于RT-PCR,使用NucleoSpin RNA II试剂盒(MachereyNagel)制备RNA,并使用Superscript III逆转录酶(Invitrogen)合成cDNA。根据制造商的指导(TCR分型扩增试剂盒,Clontech),使用Vα、Vβ、Vγ和Vδ组引物扩增TCRα、β、γ和δcDNA。通过测序鉴别功能性转录物,然后使用ImMunoGeneTics信息系统(http://www.imgt.org)进行分析。
TCR基因转移。将来自MAIT细胞克隆MRC25的TCRα和β功能性cDNA克隆到BCMGSNeo表达载体的XhoI/NotI位点(Karasuyama and Melchers Eur.J.Immunol.1988 18:97-104)和所得的构建体用于根据标准程序通过电穿孔共转染J.RT3-T3.5细胞。将表达TRAV1-2和CD3的转染子进行FACS分选。将来自MR1T克隆的TCRα和β或TCRγ和δ功能性cDNA克隆到质粒52962(Addgene)表达载体的修饰版本的XmaI/BamHI位点。用如上所述产生的含病毒颗粒的上清液转导SKW-3细胞。基于CD3表达对细胞进行FACS分选。
细胞和整个肿瘤裂解物的分离。经由轻度超声处理在水中破碎,从2.5×109THP-1细胞的单个沉淀物产生总细胞裂解物。然后将超声处理的物质离心(15,000g,以4℃持续15分钟),并收集上清液(S1)。接下来,将沉淀重新悬浮在甲醇中,经超声处理,如前所述离心,并将获得的上清液与S1上清液合并。甲醇的最终浓度为10%。然后将总细胞提取物上样到C18Sep-Pak柱(Waters Corporation)上,收集未结合的物质并干燥(E-FT分离物)。用75%甲醇(分离物E1)和100%甲醇(分离物E2)分批洗脱结合的物质。将E-FT物质重新混悬在乙腈/水(9:1体积/体积)中并装载到NH2Sep-Pak柱(Waters Corporation)上。用增加量的水洗脱未结合的物质(分离物N-FT)和4个附加的分离物。分离物N1用35%H2O洗脱,分离物N2用60%H2O洗脱,分离物N3用100%H2O洗脱,以及分离物N4用100%H2O和50mM乙酸铵(pH7.0)洗脱。将所有分离物干燥,然后在-70℃下储存之前,重新混悬于20%甲醇(分离物E1、E2和N-FT)或100%H2O(所有其他分离物)中。
如该文献中所述制备小鼠EMT6乳腺肿瘤(Zippelius et al.,Cancer ImmunolRes 3,236-244(2015))。将新切除的肿瘤在盐水中充分洗涤、称重,并使用Dounce组织研磨机将4g质量在7ml HPLC级水中匀浆。肿瘤匀浆经历两次冻-融循环,在4℃下离心(3,250g)10分钟,收集上清液并储存在-70℃。用2ml HPLC级水第二次提取沉淀,在4℃下离心(5,100g)10分钟,收集上清液并储存在-70℃下。在室温下通过涡旋将该沉淀物用9ml HPLC级甲醇进一步提取5分钟,在4℃下离心(5,100g)10分钟,并收集上清液。合并三个上清液,干燥并重新混悬于水:甲醇(10:1)中。如上所述使用C18和NH2Sep-Pak柱分离物质。
T细胞活化测定。MR1限制性T细胞(5×104/孔,除非另有指明)与指定的靶细胞(5×104/孔)在200μl总体积中一式两份或一式三份进行共培养。将T细胞与指定的APC一起培养24小时。在一些实验中,加入抗MR1mAb(克隆26.5)或小鼠IgG2a同型对照mAb(均为30μg/ml)并在加入T细胞之前孵化30分钟。从在LB培养基中生长的DH5α菌株(Invitrogen)制备大肠杆菌裂解物,并在指数级生长期间收集。将细菌细胞在PBS中洗涤两次,然后通过超声处理裂解。离心(15,000g持续15分钟)后,收集上清液、干燥,并在-70℃下储存。在加入T细胞之前,用相当于108CFU/ml(除非另有说明)的大肠杆菌裂解物将APC脉冲4小时。在一些实验中,在与T细胞共培养之前,将APC与6-FP或Ac-6-FP(Schircks Laboratories))预孵育4小时。在用表达TCRVγ9和Vδ2链的TCRγδ细胞的对照实验中,在加入T细胞之前,首先用唑来膦酸盐(10μg/ml)处理APC 6小时。通过将β2m-MR1-Fc包被在96孔板(4μg/ml)上并在37℃下用柱纯化的细胞裂解物加载4小时,用板结合的重组人β2m-MR1-Fc进行活化实验,然后洗涤两次并添加T细胞。24小时后收集上清液,并通过ELISA评估IFN-γ或GM-CSF。根据制造商的说明书,细胞培养上清液中的多种细胞因子和趋化因子使用Milliplex MAP人细胞因子/趋化因子磁珠板-预混合41plex(HCYTMAG-60K-PX41;Merck Millipore)。在Flexmap 3D系统(Merck Millipore)上获得样品,并使用Milliplex分析软件确定平均荧光强度和分析物浓度。
杀伤肿瘤细胞。在存在或不存在抗MR1mAb(30μg/ml,克隆26.5)的情况下,使用靶细胞系(2×104细胞/ml)进行杀伤测定,该靶细胞系单独或与不同E/T比例的T细胞孵育24小时。如前所述,靶细胞用PE-膜联蛋白V(BD)和碘化丙啶(PI)(Sigma-Aldrich)染色(2)。通过用抗CD3mAb染色鉴别T细胞并从分析中排除。细胞凋亡评估如下:膜联蛋白V+PI+=晚期凋亡和膜联蛋白V-PI+=坏死。还示出了在不存在T细胞的情况下(自发凋亡;没有T细胞)凋亡+坏死细胞的百分比。
统计值。使用非配对Student T检验(Prism 6,GraphPad软件)分析数据。
鉴别和表征健康供体中新型肿瘤反应性MR1限制性T细胞
发明人检测了在人MAIT细胞库的早期研究期间不与微生物配体反应的非典型MR1限制性T细胞克隆。该T细胞克隆(DGB129)识别组成型显示表面MR1的细胞系(CCRF-SB淋巴细胞白血病细胞,或THP-1单核细胞白血病细胞;图1A)或用MR1基因转染(A375黑素瘤细胞;A375-MR1;图1A),在没有任何外源添加的抗原的情况下(图1B)。MR1+靶细胞的无菌识别通过用抗MR1单克隆抗体(mAb)阻断而受到完全抑制(图1B),因此类似于平行评估的MAIT细胞对大肠杆菌衍生抗原的反应(图1C)。重要的是,DGB129T细胞也未能识别合成的MAIT细胞激动剂6,7-二甲基-8-D-核糖基嗪(RL-6,7-diMe;图1D)与对照MAIT细胞克隆不同,该克隆通过该化合物以MR1依赖性方式刺激(图1E)。DGB129细胞不表达典型的MAIT细胞的经典型半不变TCR(表1)。
发明人研究了DGB129克隆是否代表不同于微生物反应性MAIT细胞的新型肿瘤反应性MR1限制性T细胞群。因此,他们建立了一种分离和研究这些不可预测的MR1限制性T细胞的方法。来自两个健康供体的纯化T细胞用增殖标记物CellTrace紫色(CTV)标记,并在不存在外源抗原的情况下用经照射的A375-MR1细胞刺激。用A375-MR1细胞再次攻击增殖细胞,并通过有限稀释分选和克隆表达高水平活化标记CD137的那些细胞(图2A)。然后研究各个T细胞克隆识别缺少MR1的A375-MR1和A375细胞(A375-WT)的能力。在两个供体中,发明人发现大部分的T细胞克隆(分别为126/195和37/57)显示A375-MR1细胞的特异性识别(图2B、图D),其被抗MR1阻断mAb抑制(图2C、图E)。用12个MR1反应性T细胞克隆的TCR Vβ特异性mAb染色显示它们表达7种不同的TRBV链(TRBV4-3、6-5/6-6/6-9、9、18、25-1、28、29-1)其中一些克隆共享相同的TRBV基因。此外,没有一个表达TRAV1-2链,对MAIT细胞来说是经典的。
缺乏特异性标记物使得难以通过标准流式细胞术在体外单独鉴别这些新型T细胞。因此,通过在非常短时间的体外刺激和单个T细胞克隆实验之后组合流式细胞术分析来估计其频率。将来自五个健康供体的纯化的血液T细胞与MR1缺陷的或MR1足够的A375细胞共培养过夜,并分析活化标记物CD69和CD137的表达(图3A)。在筛选的所有五个供体中,用A375-MR1细胞(范围为T细胞的0.034-0.072%)刺激后检测到的CD69+CD137+T细胞百分比始终高于与A375-WT细胞共培养后的百分比(范围为0.015-0.032%)(图3A、图B)。由于两种类型的APC对MR1表达不同,MR1反应性T细胞在用MR1阳性APC刺激后导致活化的T细胞数量增加。使用该方法,发明人估计所分析的个体的循环T细胞库含有A375-MR1反应性T细胞,频率范围在1:2500(0.072-0.032=0.04%)和1:5000(0.034-0.015=0.019)之间。该估计频率高于抗原暴露后肽特异性CD4+T细胞的频率(Lucas et al.,J Virol 78:7284-7287;Su etal.,Immunity 38:373-383)。这些观察结果得到平行实验的支持,其中克隆了来自这些供体之一(供体C,图3A,右图)的分选的CD69+CD137+过夜活化的T细胞。实际上,96个筛选的T细胞克隆中的31个(32%)显示出对A375-MR1细胞的特异性反应性(图3C),其被抗MR1mAb抑制(图3D)。因此,该供体的血液T细胞中计算出的A375-MR1反应性T细胞的频率为1:5000(0.065×0.32=0.02%),该值与估计范围一致。对来自三个供体的代表性T细胞克隆的详细分析证实其显示出不同的TCRα和β链,并且表明CD4、CD8和CD161的差异表达(表1)。
总的来说,这些发现表明,所鉴别的肿瘤反应性MR1限制性T细胞是健康人个体(下文称为MR1T细胞)血液中新的但常见的淋巴细胞多克隆群。
MR1T细胞TCR基因转移赋予MR1限制的肿瘤细胞识别
发明人接下来研究了MR1T细胞对肿瘤细胞的反应性是否由TCR介导。在TCR缺陷的SKW-3细胞中克隆来自不同MR1T细胞克隆的成对TCRα和β基因并使其表达,赋予对肿瘤细胞的MR1的识别能力,其与原始MR1T细胞显示的MR1识别类似,并且被抗MR1-mAb完全阻断(图4A-图C)。在对照实验中,代表性MAIT细胞克隆的TCRα和β基因的转移赋予了仅在存在大肠杆菌抗原的情况下以MR1依赖性方式识别A375-MR1细胞的能力(图4D)。这些数据突出了TCR在介导肿瘤细胞的MR1T细胞识别中的关键作用,并且表明MR1T细胞TCR基因转移可以有效地将选定的T细胞的反应性重定向至表达MR1的肿瘤细胞。
MR1T细胞克隆对肿瘤细胞的鉴别识别
已经产生了大量的MR1T细胞克隆与表达MR1的A375黑素瘤细胞反应,发明人接下来研究了其是否也能识别组成型表达表面MR1的其他类型的肿瘤细胞,包括THP-1髓单核细胞、Huh7肝细胞瘤细胞、HCT116结肠癌细胞和LS 174T杯状结肠腺癌细胞。所有这些细胞类型在微生物抗原存在下以MR1依赖性方式支持MAIT细胞活化(图5A)。相同的细胞能够在不同程度上诱导选定的MR1T细胞克隆的无菌活化。大多数测试的MR1T细胞克隆识别THP-1细胞,随后是Huh7肝细胞瘤细胞、LS174T杯状细胞和HCT116结肠癌细胞(图5B)。重要的是,所有反应都被抗MR1mAb阻断。
这些数据进一步证实MR1T细胞是限于非多态性抗原呈递分子MR1的肿瘤反应性T细胞的新型的和多样性的细胞。
MR1T细胞识别肿瘤细胞中存在的MR1结合抗原
发明人接下来研究了MR1T细胞对肿瘤细胞的反应性的基础。首先,他们寻求明确排除MR1T细胞克隆能够识别微生物抗原的可能性,类似于MAIT细胞。而对照MAIT细胞克隆仅在大肠杆菌裂解物存在下与A375-MR1细胞反应,不同的MR1T细胞克隆的活化没有被大肠杆菌裂解物增强(图6A)。与这些数据一致,MR1阴性的A375-WT细胞未能刺激任何类型的T细胞,无论大肠杆菌裂解物是否加入(图6A),重要的是抗-MR1mAb有效阻断MR1T和MAIT细胞两者反应(图6A)。这些发现证实了存在于大肠杆菌中并刺激MAIT细胞的微生物配体不会刺激测试的MR1T细胞。
然后,发明人测试了MR1T细胞对已知的MR1配体6-FP和Ac-6-FP的反应,其先前已报道刺激TRAV1-2阴性T细胞的稀有亚组并抑制微生物抗原的MAIT细胞活化。在存在6-FP或Ac-6-FP配体的情况下MR1T细胞刺激受损,其也损害了大肠杆菌对对照MAIT细胞的刺激,但不破坏由相同APC呈递的对同源抗原的对照TCRγδ细胞反应,因此排除了化合物毒性(图6B、图C和图7A至图C)。值得注意的是,当转录靶A375细胞以表达具有缺陷配体结合能力的突变MR1分子时,6-FP或Ac-6-FP未能抑制MR1T细胞或MAIT细胞的活化(通过赖氨酸43突变为丙氨酸,A375-MR1K34A,用配体阻断席夫碱的形成;图6B、图C和图7D、图E)。用6-FP或Ac-6-FP观察到的特异性抑制表明MR1T细胞i)不识别6-FP和Ac-6-FP;ii)与MR1结合的细胞抗原反应;和iii)受不需要与MR1形成希夫碱的配体刺激。
为了获得关于识别的抗原的起源的进一步信息,发明人研究肿瘤靶细胞的刺激能力是否依赖于培养基成分,因为一些MR1配体,例如6-FP可能源自用于细胞培养的RPMI1640培养基中存在的叶酸。将THP-1和A375-MR1细胞彻底洗涤并在仅补充有5%人血清的磷酸盐缓冲盐水溶液(PBS)中培养4天。每天洗涤细胞,然后用于刺激DGB129MR1T细胞,并在PBS中进行T细胞活化测定。在RPMI 1640或PBS中生长的THP-1和A375-MR1细胞显示相同的刺激能力(图8A、图B),因此表明培养基成分不使MR1T细胞活化。为了直接研究刺激性抗原是否存在于靶肿瘤细胞中,本发明人然后使用两种类型的肿瘤裂解物作为抗原来源进行T细胞活化测定。第一裂解物从体外培养的THP-1细胞获得,而第二裂解物是在切除后立即从小鼠乳腺肿瘤制备的。获得两种疏水性和四种亲水性分离物,并使用组成型表达低水平MR1的THP-1细胞作为APC进行测试。DGB129克隆仅与N4分离物反应,其含有从新鲜移植的小鼠肿瘤和体外培养的THP-1细胞两者分离的高度亲水性化合物(图8C、图D)。这些结果排除了刺激性抗原来源于RPMI 1640成分的可能性并表明了其细胞来源。发明人还用另一种代表性MR1T细胞克隆DGB70测试了THP-1裂解物产生的分离物。DGB70细胞识别分离物N3而不识别分离物N4(图8E),表明至少两种不同的复合物不同地刺激两种MR1T克隆。将相同的分离物加载到塑料结合的MR1分子上并显示出替代和特异性刺激能力,即N3仅刺激DGB70细胞,而N4仅刺激DGB129细胞(图8F)。在不存在N3和N4分离物的情况下,两个克隆不与MR1反应,进一步表明需要特异性抗原。
总之,这些数据表明MR1T细胞识别与不是源自培养基的配体复合的MR1,并且也存在于体内生长的肿瘤细胞中。
MR1T细胞显示出不同的抗肿瘤反应
为了评估MR1T细胞的抗肿瘤活性,本发明人测试了其在体外直接杀伤肿瘤细胞的能力。两种代表性的MR1T细胞克隆(DGB129和DGB70)以各种效应子:靶比例有效杀伤表达MR1的THP-1和A375细胞两者(图9A、图B)。对照MAIT细胞克隆未能杀伤这两种细胞类型,尽管当靶向被大肠杆菌感染时其完全能够杀伤(未示出)。这些结果表明MR1T细胞显示出对表达MR1的肿瘤细胞的特异性细胞毒活性。
已经发现MR1T细胞识别并杀伤了髓单核细胞肿瘤细胞系THP-1,发明人接下来解决了其是否也能识别正常骨髓细胞,这包括来自不同供体的单核细胞和单核细胞衍生的树突细胞(Mo-DC)。任何测试的MR1T细胞克隆都未识别单核细胞(未示出)。相反,一些MR1T细胞克隆以MR1依赖性方式与Mo-DC反应(图9C)。有趣的是,用代表性DGB129MR1T细胞克隆进行的实验表明,Mo-DC的识别不会导致Mo-DC杀伤(未示出),而是通过Mo-DC促进CD83和CD86活化标记物的上调(图9D)。值得注意的是,抗-MR1mAb完全抑制了DGB129细胞诱导的Mo-DC的活化(图9D)。这些数据表明,一些肿瘤反应性MR1T细胞引发直接的抗肿瘤活性并且还促进先天免疫细胞的活化,这对建立有效的抗肿瘤免疫应答具有重要意义。
当发明人观察到一些MR1T细胞克隆与HCT116和LS174T肠肿瘤细胞反应时,他们接下来研究其是否也能识别从肠道活组织检查制备的正常肠上皮细胞(GEC)。GEC细胞对任何测试的HCT116或LS174T反应性MR1T细胞克隆都没有刺激作用(图9F、图G),因此表明MR1T细胞克隆可能显示胃肠道肿瘤细胞的特异性识别而不对正常肠上皮细胞产生反应。
为了进一步评估MR1T细胞识别肿瘤的特异性,发明人最终研究了它们是否能与其他类型的正常细胞反应,包括嗜中性粒细胞、NK细胞、B细胞和T细胞。这些细胞中没有一种被测试的MR1T细胞识别(未示出)。
总的来说,这些数据将MR1T细胞鉴别为人MR1限制性T淋巴细胞的新型和多样性细胞,其i)对各种类型的肿瘤细胞不同反应;ii)显示对肿瘤细胞的细胞毒活性;iii)不识别正常细胞体外-分化的Mo-DC和iv)不会杀伤Mo-DC而是诱导其活性。这些发现表明MR1T细胞显示出重要的抗肿瘤特性,并且值得开发用于其免疫治疗潜力。
MR1T细胞在功能上是多样性的
发明人最终分析了A375-MR1肿瘤细胞刺激后代表性MR1T细胞克隆的细胞因子分泌谱。测试的所有克隆释放IFN-γ(图10A)。然而,发明人还观察到Th1(IL-2、TNF-α和TNF-β)、Th2(IL-3、IL-4、IL-5、IL-6、IL-10、IL-13)和Th17细胞因子(IL-17A、G-CSF、GM-CSF)和其他可溶性因子(MIP-1β、可溶性CD40L PDGF-AA和VEGF的不同表达谱;图10B)。由MR1T细胞表达的细胞因子的可变组合和数量表明该细胞具有相当大的功能可塑性。例如,克隆DGA4分泌大量IL-17A、IL-6、TNF-α和GM-CSF,但未能分泌原型Th2细胞因子IL-4、IL-5、IL-10或IL-13,因此显示出'非典型'Th17样表型。相反,克隆TC5A87释放了大量的VEGF和PGDF-AA,但只有少量的Th1或Th2细胞因子,而没有IL-17A。值得注意的是,研究的7个克隆中的4个(DGB129、CH9A3、DGB70、JMA)显示出细胞因子释放的Th2-偏斜特征,这是最近与保护性抗肿瘤免疫相关的功能表型。
发明人接下来研究了已知由具有不同功能的T细胞亚组差异表达的三种选定趋化因子受体的表达,并且其替代组合表达调节T细胞再循环和向不同归巢位点的迁移。除DGA4外,所有MR1T细胞克隆显示高水平的CXCR3(图11)。此外,本发明人观察到CCR4和CCR6的不同表达模式(图11),这进一步表明MR1T细胞是多样性的。
在最后一系列研究中,研究了MR1T细胞是否使用肺实体肿瘤模型在体内维持其肿瘤杀伤能力。静脉内注射表达MR1的A375黑素瘤细胞的小鼠接受DGB129细胞或不处理。在第14天,处死小鼠并计算肺中肿瘤结节的数目。虽然未处理的小鼠显示200至250个结节,但用MR1T细胞处理的小鼠显示1-6个结节(图12)。这些结果证实,体内生长的肿瘤细胞产生刺激MR1T细胞的抗原。重要的是,它们提供了MR1T细胞体内杀伤实体瘤细胞的有效能力的有力证据。
总之,这些数据表明,此处测试的肿瘤MR1反应性T克隆在表型上和功能上是多样的,因此表明MR1T细胞包括具有不同再循环模式和组织归巢能力的多个亚组,并且可能在肿瘤免疫中具有不同的作用。最后,这些数据将MR1T细胞鉴别为识别MR1:肿瘤相关抗原复合物并可参与具有多种效应功能的抗肿瘤免疫应答的人T淋巴细胞的新群体。
表格1.选定MR1反应性T细胞克隆的表型。
表格2.由人MR1T细胞识别的肿瘤细胞系。
以下示例进一步说明了应用本发明的临床工作流程:
筛选表达MR1的癌症
使用对人MR1特异的mAb和MR1mRNA的PCR扩增分析癌症患者的组织新鲜或新鲜冷冻组织活检组织的MR1表达。
癌症治疗,示例1:选定用于识别表达原代MR1的癌细胞的最佳MRT1TCR基因。
-分离体外的原代MR1+癌细胞用于刺激先前表征的MR1T细胞克隆的库。每个克隆表达不同的TCR基因并识别不同类型的癌细胞。
-选定对患者的癌细胞最佳反应的MR1T细胞克隆,并将其TCR基因用于TCR基因疗法。根据细胞因子释放和/或表面标记物表达测定反应。通过内部(细胞因子)或表面标记染色用对测定的活化标记物具有反应性的抗体测定细胞,例如但不限于CD3、CD69、CD137、CD150和/或ICOS(表面标记物)和INF-γ以及GM-CSF(细胞因子)。
-当可用的可溶性MR1T TCR将被多聚化并用于染色从肿瘤活组织检查分离的肿瘤细胞。与肿瘤细胞结合的MR1T TCR多聚体将允许快速选定适合该患者的基因疗法的MR1TTCR。
-几种循环的患者T细胞群可用作受体T细胞(原初细胞、中枢记忆、效应记忆、CD4+、CD8+或CD4,CD8双阴性T细胞)。选定原初细胞,当其被识别MR1-肿瘤抗原的TCR基因转导时,允许未标记的T淋巴细胞在肿瘤细胞存在下成熟。使用中枢和效应记忆细胞是因为它们在识别表达MR1的肿瘤细胞时提供即时增殖和效应功能(肿瘤杀伤)。选定CD4细胞以提供足够数量的T辅助细胞,其促进具有抗肿瘤功能的其他细胞的增长和扩增。选定CD8T细胞以促进肿瘤细胞的杀伤。选定CD4至CD8双阴性T细胞用于其先天样功能,诸如立即释放大量杀伤效应分子(TNFα、颗粒酶和颗粒溶素)。
-表达转导的TCR基因和具有选定的效应子功能的T细胞用于过继细胞疗法(ACT)。
来自患者外周血的T细胞用对表面标记物(CD4、CD8、CD27、CD45RA、CD57)特异的单克隆抗体染色并分选。用Human T-Activator CD3/CD28(ThermoFisher)激活每个分选的群体,并在24小时后用编码为个体患者选定的MR1T TCR的TCR基因转染。这产生了修饰的T细胞制剂(受体T细胞)。在一些情况下,受体T细胞也通过基因编辑方法修饰以失活PD1、ILT2和ILT4抑制基因或用CD137和CD134基因转导以促进细胞存活、细胞扩增和增强抗癌效应子功能。
受体的癌症患者使用非清髓性化疗制备方案(60mg/kg环磷酰胺施用2天;2525mg/m2氟达拉滨施用5天)进行淋巴细胞清除,随后将T细胞和IL-2转移至耐受性720,000IU/kg。在某些情况下,200或1200厘戈瑞(cGy;1Gy=100拉德)将全身照射加入制备方案中。将表达MR1T外源TCR基因(修饰的T细胞制剂)的T细胞转移到受体中。
将TCR基因克隆到安全的重组慢病毒载体中(参见例如Provasi等人,Nat Med 18,807-815(2012)),其含有自杀基因并且在不存在其他辅助病毒的情况下不能产生成熟的病毒颗粒。在一些情况下,将TCR基因克隆到含有自杀基因的载体中(例如,参见Greco等人,Front Pharmacol 6,95(2015)),从而降低了由不需要的基因插入引起的风险。在一些情况下,编码TCR MR1T基因的RNA在受体细胞中转染(参见例如Zhao等人。分子疗法13,151,2006))。
癌症疗法,示例2:从待治疗患者的肿瘤浸润淋巴细胞(TIL)中分离MR1T细胞。
-根据我们先前建立的方案(De Libero,同上),从癌组织活组织检查制备自体TIL。
-使用补充有IL-2、IL-7和IL-15的培养基,在体外扩增T细胞2至3周。
-测试扩增的T细胞对自体MR1+癌细胞的反应性。增加活化标记物(CD137、CD150、CD69、ICOS)表面表达的T细胞被认为是癌症特异性的,如果它们被抗MR1单克隆抗体的存在所抑制,则它们被认为是MR1依赖性的。
-如上所述,癌症反应性T细胞根据上述活化标记物之一的表达进行分选,并扩增以及用于ACT。
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Val Lys Leu Val Glu Lys Ser Phe Glu Thr Asp Thr Asn Leu Asn Phe
225 230 235 240
Gln Asn Leu Ser Val Ile Gly Phe Arg Ile Leu Leu Leu Lys Val Ala
245 250 255
Gly Phe Asn Leu Leu Met Thr Leu Arg Leu Trp Ser Ser
260 265
<210> 8
<211> 275
<212> PRT
<213> 人类
<400> 8
Met Met Lys Ser Leu Arg Val Leu Leu Val Ile Leu Trp Leu Gln Leu
1 5 10 15
Ser Trp Val Trp Ser Gln Gln Lys Glu Val Glu Gln Asp Pro Gly Pro
20 25 30
Leu Ser Val Pro Glu Gly Ala Ile Val Ser Leu Asn Cys Thr Tyr Ser
35 40 45
Asn Ser Ala Phe Gln Tyr Phe Met Trp Tyr Arg Gln Tyr Ser Arg Lys
50 55 60
Gly Pro Glu Leu Leu Met Tyr Thr Tyr Ser Ser Gly Asn Lys Glu Asp
65 70 75 80
Gly Arg Phe Thr Ala Gln Val Asp Lys Ser Ser Lys Tyr Ile Ser Leu
85 90 95
Phe Ile Arg Asp Ser Gln Pro Ser Asp Ser Ala Thr Tyr Leu Cys Ala
100 105 110
Met Ser Leu Ser Gly Gly Ser Tyr Ile Pro Thr Phe Gly Arg Gly Thr
115 120 125
Ser Leu Ile Val His Pro Tyr Ile Gln Asn Pro Asp Pro Ala Val Tyr
130 135 140
Gln Leu Arg Asp Ser Lys Ser Ser Asp Lys Ser Val Cys Leu Phe Thr
145 150 155 160
Asp Phe Asp Ser Gln Thr Asn Val Ser Gln Ser Lys Asp Ser Asp Val
165 170 175
Tyr Ile Thr Asp Lys Thr Val Leu Asp Met Arg Ser Met Asp Phe Lys
180 185 190
Ser Asn Ser Ala Val Ala Trp Ser Asn Lys Ser Asp Phe Ala Cys Ala
195 200 205
Asn Ala Phe Asn Asn Ser Ile Ile Pro Glu Asp Thr Phe Phe Pro Ser
210 215 220
Pro Glu Ser Ser Cys Asp Val Lys Leu Val Glu Lys Ser Phe Glu Thr
225 230 235 240
Asp Thr Asn Leu Asn Phe Gln Asn Leu Ser Val Ile Gly Phe Arg Ile
245 250 255
Leu Leu Leu Lys Val Ala Gly Phe Asn Leu Leu Met Thr Leu Arg Leu
260 265 270
Trp Ser Ser
275
<210> 9
<211> 275
<212> PRT
<213> 人类
<400> 9
Met Leu Leu Glu His Leu Leu Ile Ile Leu Trp Met Gln Leu Thr Trp
1 5 10 15
Val Ser Gly Gln Gln Leu Asn Gln Ser Pro Gln Ser Met Phe Ile Gln
20 25 30
Glu Gly Glu Asp Val Ser Met Asn Cys Thr Ser Ser Ser Ile Phe Asn
35 40 45
Thr Trp Leu Trp Tyr Lys Gln Asp Pro Gly Glu Gly Pro Val Leu Leu
50 55 60
Ile Ala Leu Tyr Lys Ala Gly Glu Leu Thr Ser Asn Gly Arg Leu Thr
65 70 75 80
Ala Gln Phe Gly Ile Thr Arg Lys Asp Ser Phe Leu Asn Ile Ser Ala
85 90 95
Ser Ile Pro Ser Asp Val Gly Ile Tyr Phe Cys Ala Gly Gln Leu Gly
100 105 110
Gly Ala Gly Gly Thr Ser Tyr Gly Lys Leu Thr Phe Gly Gln Gly Thr
115 120 125
Ile Leu Thr Val His Pro Asn Ile Gln Asn Pro Asp Pro Ala Val Tyr
130 135 140
Gln Leu Arg Asp Ser Lys Ser Ser Asp Lys Ser Val Cys Leu Phe Thr
145 150 155 160
Asp Phe Asp Ser Gln Thr Asn Val Ser Gln Ser Lys Asp Ser Asp Val
165 170 175
Tyr Ile Thr Asp Lys Thr Val Leu Asp Met Arg Ser Met Asp Phe Lys
180 185 190
Ser Asn Ser Ala Val Ala Trp Ser Asn Lys Ser Asp Phe Ala Cys Ala
195 200 205
Asn Ala Phe Asn Asn Ser Ile Ile Pro Glu Asp Thr Phe Phe Pro Ser
210 215 220
Pro Glu Ser Ser Cys Asp Val Lys Leu Val Glu Lys Ser Phe Glu Thr
225 230 235 240
Asp Thr Asn Leu Asn Phe Gln Asn Leu Ser Val Ile Gly Phe Arg Ile
245 250 255
Leu Leu Leu Lys Val Ala Gly Phe Asn Leu Leu Met Thr Leu Arg Leu
260 265 270
Trp Ser Ser
275
<210> 10
<211> 274
<212> PRT
<213> 人类
<400> 10
Met Thr Ser Ile Arg Ala Val Phe Ile Phe Leu Trp Leu Gln Leu Asp
1 5 10 15
Leu Val Asn Gly Glu Asn Val Glu Gln His Pro Ser Thr Leu Ser Val
20 25 30
Gln Glu Gly Asp Ser Ala Val Ile Lys Cys Thr Tyr Ser Asp Ser Ala
35 40 45
Ser Asn Tyr Phe Pro Trp Tyr Lys Gln Glu Leu Gly Lys Gly Pro Gln
50 55 60
Leu Ile Ile Asp Ile Arg Ser Asn Val Gly Glu Lys Lys Asp Gln Arg
65 70 75 80
Ile Ala Val Thr Leu Asn Lys Thr Ala Lys His Phe Ser Leu His Ile
85 90 95
Thr Glu Thr Gln Pro Glu Asp Ser Ala Val Tyr Phe Cys Ala Ala Asn
100 105 110
Trp Ser Pro Gln Gly Asn Glu Lys Leu Thr Phe Gly Thr Gly Thr Arg
115 120 125
Leu Thr Ile Ile Pro Asn Ile Gln Asn Pro Asp Pro Ala Val Tyr Gln
130 135 140
Leu Arg Asp Ser Lys Ser Ser Asp Lys Ser Val Cys Leu Phe Thr Asp
145 150 155 160
Phe Asp Ser Gln Thr Asn Val Ser Gln Ser Lys Asp Ser Asp Val Tyr
165 170 175
Ile Thr Asp Lys Thr Val Leu Asp Met Arg Ser Met Asp Phe Lys Ser
180 185 190
Asn Ser Ala Val Ala Trp Ser Asn Lys Ser Asp Phe Ala Cys Ala Asn
195 200 205
Ala Phe Asn Asn Ser Ile Ile Pro Glu Asp Thr Phe Phe Pro Ser Pro
210 215 220
Glu Ser Ser Cys Asp Val Lys Leu Val Glu Lys Ser Phe Glu Thr Asp
225 230 235 240
Thr Asn Leu Asn Phe Gln Asn Leu Ser Val Ile Gly Phe Arg Ile Leu
245 250 255
Leu Leu Lys Val Ala Gly Phe Asn Leu Leu Met Thr Leu Arg Leu Trp
260 265 270
Ser Ser
<210> 11
<211> 267
<212> PRT
<213> 人类
<400> 11
Met Trp Gly Val Phe Leu Leu Tyr Val Ser Met Lys Met Gly Gly Thr
1 5 10 15
Thr Gly Gln Asn Ile Asp Gln Pro Thr Glu Met Thr Ala Thr Glu Gly
20 25 30
Ala Ile Val Gln Ile Asn Cys Thr Tyr Gln Thr Ser Gly Phe Asn Gly
35 40 45
Leu Phe Trp Tyr Gln Gln His Ala Gly Glu Ala Pro Thr Phe Leu Ser
50 55 60
Tyr Asn Val Leu Asp Gly Leu Glu Glu Lys Gly Arg Phe Ser Ser Phe
65 70 75 80
Leu Ser Arg Ser Lys Gly Tyr Ser Tyr Leu Leu Leu Lys Glu Leu Gln
85 90 95
Met Lys Asp Ser Ala Ser Tyr Leu Cys Ala Ser Met Asp Ser Asn Tyr
100 105 110
Gln Leu Ile Trp Gly Ala Gly Thr Lys Leu Ile Ile Lys Pro Asp Ile
115 120 125
Gln Asn Pro Asp Pro Ala Val Tyr Gln Leu Arg Asp Ser Lys Ser Ser
130 135 140
Asp Lys Ser Val Cys Leu Phe Thr Asp Phe Asp Ser Gln Thr Asn Val
145 150 155 160
Ser Gln Ser Lys Asp Ser Asp Val Tyr Ile Thr Asp Lys Thr Val Leu
165 170 175
Asp Met Arg Ser Met Asp Phe Lys Ser Asn Ser Ala Val Ala Trp Ser
180 185 190
Asn Lys Ser Asp Phe Ala Cys Ala Asn Ala Phe Asn Asn Ser Ile Ile
195 200 205
Pro Glu Asp Thr Phe Phe Pro Ser Pro Glu Ser Ser Cys Asp Val Lys
210 215 220
Leu Val Glu Lys Ser Phe Glu Thr Asp Thr Asn Leu Asn Phe Gln Asn
225 230 235 240
Leu Ser Val Ile Gly Phe Arg Ile Leu Leu Leu Lys Val Ala Gly Phe
245 250 255
Asn Leu Leu Met Thr Leu Arg Leu Trp Ser Ser
260 265
<210> 12
<211> 274
<212> PRT
<213> 人类
<400> 12
Met Ile Ser Leu Arg Val Leu Leu Val Ile Leu Trp Leu Gln Leu Ser
1 5 10 15
Trp Val Trp Ser Gln Arg Lys Glu Val Glu Gln Asp Pro Gly Pro Phe
20 25 30
Asn Val Pro Glu Gly Ala Thr Val Ala Phe Asn Cys Thr Tyr Ser Asn
35 40 45
Ser Ala Ser Gln Ser Phe Phe Trp Tyr Arg Gln Asp Cys Arg Lys Glu
50 55 60
Pro Lys Leu Leu Met Ser Val Tyr Ser Ser Gly Asn Glu Asp Gly Arg
65 70 75 80
Phe Thr Ala Gln Leu Asn Arg Ala Ser Gln Tyr Ile Ser Leu Leu Ile
85 90 95
Arg Asp Ser Lys Leu Ser Asp Ser Ala Thr Tyr Leu Cys Val Val Asn
100 105 110
Arg Phe Thr Arg Asp Gly Asn Lys Leu Val Phe Gly Ala Gly Thr Ile
115 120 125
Leu Arg Val Lys Ser Tyr Ile Gln Asn Pro Asp Pro Ala Val Tyr Gln
130 135 140
Leu Arg Asp Ser Lys Ser Ser Asp Lys Ser Val Cys Leu Phe Thr Asp
145 150 155 160
Phe Asp Ser Gln Thr Asn Val Ser Gln Ser Lys Asp Ser Asp Val Tyr
165 170 175
Ile Thr Asp Lys Thr Val Leu Asp Met Arg Ser Met Asp Phe Lys Ser
180 185 190
Asn Ser Ala Val Ala Trp Ser Asn Lys Ser Asp Phe Ala Cys Ala Asn
195 200 205
Ala Phe Asn Asn Ser Ile Ile Pro Glu Asp Thr Phe Phe Pro Ser Pro
210 215 220
Glu Ser Ser Cys Asp Val Lys Leu Val Glu Lys Ser Phe Glu Thr Asp
225 230 235 240
Thr Asn Leu Asn Phe Gln Asn Leu Ser Val Ile Gly Phe Arg Ile Leu
245 250 255
Leu Leu Lys Val Ala Gly Phe Asn Leu Leu Met Thr Leu Arg Leu Trp
260 265 270
Ser Ser
<210> 13
<211> 314
<212> PRT
<213> 人类
<400> 13
Met Leu Leu Leu Leu Leu Leu Leu Gly Pro Gly Ser Gly Leu Gly Ala
1 5 10 15
Val Val Ser Gln His Pro Ser Trp Val Ile Cys Lys Ser Gly Thr Ser
20 25 30
Val Lys Ile Glu Cys Arg Ser Leu Asp Phe Gln Ala Thr Thr Met Phe
35 40 45
Trp Tyr Arg Gln Phe Pro Lys Gln Ser Leu Met Leu Met Ala Thr Ser
50 55 60
Asn Glu Gly Ser Lys Ala Thr Tyr Glu Gln Gly Val Glu Lys Asp Lys
65 70 75 80
Phe Leu Ile Asn His Ala Ser Leu Thr Leu Ser Thr Leu Thr Val Thr
85 90 95
Ser Ala His Pro Glu Asp Ser Ser Phe Tyr Ile Cys Ser Ala Lys Val
100 105 110
Thr Ser Gly Gln His Gln Gly Thr Thr Asp Thr Gln Tyr Phe Gly Pro
115 120 125
Gly Thr Arg Leu Thr Val Leu Glu Asp Leu Lys Asn Val Phe Pro Pro
130 135 140
Glu Val Ala Val Phe Glu Pro Ser Glu Ala Glu Ile Ser His Thr Gln
145 150 155 160
Lys Ala Thr Leu Val Cys Leu Ala Thr Gly Phe Tyr Pro Asp His Val
165 170 175
Glu Leu Ser Trp Trp Val Asn Gly Lys Glu Val His Ser Gly Val Ser
180 185 190
Thr Asp Pro Gln Pro Leu Lys Glu Gln Pro Ala Leu Asn Asp Ser Arg
195 200 205
Tyr Cys Leu Ser Ser Arg Leu Arg Val Ser Ala Thr Phe Trp Gln Asn
210 215 220
Pro Arg Asn His Phe Arg Cys Gln Val Gln Phe Tyr Gly Leu Ser Glu
225 230 235 240
Asn Asp Glu Trp Thr Gln Asp Arg Ala Lys Pro Val Thr Gln Ile Val
245 250 255
Ser Ala Glu Ala Trp Gly Arg Ala Asp Cys Gly Phe Thr Ser Glu Ser
260 265 270
Tyr Gln Gln Gly Val Leu Ser Ala Thr Ile Leu Tyr Glu Ile Leu Leu
275 280 285
Gly Lys Ala Thr Leu Tyr Ala Val Leu Val Ser Ala Leu Val Leu Met
290 295 300
Ala Met Val Lys Arg Lys Asp Ser Arg Gly
305 310
<210> 14
<211> 311
<212> PRT
<213> 人类
<400> 14
Met Thr Ile Arg Leu Leu Cys Tyr Met Gly Phe Tyr Phe Leu Gly Ala
1 5 10 15
Gly Leu Met Glu Ala Asp Ile Tyr Gln Thr Pro Arg Tyr Leu Val Ile
20 25 30
Gly Thr Gly Lys Lys Ile Thr Leu Glu Cys Ser Gln Thr Met Gly His
35 40 45
Asp Lys Met Tyr Trp Tyr Gln Gln Asp Pro Gly Met Glu Leu His Leu
50 55 60
Ile His Tyr Ser Tyr Gly Val Asn Ser Thr Glu Lys Gly Asp Leu Ser
65 70 75 80
Ser Glu Ser Thr Val Ser Arg Ile Arg Thr Glu His Phe Pro Leu Thr
85 90 95
Leu Glu Ser Ala Arg Pro Ser His Thr Ser Gln Tyr Leu Cys Ala Ser
100 105 110
Ser Glu Tyr Ile Gln Tyr Ser Gly Asn Thr Ile Tyr Phe Gly Glu Gly
115 120 125
Ser Trp Leu Thr Val Val Glu Asp Leu Asn Lys Val Phe Pro Pro Glu
130 135 140
Val Ala Val Phe Glu Pro Ser Glu Ala Glu Ile Ser His Thr Gln Lys
145 150 155 160
Ala Thr Leu Val Cys Leu Ala Thr Gly Phe Phe Pro Asp His Val Glu
165 170 175
Leu Ser Trp Trp Val Asn Gly Lys Glu Val His Ser Gly Val Ser Thr
180 185 190
Asp Pro Gln Pro Leu Lys Glu Gln Pro Ala Leu Asn Asp Ser Arg Tyr
195 200 205
Cys Leu Ser Ser Arg Leu Arg Val Ser Ala Thr Phe Trp Gln Asn Pro
210 215 220
Arg Asn His Phe Arg Cys Gln Val Gln Phe Tyr Gly Leu Ser Glu Asn
225 230 235 240
Asp Glu Trp Thr Gln Asp Arg Ala Lys Pro Val Thr Gln Ile Val Ser
245 250 255
Ala Glu Ala Trp Gly Arg Ala Asp Cys Gly Phe Thr Ser Val Ser Tyr
260 265 270
Gln Gln Gly Val Leu Ser Ala Thr Ile Leu Tyr Glu Ile Leu Leu Gly
275 280 285
Lys Ala Thr Leu Tyr Ala Val Leu Val Ser Ala Leu Val Leu Met Ala
290 295 300
Met Val Lys Arg Lys Asp Phe
305 310
<210> 15
<211> 312
<212> PRT
<213> 人类
<400> 15
Met Gly Phe Arg Leu Leu Cys Cys Val Ala Phe Cys Leu Leu Gly Ala
1 5 10 15
Gly Pro Val Asp Ser Gly Val Thr Gln Thr Pro Lys His Leu Ile Thr
20 25 30
Ala Thr Gly Gln Arg Val Thr Leu Arg Cys Ser Pro Arg Ser Gly Asp
35 40 45
Leu Ser Val Tyr Trp Tyr Gln Gln Ser Leu Asp Gln Gly Leu Gln Phe
50 55 60
Leu Ile Gln Tyr Tyr Asn Gly Glu Glu Arg Ala Lys Gly Asn Ile Leu
65 70 75 80
Glu Arg Phe Ser Ala Gln Gln Phe Pro Asp Leu His Ser Glu Leu Asn
85 90 95
Leu Ser Ser Leu Glu Leu Gly Asp Ser Ala Leu Tyr Phe Cys Ala Ser
100 105 110
Ser Val Gly Gly Gly Leu Ala Asp Thr Gln Tyr Phe Gly Pro Gly Thr
115 120 125
Arg Leu Thr Val Leu Glu Asp Leu Lys Asn Val Phe Pro Pro Glu Val
130 135 140
Ala Val Phe Glu Pro Ser Glu Ala Glu Ile Ser His Thr Gln Lys Ala
145 150 155 160
Thr Leu Val Cys Leu Ala Thr Gly Phe Tyr Pro Asp His Val Glu Leu
165 170 175
Ser Trp Trp Val Asn Gly Lys Glu Val His Ser Gly Val Ser Thr Asp
180 185 190
Pro Gln Pro Leu Lys Glu Gln Pro Ala Leu Asn Asp Ser Arg Tyr Cys
195 200 205
Leu Ser Ser Arg Leu Arg Val Ser Ala Thr Phe Trp Gln Asn Pro Arg
210 215 220
Asn His Phe Arg Cys Gln Val Gln Phe Tyr Gly Leu Ser Glu Asn Asp
225 230 235 240
Glu Trp Thr Gln Asp Arg Ala Lys Pro Val Thr Gln Ile Val Ser Ala
245 250 255
Glu Ala Trp Gly Arg Ala Asp Cys Gly Phe Thr Ser Glu Ser Tyr Gln
260 265 270
Gln Gly Val Leu Ser Ala Thr Ile Leu Tyr Glu Ile Leu Leu Gly Lys
275 280 285
Ala Thr Leu Tyr Ala Val Leu Val Ser Ala Leu Val Leu Met Ala Met
290 295 300
Val Lys Arg Lys Asp Ser Arg Gly
305 310
<210> 16
<211> 313
<212> PRT
<213> 人类
<400> 16
Met Ser Ile Gly Leu Leu Cys Cys Ala Ala Leu Ser Leu Leu Trp Ala
1 5 10 15
Gly Pro Val Asn Ala Gly Val Thr Gln Thr Pro Lys Phe Gln Val Leu
20 25 30
Lys Thr Gly Gln Ser Met Thr Leu Gln Cys Ala Gln Asp Met Asn His
35 40 45
Glu Tyr Met Ser Trp Tyr Arg Gln Asp Pro Gly Met Gly Leu Arg Leu
50 55 60
Ile His Tyr Ser Val Gly Ala Gly Ile Thr Asp Gln Gly Glu Val Pro
65 70 75 80
Asn Gly Tyr Asn Val Ser Arg Ser Thr Thr Glu Asp Phe Pro Leu Arg
85 90 95
Leu Leu Ser Ala Ala Pro Ser Gln Thr Ser Val Tyr Phe Cys Ala Ser
100 105 110
Gly Ile Ser Gly Thr Ala Ser Ser Tyr Asn Ser Pro Leu His Phe Gly
115 120 125
Asn Gly Thr Arg Leu Thr Val Thr Glu Asp Leu Asn Lys Val Phe Pro
130 135 140
Pro Glu Val Ala Val Phe Glu Pro Ser Glu Ala Glu Ile Ser His Thr
145 150 155 160
Gln Lys Ala Thr Leu Val Cys Leu Ala Thr Gly Phe Phe Pro Asp His
165 170 175
Val Glu Leu Ser Trp Trp Val Asn Gly Lys Glu Val His Ser Gly Val
180 185 190
Ser Thr Asp Pro Gln Pro Leu Lys Glu Gln Pro Ala Leu Asn Asp Ser
195 200 205
Arg Tyr Cys Leu Ser Ser Arg Leu Arg Val Ser Ala Thr Phe Trp Gln
210 215 220
Asn Pro Arg Asn His Phe Arg Cys Gln Val Gln Phe Tyr Gly Leu Ser
225 230 235 240
Glu Asn Asp Glu Trp Thr Gln Asp Arg Ala Lys Pro Val Thr Gln Ile
245 250 255
Val Ser Ala Glu Ala Trp Gly Arg Ala Asp Cys Gly Phe Thr Ser Val
260 265 270
Ser Tyr Gln Gln Gly Val Leu Ser Ala Thr Ile Leu Tyr Glu Ile Leu
275 280 285
Leu Gly Lys Ala Thr Leu Tyr Ala Val Leu Val Ser Ala Leu Val Leu
290 295 300
Met Ala Met Val Lys Arg Lys Asp Phe
305 310
<210> 17
<211> 309
<212> PRT
<213> 人类
<400> 17
Met Gly Pro Gly Leu Leu His Trp Met Ala Leu Cys Leu Leu Gly Thr
1 5 10 15
Gly His Gly Asp Ala Met Val Ile Gln Asn Pro Arg Tyr Gln Val Thr
20 25 30
Gln Phe Gly Lys Pro Val Thr Leu Ser Cys Ser Gln Thr Leu Asn His
35 40 45
Asn Val Met Tyr Trp Tyr Gln Gln Lys Ser Ser Gln Ala Pro Lys Leu
50 55 60
Leu Phe His Tyr Tyr Asp Lys Asp Phe Asn Asn Glu Ala Asp Thr Pro
65 70 75 80
Asp Asn Phe Gln Ser Arg Arg Pro Asn Thr Ser Phe Cys Phe Leu Asp
85 90 95
Ile Arg Ser Pro Gly Leu Gly Asp Ala Ala Met Tyr Leu Cys Ala Thr
100 105 110
Ser Arg Glu Trp Glu Thr Gln Tyr Phe Gly Pro Gly Thr Arg Leu Leu
115 120 125
Val Leu Glu Asp Leu Lys Asn Val Phe Pro Pro Glu Val Ala Val Phe
130 135 140
Glu Pro Ser Glu Ala Glu Ile Ser His Thr Gln Lys Ala Thr Leu Val
145 150 155 160
Cys Leu Ala Thr Gly Phe Tyr Pro Asp His Val Glu Leu Ser Trp Trp
165 170 175
Val Asn Gly Lys Glu Val His Ser Gly Val Ser Thr Asp Pro Gln Pro
180 185 190
Leu Lys Glu Gln Pro Ala Leu Asn Asp Ser Arg Tyr Cys Leu Ser Ser
195 200 205
Arg Leu Arg Val Ser Ala Thr Phe Trp Gln Asn Pro Arg Asn His Phe
210 215 220
Arg Cys Gln Val Gln Phe Tyr Gly Leu Ser Glu Asn Asp Glu Trp Thr
225 230 235 240
Gln Asp Arg Ala Lys Pro Val Thr Gln Ile Val Ser Ala Glu Ala Trp
245 250 255
Gly Arg Ala Asp Cys Gly Phe Thr Ser Glu Ser Tyr Gln Gln Gly Val
260 265 270
Leu Ser Ala Thr Ile Leu Tyr Glu Ile Leu Leu Gly Lys Ala Thr Leu
275 280 285
Tyr Ala Val Leu Val Ser Ala Leu Val Leu Met Ala Met Val Lys Arg
290 295 300
Lys Asp Ser Arg Gly
305
<210> 18
<211> 315
<212> PRT
<213> 人类
<400> 18
Met Thr Ile Arg Leu Leu Cys Tyr Met Gly Phe Tyr Phe Leu Gly Ala
1 5 10 15
Gly Leu Met Glu Ala Asp Ile Tyr Gln Thr Pro Arg Tyr Leu Val Ile
20 25 30
Gly Thr Gly Lys Lys Ile Thr Leu Glu Cys Ser Gln Thr Met Gly His
35 40 45
Asp Lys Met Tyr Trp Tyr Gln Gln Asp Pro Gly Met Glu Leu His Leu
50 55 60
Ile His Tyr Ser Tyr Gly Val Asn Ser Thr Glu Lys Gly Asp Leu Ser
65 70 75 80
Ser Glu Ser Thr Val Ser Arg Ile Arg Thr Glu His Phe Pro Leu Thr
85 90 95
Leu Glu Ser Ala Arg Pro Ser His Thr Ser Gln Tyr Leu Cys Ala Ser
100 105 110
Ser Gln Leu Tyr Arg Asp Thr Ser Asn Thr Gly Glu Leu Phe Phe Gly
115 120 125
Glu Gly Ser Arg Leu Thr Val Leu Glu Asp Leu Lys Asn Val Phe Pro
130 135 140
Pro Glu Val Ala Val Phe Glu Pro Ser Glu Ala Glu Ile Ser His Thr
145 150 155 160
Gln Lys Ala Thr Leu Val Cys Leu Ala Thr Gly Phe Tyr Pro Asp His
165 170 175
Val Glu Leu Ser Trp Trp Val Asn Gly Lys Glu Val His Ser Gly Val
180 185 190
Ser Thr Asp Pro Gln Pro Leu Lys Glu Gln Pro Ala Leu Asn Asp Ser
195 200 205
Arg Tyr Cys Leu Ser Ser Arg Leu Arg Val Ser Ala Thr Phe Trp Gln
210 215 220
Asn Pro Arg Asn His Phe Arg Cys Gln Val Gln Phe Tyr Gly Leu Ser
225 230 235 240
Glu Asn Asp Glu Trp Thr Gln Asp Arg Ala Lys Pro Val Thr Gln Ile
245 250 255
Val Ser Ala Glu Ala Trp Gly Arg Ala Asp Cys Gly Phe Thr Ser Glu
260 265 270
Ser Tyr Gln Gln Gly Val Leu Ser Ala Thr Ile Leu Tyr Glu Ile Leu
275 280 285
Leu Gly Lys Ala Thr Leu Tyr Ala Val Leu Val Ser Ala Leu Val Leu
290 295 300
Met Ala Met Val Lys Arg Lys Asp Ser Arg Gly
305 310 315
<210> 19
<211> 309
<212> PRT
<213> 人类
<400> 19
Met Gly Pro Gly Leu Leu Cys Trp Val Leu Leu Cys Leu Leu Gly Ala
1 5 10 15
Gly Pro Val Asp Ala Gly Val Thr Gln Ser Pro Thr His Leu Ile Lys
20 25 30
Thr Arg Gly Gln His Val Thr Leu Arg Cys Ser Pro Ile Ser Gly His
35 40 45
Lys Ser Val Ser Trp Tyr Gln Gln Val Leu Gly Gln Gly Pro Gln Phe
50 55 60
Ile Phe Gln Tyr Tyr Glu Lys Glu Glu Arg Gly Arg Gly Asn Phe Pro
65 70 75 80
Asp Arg Phe Ser Ala Arg Gln Phe Pro Asn Tyr Ser Ser Glu Leu Asn
85 90 95
Val Asn Ala Leu Leu Leu Gly Asp Ser Ala Leu Tyr Leu Cys Ala Ser
100 105 110
Ser Phe Asp Val Gly Leu Pro Pro Leu His Phe Gly Asn Gly Thr Arg
115 120 125
Leu Thr Val Thr Glu Asp Leu Asn Lys Val Phe Pro Pro Glu Val Ala
130 135 140
Val Phe Glu Pro Ser Glu Ala Glu Ile Ser His Thr Gln Lys Ala Thr
145 150 155 160
Leu Val Cys Leu Ala Thr Gly Phe Phe Pro Asp His Val Glu Leu Ser
165 170 175
Trp Trp Val Asn Gly Lys Glu Val His Ser Gly Val Ser Thr Asp Pro
180 185 190
Gln Pro Leu Lys Glu Gln Pro Ala Leu Asn Asp Ser Arg Tyr Cys Leu
195 200 205
Ser Ser Arg Leu Arg Val Ser Ala Thr Phe Trp Gln Asn Pro Arg Asn
210 215 220
His Phe Arg Cys Gln Val Gln Phe Tyr Gly Leu Ser Glu Asn Asp Glu
225 230 235 240
Trp Thr Gln Asp Arg Ala Lys Pro Val Thr Gln Ile Val Ser Ala Glu
245 250 255
Ala Trp Gly Arg Ala Asp Cys Gly Phe Thr Ser Val Ser Tyr Gln Gln
260 265 270
Gly Val Leu Ser Ala Thr Ile Leu Tyr Glu Ile Leu Leu Gly Lys Ala
275 280 285
Thr Leu Tyr Ala Val Leu Val Ser Ala Leu Val Leu Met Ala Met Val
290 295 300
Lys Arg Lys Asp Phe
305
<210> 20
<211> 308
<212> PRT
<213> 人类
<400> 20
Met Gly Ser Trp Thr Leu Cys Cys Val Ser Leu Cys Ile Leu Val Ala
1 5 10 15
Lys His Thr Asp Ala Gly Val Ile Gln Ser Pro Arg His Glu Val Thr
20 25 30
Glu Met Gly Gln Glu Val Thr Leu Arg Cys Lys Pro Ile Ser Gly His
35 40 45
Asp Tyr Leu Phe Trp Tyr Arg Gln Thr Met Met Arg Gly Leu Glu Leu
50 55 60
Leu Ile Tyr Phe Asn Asn Asn Val Pro Ile Asp Asp Ser Gly Met Pro
65 70 75 80
Glu Asp Arg Phe Ser Ala Lys Met Pro Asn Ala Ser Phe Ser Thr Leu
85 90 95
Lys Ile Gln Pro Ser Glu Pro Arg Asp Ser Ala Val Tyr Phe Cys Ala
100 105 110
Ser Ser Tyr Arg Gly Thr Glu Ala Phe Phe Gly Gln Gly Thr Arg Leu
115 120 125
Thr Val Val Glu Asp Leu Asn Lys Val Phe Pro Pro Glu Val Ala Val
130 135 140
Phe Glu Pro Ser Glu Ala Glu Ile Ser His Thr Gln Lys Ala Thr Leu
145 150 155 160
Val Cys Leu Ala Thr Gly Phe Phe Pro Asp His Val Glu Leu Ser Trp
165 170 175
Trp Val Asn Gly Lys Glu Val His Ser Gly Val Ser Thr Asp Pro Gln
180 185 190
Pro Leu Lys Glu Gln Pro Ala Leu Asn Asp Ser Arg Tyr Cys Leu Ser
195 200 205
Ser Arg Leu Arg Val Ser Ala Thr Phe Trp Gln Asn Pro Arg Asn His
210 215 220
Phe Arg Cys Gln Val Gln Phe Tyr Gly Leu Ser Glu Asn Asp Glu Trp
225 230 235 240
Thr Gln Asp Arg Ala Lys Pro Val Thr Gln Ile Val Ser Ala Glu Ala
245 250 255
Trp Gly Arg Ala Asp Cys Gly Phe Thr Ser Val Ser Tyr Gln Gln Gly
260 265 270
Val Leu Ser Ala Thr Ile Leu Tyr Glu Ile Leu Leu Gly Lys Ala Thr
275 280 285
Leu Tyr Ala Val Leu Val Ser Ala Leu Val Leu Met Ala Met Val Lys
290 295 300
Arg Lys Asp Phe
305
<210> 21
<211> 311
<212> PRT
<213> 人类
<400> 21
Met Gly Ile Arg Leu Leu Cys Arg Val Ala Phe Cys Phe Leu Ala Val
1 5 10 15
Gly Leu Val Asp Val Lys Val Thr Gln Ser Ser Arg Tyr Leu Val Lys
20 25 30
Arg Thr Gly Glu Lys Val Phe Leu Glu Cys Val Gln Asp Met Asp His
35 40 45
Glu Asn Met Phe Trp Tyr Arg Gln Asp Pro Gly Leu Gly Leu Arg Leu
50 55 60
Ile Tyr Phe Ser Tyr Asp Val Lys Met Lys Glu Lys Gly Asp Ile Pro
65 70 75 80
Glu Gly Tyr Ser Val Ser Arg Glu Lys Lys Glu Arg Phe Ser Leu Ile
85 90 95
Leu Glu Ser Ala Ser Thr Asn Gln Thr Ser Met Tyr Leu Cys Ala Ser
100 105 110
Ser Leu Gly Ala Thr Gly Ala Asn Glu Lys Leu Phe Phe Gly Ser Gly
115 120 125
Thr Gln Leu Ser Val Leu Glu Asp Leu Asn Lys Val Phe Pro Pro Glu
130 135 140
Val Ala Val Phe Glu Pro Ser Glu Ala Glu Ile Ser His Thr Gln Lys
145 150 155 160
Ala Thr Leu Val Cys Leu Ala Thr Gly Phe Phe Pro Asp His Val Glu
165 170 175
Leu Ser Trp Trp Val Asn Gly Lys Glu Val His Ser Gly Val Ser Thr
180 185 190
Asp Pro Gln Pro Leu Lys Glu Gln Pro Ala Leu Asn Asp Ser Arg Tyr
195 200 205
Cys Leu Ser Ser Arg Leu Arg Val Ser Ala Thr Phe Trp Gln Asn Pro
210 215 220
Arg Asn His Phe Arg Cys Gln Val Gln Phe Tyr Gly Leu Ser Glu Asn
225 230 235 240
Asp Glu Trp Thr Gln Asp Arg Ala Lys Pro Val Thr Gln Ile Val Ser
245 250 255
Ala Glu Ala Trp Gly Arg Ala Asp Cys Gly Phe Thr Ser Val Ser Tyr
260 265 270
Gln Gln Gly Val Leu Ser Ala Thr Ile Leu Tyr Glu Ile Leu Leu Gly
275 280 285
Lys Ala Thr Leu Tyr Ala Val Leu Val Ser Ala Leu Val Leu Met Ala
290 295 300
Met Val Lys Arg Lys Asp Phe
305 310
<210> 22
<211> 311
<212> PRT
<213> 人类
<400> 22
Met Leu Ser Leu Leu Leu Leu Leu Leu Gly Leu Gly Ser Val Phe Ser
1 5 10 15
Ala Val Ile Ser Gln Lys Pro Ser Arg Asp Ile Cys Gln Arg Gly Thr
20 25 30
Ser Leu Thr Ile Gln Cys Gln Val Asp Ser Gln Val Thr Met Met Phe
35 40 45
Trp Tyr Arg Gln Gln Pro Gly Gln Ser Leu Thr Leu Ile Ala Thr Ala
50 55 60
Asn Gln Gly Ser Glu Ala Thr Tyr Glu Ser Gly Phe Val Ile Asp Lys
65 70 75 80
Phe Pro Ile Ser Arg Pro Asn Leu Thr Phe Ser Thr Leu Thr Val Ser
85 90 95
Asn Met Ser Pro Glu Asp Ser Ser Ile Tyr Leu Cys Ser Val Gly Ala
100 105 110
Gly Gln Gly Pro Tyr Thr Asp Thr Gln Tyr Phe Gly Pro Gly Thr Arg
115 120 125
Leu Thr Val Leu Glu Asp Leu Lys Asn Val Phe Pro Pro Glu Val Ala
130 135 140
Val Phe Glu Pro Ser Glu Ala Glu Ile Ser His Thr Gln Lys Ala Thr
145 150 155 160
Leu Val Cys Leu Ala Thr Gly Phe Tyr Pro Asp His Val Glu Leu Ser
165 170 175
Trp Trp Val Asn Gly Lys Glu Val His Ser Gly Val Ser Thr Asp Pro
180 185 190
Gln Pro Leu Lys Glu Gln Pro Ala Leu Asn Asp Ser Arg Tyr Cys Leu
195 200 205
Ser Ser Arg Leu Arg Val Ser Ala Thr Phe Trp Gln Asn Pro Arg Asn
210 215 220
His Phe Arg Cys Gln Val Gln Phe Tyr Gly Leu Ser Glu Asn Asp Glu
225 230 235 240
Trp Thr Gln Asp Arg Ala Lys Pro Val Thr Gln Ile Val Ser Ala Glu
245 250 255
Ala Trp Gly Arg Ala Asp Cys Gly Phe Thr Ser Glu Ser Tyr Gln Gln
260 265 270
Gly Val Leu Ser Ala Thr Ile Leu Tyr Glu Ile Leu Leu Gly Lys Ala
275 280 285
Thr Leu Tyr Ala Val Leu Val Ser Ala Leu Val Leu Met Ala Met Val
290 295 300
Lys Arg Lys Asp Ser Arg Gly
305 310
<210> 23
<211> 312
<212> PRT
<213> 人类
<400> 23
Met Ser Ile Gly Leu Leu Cys Cys Val Ala Phe Ser Leu Leu Trp Ala
1 5 10 15
Ser Pro Val Asn Ala Gly Val Thr Gln Thr Pro Lys Phe Gln Val Leu
20 25 30
Lys Thr Gly Gln Ser Met Thr Leu Gln Cys Ala Gln Asp Met Asn His
35 40 45
Asn Ser Met Tyr Trp Tyr Arg Gln Asp Pro Gly Met Gly Leu Arg Leu
50 55 60
Ile Tyr Tyr Ser Ala Ser Glu Gly Thr Thr Asp Lys Gly Glu Val Pro
65 70 75 80
Asn Gly Tyr Asn Val Ser Arg Leu Asn Lys Arg Glu Phe Ser Leu Arg
85 90 95
Leu Glu Ser Ala Ala Pro Ser Gln Thr Ser Val Tyr Phe Cys Ala Ser
100 105 110
Ser Glu Val Thr Gly Gly Tyr Asn Glu Gln Phe Phe Gly Pro Gly Thr
115 120 125
Arg Leu Thr Val Leu Glu Asp Leu Lys Asn Val Phe Pro Pro Glu Val
130 135 140
Ala Val Phe Glu Pro Ser Glu Ala Glu Ile Ser His Thr Gln Lys Ala
145 150 155 160
Thr Leu Val Cys Leu Ala Thr Gly Phe Tyr Pro Asp His Val Glu Leu
165 170 175
Ser Trp Trp Val Asn Gly Lys Glu Val His Ser Gly Val Ser Thr Asp
180 185 190
Pro Gln Pro Leu Lys Glu Gln Pro Ala Leu Asn Asp Ser Arg Tyr Cys
195 200 205
Leu Ser Ser Arg Leu Arg Val Ser Ala Thr Phe Trp Gln Asn Pro Arg
210 215 220
Asn His Phe Arg Cys Gln Val Gln Phe Tyr Gly Leu Ser Glu Asn Asp
225 230 235 240
Glu Trp Thr Gln Asp Arg Ala Lys Pro Val Thr Gln Ile Val Ser Ala
245 250 255
Glu Ala Trp Gly Arg Ala Asp Cys Gly Phe Thr Ser Glu Ser Tyr Gln
260 265 270
Gln Gly Val Leu Ser Ala Thr Ile Leu Tyr Glu Ile Leu Leu Gly Lys
275 280 285
Ala Thr Leu Tyr Ala Val Leu Val Ser Ala Leu Val Leu Met Ala Met
290 295 300
Val Lys Arg Lys Asp Ser Arg Gly
305 310
<210> 24
<211> 307
<212> PRT
<213> 人类
<400> 24
Met Leu Ser Leu Leu Leu Leu Leu Leu Gly Leu Gly Ser Val Phe Ser
1 5 10 15
Ala Val Ile Ser Gln Lys Pro Ser Arg Asp Ile Cys Gln Arg Gly Thr
20 25 30
Ser Leu Thr Ile Gln Cys Gln Val Asp Ser Gln Val Thr Met Met Phe
35 40 45
Trp Tyr Arg Gln Gln Pro Gly Gln Ser Leu Thr Leu Ile Ala Thr Ala
50 55 60
Asn Gln Gly Ser Glu Ala Thr Tyr Glu Ser Gly Phe Val Ile Asp Lys
65 70 75 80
Phe Pro Ile Ser Arg Pro Asn Leu Thr Phe Ser Thr Leu Thr Val Ser
85 90 95
Asn Met Ser Pro Glu Asp Ser Ser Ile Tyr Leu Cys Ser Val Glu Gly
100 105 110
Arg Gly Tyr Glu Gln Tyr Phe Gly Pro Gly Thr Arg Leu Thr Val Thr
115 120 125
Glu Asp Leu Lys Asn Val Phe Pro Pro Glu Val Ala Val Phe Glu Pro
130 135 140
Ser Glu Ala Glu Ile Ser His Thr Gln Lys Ala Thr Leu Val Cys Leu
145 150 155 160
Ala Thr Gly Phe Tyr Pro Asp His Val Glu Leu Ser Trp Trp Val Asn
165 170 175
Gly Lys Glu Val His Ser Gly Val Ser Thr Asp Pro Gln Pro Leu Lys
180 185 190
Glu Gln Pro Ala Leu Asn Asp Ser Arg Tyr Cys Leu Ser Ser Arg Leu
195 200 205
Arg Val Ser Ala Thr Phe Trp Gln Asn Pro Arg Asn His Phe Arg Cys
210 215 220
Gln Val Gln Phe Tyr Gly Leu Ser Glu Asn Asp Glu Trp Thr Gln Asp
225 230 235 240
Arg Ala Lys Pro Val Thr Gln Ile Val Ser Ala Glu Ala Trp Gly Arg
245 250 255
Ala Asp Cys Gly Phe Thr Ser Glu Ser Tyr Gln Gln Gly Val Leu Ser
260 265 270
Ala Thr Ile Leu Tyr Glu Ile Leu Leu Gly Lys Ala Thr Leu Tyr Ala
275 280 285
Val Leu Val Ser Ala Leu Val Leu Met Ala Met Val Lys Arg Lys Asp
290 295 300
Ser Arg Gly
305
<210> 25
<211> 310
<212> PRT
<213> 人类
<400> 25
Met Gln Trp Ala Leu Ala Val Leu Leu Ala Phe Leu Ser Pro Ala Ser
1 5 10 15
Gln Lys Ser Ser Asn Leu Glu Gly Arg Thr Lys Ser Val Ile Arg Gln
20 25 30
Thr Gly Ser Ser Ala Glu Ile Thr Cys Asp Leu Ala Glu Gly Ser Thr
35 40 45
Gly Tyr Ile His Trp Tyr Leu His Gln Glu Gly Lys Ala Pro Gln Arg
50 55 60
Leu Leu Tyr Tyr Asp Ser Tyr Thr Ser Ser Val Val Leu Glu Ser Gly
65 70 75 80
Ile Ser Pro Gly Lys Tyr Asp Thr Tyr Gly Ser Thr Arg Lys Asn Leu
85 90 95
Arg Met Ile Leu Arg Asn Leu Ile Glu Asn Asp Ser Gly Val Tyr Tyr
100 105 110
Cys Ala Thr Trp Glu Thr Gln Glu Leu Gly Lys Lys Ile Lys Val Phe
115 120 125
Gly Pro Gly Thr Lys Leu Ile Ile Thr Asp Lys Gln Leu Asp Ala Asp
130 135 140
Val Ser Pro Lys Pro Thr Ile Phe Leu Pro Ser Ile Ala Glu Thr Lys
145 150 155 160
Leu Gln Lys Ala Gly Thr Tyr Leu Cys Leu Leu Glu Lys Phe Phe Pro
165 170 175
Asp Val Ile Lys Ile His Trp Gln Glu Lys Lys Ser Asn Thr Ile Leu
180 185 190
Gly Ser Gln Glu Gly Asn Thr Met Lys Thr Asn Asp Thr Tyr Met Lys
195 200 205
Phe Ser Trp Leu Thr Val Pro Glu Lys Ser Leu Asp Lys Glu His Arg
210 215 220
Cys Ile Val Arg His Glu Asn Asn Lys Asn Gly Val Asp Gln Glu Ile
225 230 235 240
Ile Phe Pro Pro Ile Lys Thr Asp Val Ile Thr Met Asp Pro Lys Asp
245 250 255
Asn Cys Ser Lys Asp Ala Asn Asp Thr Leu Leu Leu Gln Leu Thr Asn
260 265 270
Thr Ser Ala Tyr Tyr Met Tyr Leu Leu Leu Leu Leu Lys Ser Val Val
275 280 285
Tyr Phe Ala Ile Ile Thr Cys Cys Leu Leu Arg Arg Thr Ala Phe Cys
290 295 300
Cys Asn Gly Glu Lys Ser
305 310
<210> 26
<211> 295
<212> PRT
<213> 人类
<400> 26
Met Leu Phe Ser Ser Leu Leu Cys Val Phe Val Ala Phe Ser Tyr Ser
1 5 10 15
Gly Ser Ser Val Ala Gln Lys Val Thr Gln Ala Gln Ser Ser Val Ser
20 25 30
Met Pro Val Arg Lys Ala Val Thr Leu Asn Cys Leu Tyr Glu Thr Ser
35 40 45
Trp Trp Ser Tyr Tyr Ile Phe Trp Tyr Lys Gln Leu Pro Ser Lys Glu
50 55 60
Met Ile Phe Leu Ile Arg Gln Gly Ser Asp Glu Gln Asn Ala Lys Ser
65 70 75 80
Gly Arg Tyr Ser Val Asn Phe Lys Lys Ala Val Lys Ser Val Ala Leu
85 90 95
Thr Ile Ser Ala Leu Gln Leu Glu Asp Ser Ala Lys Tyr Phe Cys Ala
100 105 110
Leu Gly Val Gln Ala Leu Leu Pro Ile Leu Gly Asp Thr Thr Asp Lys
115 120 125
Leu Ile Phe Gly Lys Gly Thr Arg Val Thr Val Glu Pro Arg Ser Gln
130 135 140
Pro His Thr Lys Pro Ser Val Phe Val Met Lys Asn Gly Thr Asn Val
145 150 155 160
Ala Cys Leu Val Lys Glu Phe Tyr Pro Lys Asp Ile Arg Ile Asn Leu
165 170 175
Val Ser Ser Lys Lys Ile Thr Glu Phe Asp Pro Ala Ile Val Ile Ser
180 185 190
Pro Ser Gly Lys Tyr Asn Ala Val Lys Leu Gly Lys Tyr Glu Asp Ser
195 200 205
Asn Ser Val Thr Cys Ser Val Gln His Asp Asn Lys Thr Val His Ser
210 215 220
Thr Asp Phe Glu Val Lys Thr Asp Ser Thr Asp His Val Lys Pro Lys
225 230 235 240
Glu Thr Glu Asn Thr Lys Gln Pro Ser Lys Ser Cys His Lys Pro Lys
245 250 255
Ala Ile Val His Thr Glu Lys Val Asn Met Met Ser Leu Thr Val Leu
260 265 270
Gly Leu Arg Met Leu Phe Ala Lys Thr Val Ala Val Asn Phe Leu Leu
275 280 285
Thr Ala Lys Leu Phe Phe Leu
290 295
<210> 27
<211> 801
<212> DNA
<213> 人类
<400> 27
atgtggggag ttttccttct ttatgtttcc atgaagatgg gaggcactac aggacaaaac 60
attgaccagc ccactgagat gacagctacg gaaggtgcca ttgtccagat caactgcacg 120
taccagacat ctgggttcaa cgggctgttc tggtaccagc aacatgctgg cgaagcaccc 180
acatttctgt cttacaatgt tctggatggt ttggaggaga aaggtcgttt ttcttcattc 240
cttagtcggt ctaaagggta cagttacctc cttttgaagg agctccagat gaaagactct 300
gcctcttacc tctgtgctgt gatggatagc agctataaat tgatcttcgg gagtgggacc 360
agactgctgg tcaggcctga tatccagaac cctgaccctg ccgtgtacca gctgagagac 420
tctaaatcca gtgacaagtc tgtctgccta ttcaccgatt ttgattctca aacaaatgtg 480
tcacaaagta aggattctga tgtgtatatc acagacaaaa ctgtgctaga catgaggtct 540
atggacttca agagcaacag tgctgtggcc tggagcaaca aatctgactt tgcatgtgca 600
aacgccttca acaacagcat tattccagaa gacaccttct tccccagccc agaaagttcc 660
tgtgatgtca agctggtcga gaaaagcttt gaaacagata cgaacctaaa ctttcaaaac 720
ctgtcagtga ttgggttccg aatcctcctc ctgaaagtgg ccgggtttaa tctgctcatg 780
acgctgcggc tgtggtccag c 801
<210> 28
<211> 813
<212> DNA
<213> 人类
<400> 28
atgctactca tcacatcaat gttggtctta tggatgcaat tgtcacaggt gaatggacaa 60
caggtaatgc aaattcctca gtaccagcat gtacaagaag gagaggactt caccacgtac 120
tgcaattcct caactacttt aagcaatata cagtggtata agcaaaggcc tggtggacat 180
cccgtttttt tgatacagtt agtgaagagt ggagaagtga agaagcagaa aagactgaca 240
tttcagtttg gagaagcaaa aaagaacagc tccctgcaca tcacagccac ccagactaca 300
gatgtaggaa cctacttctg tgcggctgct ggtggtacta gctatggaaa gctgacattt 360
ggacaaggga ccatcttgac tgtccatcca aatatccaga accctgaccc tgccgtgtac 420
cagctgagag actctaaatc cagtgacaag tctgtctgcc tattcaccga ttttgattct 480
caaacaaatg tgtcacaaag taaggattct gatgtgtata tcacagacaa aactgtgcta 540
gacatgaggt ctatggactt caagagcaac agtgctgtgg cctggagcaa caaatctgac 600
tttgcatgtg caaacgcctt caacaacagc attattccag aagacacctt cttccccagc 660
ccagaaagtt cctgtgatgt caagctggtc gagaaaagct ttgaaacaga tacgaaccta 720
aactttcaaa acctgtcagt gattgggttc cgaatcctcc tcctgaaagt ggccgggttt 780
aatctgctca tgacgctgcg gctgtggtcc agc 813
<210> 29
<211> 830
<212> DNA
<213> 人类
<400> 29
atgaagacat ttgctggatt ttcgttcctg tttttgtggc tgcagctgga ctgtatgagt 60
agaggagagg atgtggagca gagtcttttc ctgagtgtcc gagagggaga cagctccgtt 120
ataaactgca cttacacaga cagctcctcc acctacttat actggtataa gcaagaacct 180
ggagcaggtc tccagttgct gacgtatatt ttttcaaata tggacatgaa acaagaccaa 240
agactcactg ttctattgaa taaaaaggat aaacatctgt ctctgcgcat tgcagacacc 300
cagactgggg actcagctat ctacttctgt gcagagacct ggaccgacag aggctcaacc 360
ctggggaggc tatactttgg aagaggaact cagttgactg tctggcctga tatccagaac 420
cctgaccctg ccgtgtacca gctgagagac tctaaatcca gtgacaagtc tgtctgccta 480
ttcaccgatt ttgattctca aacaaatgtg tcacaaagta aggattctga tgtgtatatc 540
acagacaaaa ctgtgctaga catgaggtct atggacttca agagcaacag tgctgtggcc 600
tggagcaaca aatctgactt tgcatgtgca aacgccttca acaacagcat tattccagaa 660
gacaccttct tccccagccc agaaagttcc tgtgatgtca agctggtcga gaaaagcttt 720
gaaacagata cgaacctaaa ctttcaaaac ctgtcagtga ttgggttccg aatcctcctc 780
ctgaaagtgg ccgggtttaa tctgctcatg acgttgcggc tgtggtccag 830
<210> 30
<211> 840
<212> DNA
<213> 人类
<400> 30
atggccatgc tcctgggggc atcagtgctg attctgtggc ttcagacaga ctgggtaaac 60
agtcaacaga agaatgatga ccagcaagtt aagcaaaatt caccatccct gagcgtccag 120
gaaggaagaa tttctattct gaactgtgac tatactaaca gcatgtttga ttatttccta 180
tggtacaaaa aataccctgc tgaaggtcct acattcctga tatctataag ttccattaag 240
gataaaaatg aagatggaag attcactgtc ttcttaaaca aaagtgccaa gcacctctct 300
ctgcacattg tgccctccca gcctggagac tctgcagtgt acttctgtgc agcaagtctt 360
tataaccagg gaggaaagct tatcttcgga cagggaacgg agttatctgt gaaacccaat 420
atccagaacc ctgaccctgc cgtgtaccag ctgagagact ctaaatccag tgacaagtct 480
gtctgcctat tcaccgattt tgattctcaa acaaatgtgt cacaaagtaa ggattctgat 540
gtgtatatca cagacaaaac tgtgctagac atgaggtcta tggacttcaa gagcaacagt 600
gctgtggcct ggagcaacaa atctgacttt gcatgtgcaa acgccttcaa caacagcatt 660
attccagaag acaccttctt ccccagccca gaaagttcct gtgatgtcaa gctggtcgag 720
aaaagctttg aaacagatac gaacctaaac tttcaaaacc tgtcagtgat tgggttccga 780
atcctcctcc tgaaagtggc cgggtttaat ctgctcatga cgctgcggct gtggtccagc 840
<210> 31
<211> 822
<212> DNA
<213> 人类
<400> 31
atggagaaga atcctttggc agccccatta ctaatcctct ggtttcatct tgactgcgtg 60
agcagcatac tgaacgtgga acaaagtcct cagtcactgc atgttcagga gggagacagc 120
accaatttca cctgcagctt cccttccagc aatttttatg ccttacactg gtacagatgg 180
gaaactgcaa aaagccccga ggccttgttt gtaatgactt taaatgggga tgaaaagaag 240
aaaggacgaa taagtgccac tcttaatacc aaggagggtt acagctattt gtacatcaaa 300
ggatcccagc ctgaagactc agccacatac ctctgtgcct cgggggattc cgggtatgca 360
ctcaacttcg gcaaaggcac ctcgctgttg gtcacacccc atatccagaa ccctgaccct 420
gccgtgtacc agctgagaga ctctaaatcc agtgacaagt ctgtctgcct attcaccgat 480
tttgattctc aaacaaatgt gtcacaaagt aaggattctg atgtgtatat cacagacaaa 540
actgtgctag acatgaggtc tatggacttc aagagcaaca gtgctgtggc ctggagcaac 600
aaatctgact ttgcatgtgc aaacgccttc aacaacagca ttattccaga agacaccttc 660
ttccccagcc cagaaagttc ctgtgatgtc aagctggtcg agaaaagctt tgaaacagat 720
acgaacctaa actttcaaaa cctgtcagtg attgggttcc gaatcctcct cctgaaagtg 780
gccgggttta atctgctcat gacgctgcgg ctgtggtcca gc 822
<210> 32
<211> 828
<212> DNA
<213> 人类
<400> 32
atgaactatt ctccaggctt agtatctctg atactcttac tgcttggaag aacccgtgga 60
aattcagtga cccagatgga agggccagtg actctctcag aagaggcctt cctgactata 120
aactgcacgt acacagccac aggataccct tcccttttct ggtatgtcca atatcctgga 180
gaaggtctac agctcctcct gaaagccacg aaggctgatg acaagggaag caacaaaggt 240
tttgaagcca cataccgtaa agaaaccact tctttccact tggagaaagg ctcagttcaa 300
gtgtcagact cagcggtgta cttctgtgct ctgacaatat gggattatgg aggaagccaa 360
ggaaatctca tctttggaaa aggcactaaa ctctctgtta aaccaaatat ccagaaccct 420
gaccctgccg tgtaccagct gagagactct aaatccagtg acaagtctgt ctgcctattc 480
accgattttg attctcaaac aaatgtgtca caaagtaagg attctgatgt gtatatcaca 540
gacaaaactg tgctagacat gaggtctatg gacttcaaga gcaacagtgc tgtggcctgg 600
agcaacaaat ctgactttgc atgtgcaaac gccttcaaca acagcattat tccagaagac 660
accttcttcc ccagcccaga aagttcctgt gatgtcaagc tggtcgagaa aagctttgaa 720
acagatacga acctaaactt tcaaaacctg tcagtgattg ggttccgaat cctcctcctg 780
aaagtggccg ggtttaatct gctcatgacg ctgcggctgt ggtccagc 828
<210> 33
<211> 807
<212> DNA
<213> 人类
<400> 33
atggtcctga aattctccgt gtccattctt tggattcagt tggcatgggt gagcacccag 60
ctgctggagc agagccctca gtttctaagc atccaagagg gagaaaatct cactgtgtac 120
tgcaactcct caagtgtttt ttccagctta caatggtaca gacaggagcc tggggaaggt 180
cctgtcctcc tggtgacagt agttacgggt ggagaagtga agaagctgaa gagactaacc 240
tttcagtttg gtgatgcaag aaaggacagt tctctccaca tcactgcagc ccagcctggt 300
gatacaggcc tctacctctg tgcaggagaa aattccgggt atgcactcaa cttcggcaaa 360
ggcacctcgc tgttggtcac accccatatc cagaaccctg accctgccgt gtaccagctg 420
agagactcta aatccagtga caagtctgtc tgcctattca ccgattttga ttctcaaaca 480
aatgtgtcac aaagtaagga ttctgatgtg tatatcacag acaaaactgt gctagacatg 540
aggtctatgg acttcaagag caacagtgct gtggcctgga gcaacaaatc tgactttgca 600
tgtgcaaacg ccttcaacaa cagcattatt ccagaagaca ccttcttccc cagcccagaa 660
agttcctgtg atgtcaagct ggtcgagaaa agctttgaaa cagatacgaa cctaaacttt 720
caaaacctgt cagtgattgg gttccgaatc ctcctcctga aagtggccgg gtttaatctg 780
ctcatgacgc tgcggctgtg gtccagc 807
<210> 34
<211> 825
<212> DNA
<213> 人类
<400> 34
atgatgaaat ccttgagagt tttactggtg atcctgtggc ttcagttaag ctgggtttgg 60
agccaacaga aggaggtgga gcaggatcct ggaccactca gtgttccaga gggagccatt 120
gtttctctca actgcactta cagcaacagt gcttttcaat acttcatgtg gtacagacag 180
tattccagaa aaggccctga gttgctgatg tacacatact ccagtggtaa caaagaagat 240
ggaaggttta cagcacaggt cgataaatcc agcaagtata tctccttgtt catcagagac 300
tcacagccca gtgattcagc cacctacctc tgtgcaatga gcctatcagg aggaagctac 360
atacctacat ttggaagagg aaccagcctt attgttcatc cgtatatcca gaaccctgac 420
cctgccgtgt accagctgag agactctaaa tccagtgaca agtctgtctg cctattcacc 480
gattttgatt ctcaaacaaa tgtgtcacaa agtaaggatt ctgatgtgta tatcacagac 540
aaaactgtgc tagacatgag gtctatggac ttcaagagca acagtgctgt ggcctggagc 600
aacaaatctg actttgcatg tgcaaacgcc ttcaacaaca gcattattcc agaagacacc 660
ttcttcccca gcccagaaag ttcctgtgat gtcaagctgg tcgagaaaag ctttgaaaca 720
gatacgaacc taaactttca aaacctgtca gtgattgggt tccgaatcct cctcctgaaa 780
gtggccgggt ttaatctgct catgacgctg cggctgtggt ccagc 825
<210> 35
<211> 825
<212> DNA
<213> 人类
<400> 35
atgctccttg aacatttatt aataatcttg tggatgcagc tgacatgggt cagtggtcaa 60
cagctgaatc agagtcctca atctatgttt atccaggaag gagaagatgt ctccatgaac 120
tgcacttctt caagcatatt taacacctgg ctatggtaca agcaggaccc tggggaaggt 180
cctgtcctct tgatagcctt atataaggct ggtgaattga cctcaaatgg aagactgact 240
gctcagtttg gtataaccag aaaggacagc ttcctgaata tctcagcatc catacctagt 300
gatgtaggca tctacttctg tgctgggcag ctaggagggg ctggtggtac tagctatgga 360
aagctgacat ttggacaagg gaccatcttg actgtccatc caaatatcca gaaccctgac 420
cctgccgtgt accagctgag agactctaaa tccagtgaca agtctgtctg cctattcacc 480
gattttgatt ctcaaacaaa tgtgtcacaa agtaaggatt ctgatgtgta tatcacagac 540
aaaactgtgc tagacatgag gtctatggac ttcaagagca acagtgctgt ggcctggagc 600
aacaaatctg actttgcatg tgcaaacgcc ttcaacaaca gcattattcc agaagacacc 660
ttcttcccca gcccagaaag ttcctgtgat gtcaagctgg tcgagaaaag ctttgaaaca 720
gatacgaacc taaactttca aaacctgtca gtgattgggt tccgaatcct cctcctgaaa 780
gtggccgggt ttaatctgct catgacgctg cggctgtggt ccagc 825
<210> 36
<211> 822
<212> DNA
<213> 人类
<400> 36
atgacatcca ttcgagctgt atttatattc ctgtggctgc agctggactt ggtgaatgga 60
gagaatgtgg agcagcatcc ttcaaccctg agtgtccagg agggagacag cgctgttatc 120
aagtgtactt attcagacag tgcctcaaac tacttccctt ggtataagca agaacttgga 180
aaaggacctc agcttattat agacattcgt tcaaatgtgg gcgaaaagaa agaccaacga 240
attgctgtta cattgaacaa gacagccaaa catttctccc tgcacatcac agagacccaa 300
cctgaagact cggctgtcta cttctgtgca gcaaactgga gcccgcaagg aaatgagaaa 360
ttaacctttg ggactggaac aagactcacc atcataccca atatccagaa ccctgaccct 420
gccgtgtacc agctgagaga ctctaaatcc agtgacaagt ctgtctgcct attcaccgat 480
tttgattctc aaacaaatgt gtcacaaagt aaggattctg atgtgtatat cacagacaaa 540
actgtgctag acatgaggtc tatggacttc aagagcaaca gtgctgtggc ctggagcaac 600
aaatctgact ttgcatgtgc aaacgccttc aacaacagca ttattccaga agacaccttc 660
ttccccagcc cagaaagttc ctgtgatgtc aagctggtcg agaaaagctt tgaaacagat 720
acgaacctaa actttcaaaa cctgtcagtg attgggttcc gaatcctcct cctgaaagtg 780
gccgggttta atctgctcat gacgctgcgg ctgtggtcca gc 822
<210> 37
<211> 801
<212> DNA
<213> 人类
<400> 37
atgtggggag ttttccttct ttatgtttcc atgaagatgg gaggcactac aggacaaaac 60
attgaccagc ccactgagat gacagctacg gaaggtgcca ttgtccagat caactgcacg 120
taccagacat ctgggttcaa cgggctgttc tggtaccagc aacatgctgg cgaagcaccc 180
acatttctgt cttacaatgt tctggatggt ttggaggaga aaggtcgttt ttcttcattc 240
cttagtcggt ctaaagggta cagttacctc cttttgaagg agctccagat gaaagactct 300
gcctcttacc tctgtgcttc catggatagc aactatcagt taatctgggg cgctgggacc 360
aagctaatta taaagccaga tatccagaac cctgaccctg ccgtgtacca gctgagagac 420
tctaaatcca gtgacaagtc tgtctgccta ttcaccgatt ttgattctca aacaaatgtg 480
tcacaaagta aggattctga tgtgtatatc acagacaaaa ctgtgctaga catgaggtct 540
atggacttca agagcaacag tgctgtggcc tggagcaaca aatctgactt tgcatgtgca 600
aacgccttca acaacagcat tattccagaa gacaccttct tccccagccc agaaagttcc 660
tgtgatgtca agctggtcga gaaaagcttt gaaacagata cgaacctaaa ctttcaaaac 720
ctgtcagtga ttgggttccg aatcctcctc ctgaaagtgg ccgggtttaa tctgctcatg 780
acgctgcggc tgtggtccag c 801
<210> 38
<211> 822
<212> DNA
<213> 人类
<400> 38
atgatatcct tgagagtttt actggtgatc ctgtggcttc agttaagctg ggtttggagc 60
caacggaagg aggtggagca ggatcctgga cccttcaatg ttccagaggg agccactgtc 120
gctttcaact gtacttacag caacagtgct tctcagtctt tcttctggta cagacaggat 180
tgcaggaaag aacctaagtt gctgatgtcc gtatactcca gtggtaatga agatggaagg 240
tttacagcac agctcaatag agccagccag tatatttccc tgctcatcag agactccaag 300
ctcagtgatt cagccaccta cctctgtgtg gtgaacagat tcacaaggga tggaaacaaa 360
ctggtctttg gcgcaggaac cattctgaga gtcaagtcct atatccagaa ccctgaccct 420
gccgtgtacc agctgagaga ctctaaatcc agtgacaagt ctgtctgcct attcaccgat 480
tttgattctc aaacaaatgt gtcacaaagt aaggattctg atgtgtatat cacagacaaa 540
actgtgctag acatgaggtc tatggacttc aagagcaaca gtgctgtggc ctggagcaac 600
aaatctgact ttgcatgtgc aaacgccttc aacaacagca ttattccaga agacaccttc 660
ttccccagcc cagaaagttc ctgtgatgtc aagctggtcg agaaaagctt tgaaacagat 720
acgaacctaa actttcaaaa cctgtcagtg attgggttcc gaatcctcct cctgaaagtg 780
gccgggttta atctgctcat gacgctgcgg ctgtggtcca gc 822
<210> 39
<211> 942
<212> DNA
<213> 人类
<400> 39
atgctgctgc ttctgctgct tctggggcca ggctccgggc ttggtgctgt cgtctctcaa 60
catccgagct gggttatctg taagagtgga acctctgtga agatcgagtg ccgttccctg 120
gactttcagg ccacaactat gttttggtat cgtcagttcc cgaaacagag tctcatgctg 180
atggcaactt ccaatgaggg ctccaaggcc acatacgagc aaggcgtcga gaaggacaag 240
tttctcatca accatgcaag cctgaccttg tccactctga cagtgaccag tgcccatcct 300
gaagacagca gcttctacat ctgcagtgcg aaggtgacta gcgggcaaca ccaagggacc 360
acagatacgc agtattttgg cccaggcacc cggctgacag tgctcgagga cctgaaaaac 420
gtgttcccac ccgaggtcgc tgtgtttgag ccatcagaag cagagatctc ccacacccaa 480
aaggccacac tggtgtgcct ggccacaggc ttctaccccg accacgtgga gctgagctgg 540
tgggtgaatg ggaaggaggt gcacagtggg gtcagcacag acccgcagcc cctcaaggag 600
cagcccgccc tcaatgactc cagatactgc ctgagcagcc gcctgagggt ctcggccacc 660
ttctggcaga acccccgcaa ccacttccgc tgtcaagtcc agttctacgg gctctcggag 720
aatgacgagt ggacccagga tagggccaaa cctgtcaccc agatcgtcag cgccgaggcc 780
tggggtagag cagactgtgg cttcacctcc gagtcttacc agcaaggggt cctgtctgcc 840
accatcctct atgagatctt gctagggaag gccaccttgt atgccgtgct ggtcagtgcc 900
ctcgtgctga tggccatggt caagagaaag gattccagag gc 942
<210> 40
<211> 933
<212> DNA
<213> 人类
<400> 40
atgactatca ggctcctctg ctacatgggc ttttattttc tgggggcagg cctcatggaa 60
gctgacatct accagacccc aagatacctt gttataggga caggaaagaa gatcactctg 120
gaatgttctc aaaccatggg ccatgacaaa atgtactggt atcaacaaga tccaggaatg 180
gaactacacc tcatccacta ttcctatgga gttaattcca cagagaaggg agatctttcc 240
tctgagtcaa cagtctccag aataaggacg gagcattttc ccctgaccct ggagtctgcc 300
aggccctcac atacctctca gtacctctgt gccagcagtg aatatatcca gtactctgga 360
aacaccatat attttggaga gggaagttgg ctcactgttg tagaggacct gaacaaggtg 420
ttcccacccg aggtcgctgt gtttgagcca tcagaagcag agatctccca cacccaaaag 480
gccacactgg tgtgcctggc cacaggcttc ttccctgacc acgtggagct gagctggtgg 540
gtgaatggga aggaggtgca cagtggggtc agcacggacc cgcagcccct caaggagcag 600
cccgccctca atgactccag atactgcctg agcagccgcc tgagggtctc ggccaccttc 660
tggcagaacc cccgcaacca cttccgctgt caagtccagt tctacgggct ctcggagaat 720
gacgagtgga cccaggatag ggccaaaccc gtcacccaga tcgtcagcgc cgaggcctgg 780
ggtagagcag actgtggctt tacctcggtg tcctaccagc aaggggtcct gtctgccacc 840
atcctctatg agatcctgct agggaaggcc accctgtatg ctgtgctggt cagcgccctt 900
gtgttgatgg ccatggtcaa gagaaaggat ttc 933
<210> 41
<211> 936
<212> DNA
<213> 人类
<400> 41
atgggcttca ggctcctctg ctgtgtggcc ttttgtctcc tgggagcagg cccagtggat 60
tctggagtca cacaaacccc aaagcacctg atcacagcaa ctggacagcg agtgacgctg 120
agatgctccc ctaggtctgg agacctctct gtgtactggt accaacagag cctggaccag 180
ggcctccagt tcctcattca gtattataat ggagaagaga gagcaaaagg aaacattctt 240
gaacgattct ccgcacaaca gttccctgac ttgcactctg aactaaacct gagctctctg 300
gagctggggg actcagcttt gtatttctgt gccagcagcg tcggaggggg attggcagat 360
acgcagtatt ttggcccagg cacccggctg acagtgctcg aggacctgaa aaacgtgttc 420
ccacccgagg tcgctgtgtt tgagccatca gaagcagaga tctcccacac ccaaaaggcc 480
acactggtgt gcctggccac aggcttctac cccgaccacg tggagctgag ctggtgggtg 540
aatgggaagg aggtgcacag tggggtcagc acagacccgc agcccctcaa ggagcagccc 600
gccctcaatg actccagata ctgcctgagc agccgcctga gggtctcggc caccttctgg 660
cagaaccccc gcaaccactt ccgctgtcaa gtccagttct acgggctctc ggagaatgac 720
gagtggaccc aggatagggc caaacctgtc acccagatcg tcagcgccga ggcctggggt 780
agagcagact gtggcttcac ctccgagtct taccagcaag gggtcctgtc tgccaccatc 840
ctctatgaga tcttgctagg gaaggccacc ttgtatgccg tgctggtcag tgccctcgtg 900
ctgatggcca tggtcaagag aaaggattcc agaggc 936
<210> 42
<211> 939
<212> DNA
<213> 人类
<400> 42
atgagcatcg gcctcctgtg ctgtgcagcc ttgtctctcc tgtgggcagg tccagtgaat 60
gctggtgtca ctcagacccc aaaattccag gtcctgaaga caggacagag catgacactg 120
cagtgtgccc aggatatgaa ccatgaatac atgtcctggt atcgacaaga cccaggcatg 180
gggctgaggc tgattcatta ctcagttggt gctggtatca ctgaccaagg agaagtcccc 240
aatggctaca atgtctccag atcaaccaca gaggatttcc cgctcaggct gctgtcggct 300
gctccctccc agacatctgt gtacttctgt gccagcggaa tcagcgggac agcgagctcc 360
tataattcac ccctccactt tgggaacggg accaggctca ctgtgacaga ggacctgaac 420
aaggtgttcc cacccgaggt cgctgtgttt gagccatcag aagcagagat ctcccacacc 480
caaaaggcca cactggtgtg cctggccaca ggcttcttcc ctgaccacgt ggagctgagc 540
tggtgggtga atgggaagga ggtgcacagt ggggtcagca cggacccgca gcccctcaag 600
gagcagcccg ccctcaatga ctccagatac tgcctgagca gccgcctgag ggtctcggcc 660
accttctggc agaacccccg caaccacttc cgctgtcaag tccagttcta cgggctctcg 720
gagaatgacg agtggaccca ggatagggcc aaacccgtca cccagatcgt cagcgccgag 780
gcctggggta gagcagactg tggctttacc tcggtgtcct accagcaagg ggtcctgtct 840
gccaccatcc tctatgagat cctgctaggg aaggccaccc tgtatgctgt gctggtcagc 900
gcccttgtgt tgatggccat ggtcaagaga aaggatttc 939
<210> 43
<211> 927
<212> DNA
<213> 人类
<400> 43
atgggtcctg ggcttctcca ctggatggcc ctttgtctcc ttggaacagg tcatggggat 60
gccatggtca tccagaaccc aagataccag gttacccagt ttggaaagcc agtgaccctg 120
agttgttctc agactttgaa ccataacgtc atgtactggt accagcagaa gtcaagtcag 180
gccccaaagc tgctgttcca ctactatgac aaagatttta acaatgaagc agacacccct 240
gataacttcc aatccaggag gccgaacact tctttctgct ttcttgacat ccgctcacca 300
ggcctggggg acgcagccat gtacctgtgt gccaccagca gagagtggga gacccagtac 360
ttcgggccag gcacgcggct cctggtgctc gaggacctga aaaacgtgtt cccacccgag 420
gtcgctgtgt ttgagccatc agaagcagag atctcccaca cccaaaaggc cacactggtg 480
tgcctggcca caggcttcta ccccgaccac gtggagctga gctggtgggt gaatgggaag 540
gaggtgcaca gtggggtcag cacagacccg cagcccctca aggagcagcc cgccctcaat 600
gactccagat actgcctgag cagccgcctg agggtctcgg ccaccttctg gcagaacccc 660
cgcaaccact tccgctgtca agtccagttc tacgggctct cggagaatga cgagtggacc 720
caggataggg ccaaacctgt cacccagatc gtcagcgccg aggcctgggg tagagcagac 780
tgtggcttca cctccgagtc ttaccagcaa ggggtcctgt ctgccaccat cctctatgag 840
atcttgctag ggaaggccac cttgtatgcc gtgctggtca gtgccctcgt gctgatggcc 900
atggtcaaga gaaaggattc cagaggc 927
<210> 44
<211> 945
<212> DNA
<213> 人类
<400> 44
atgactatca ggctcctctg ctacatgggc ttttattttc tgggggcagg cctcatggaa 60
gctgacatct accagacccc aagatacctt gttataggga caggaaagaa gatcactctg 120
gaatgttctc aaaccatggg ccatgacaaa atgtactggt atcaacaaga tccaggaatg 180
gaactacacc tcatccacta ttcctatgga gttaattcca cagagaaggg agatctttcc 240
tctgagtcaa cagtctccag aataaggacg gagcattttc ccctgaccct ggagtctgcc 300
aggccctcac atacctctca gtacctctgt gccagcagcc aactttaccg ggacacctcg 360
aacaccgggg agctgttttt tggagaaggc tctaggctga ccgtactgga ggacctgaaa 420
aacgtgttcc cacccgaggt cgctgtgttt gagccatcag aagcagagat ctcccacacc 480
caaaaggcca cactggtgtg cctggccaca ggcttctacc ccgaccacgt ggagctgagc 540
tggtgggtga atgggaagga ggtgcacagt ggggtcagca cagacccgca gcccctcaag 600
gagcagcccg ccctcaatga ctccagatac tgcctgagca gccgcctgag ggtctcggcc 660
accttctggc agaacccccg caaccacttc cgctgtcaag tccagttcta cgggctctcg 720
gagaatgacg agtggaccca ggatagggcc aaacctgtca cccagatcgt cagcgccgag 780
gcctggggta gagcagactg tggcttcacc tccgagtctt accagcaagg ggtcctgtct 840
gccaccatcc tctatgagat cttgctaggg aaggccacct tgtatgccgt gctggtcagt 900
gccctcgtgc tgatggccat ggtcaagaga aaggattcca gaggc 945
<210> 45
<211> 927
<212> DNA
<213> 人类
<400> 45
atgggccctg ggctcctctg ctgggtgctg ctttgtctcc tgggagcagg cccagtggac 60
gctggagtca cccaaagtcc cacacacctg atcaaaacga gaggacagca cgtgactctg 120
agatgctctc ctatctctgg gcacaagagt gtgtcctggt accaacaggt cctgggtcag 180
gggccccagt ttatctttca gtattatgag aaagaagaga gaggaagagg aaacttccct 240
gatcgattct cagctcgcca gttccctaac tatagctctg agctgaatgt gaacgccttg 300
ttgctggggg actcggccct gtatctctgt gccagcagct ttgacgttgg tttgccaccc 360
ctccactttg ggaacgggac caggctcact gtgacagagg acctgaacaa ggtgttccca 420
cccgaggtcg ctgtgtttga gccatcagaa gcagagatct cccacaccca aaaggccaca 480
ctggtgtgcc tggccacagg cttcttccct gaccacgtgg agctgagctg gtgggtgaat 540
gggaaggagg tgcacagtgg ggtcagcacg gacccgcagc ccctcaagga gcagcccgcc 600
ctcaatgact ccagatactg cctgagcagc cgcctgaggg tctcggccac cttctggcag 660
aacccccgca accacttccg ctgtcaagtc cagttctacg ggctctcgga gaatgacgag 720
tggacccagg atagggccaa acccgtcacc cagatcgtca gcgccgaggc ctggggtaga 780
gcagactgtg gctttacctc ggtgtcctac cagcaagggg tcctgtctgc caccatcctc 840
tatgagatcc tgctagggaa ggccaccctg tatgctgtgc tggtcagcgc ccttgtgttg 900
atggccatgg tcaagagaaa ggatttc 927
<210> 46
<211> 924
<212> DNA
<213> 人类
<400> 46
atgggctcct ggaccctctg ctgtgtgtcc ctttgcatcc tggtagcaaa gcacacagat 60
gctggagtta tccagtcacc ccggcacgag gtgacagaga tgggacaaga agtgactctg 120
agatgtaaac caatttcagg acacgactac cttttctggt acagacagac catgatgcgg 180
ggactggagt tgctcattta ctttaacaac aacgttccga tagatgattc agggatgccc 240
gaggatcgat tctcagctaa gatgcctaat gcatcattct ccactctgaa gatccagccc 300
tcagaaccca gggactcagc tgtgtacttc tgtgccagca gctacagggg cactgaagct 360
ttctttggac aaggcaccag actcacagtt gtagaggacc tgaacaaggt gttcccaccc 420
gaggtcgctg tgtttgagcc atcagaagca gagatctccc acacccaaaa ggccacactg 480
gtgtgcctgg ccacaggctt cttccctgac cacgtggagc tgagctggtg ggtgaatggg 540
aaggaggtgc acagtggggt cagcacggac ccgcagcccc tcaaggagca gcccgccctc 600
aatgactcca gatactgcct gagcagccgc ctgagggtct cggccacctt ctggcagaac 660
ccccgcaacc acttccgctg tcaagtccag ttctacgggc tctcggagaa tgacgagtgg 720
acccaggata gggccaaacc cgtcacccag atcgtcagcg ccgaggcctg gggtagagca 780
gactgtggct ttacctcggt gtcctaccag caaggggtcc tgtctgccac catcctctat 840
gagatcctgc tagggaaggc caccctgtat gctgtgctgg tcagcgccct tgtgttgatg 900
gccatggtca agagaaagga tttc 924
<210> 47
<211> 933
<212> DNA
<213> 人类
<400> 47
atgggaatca ggctcctgtg tcgtgtggcc ttttgtttcc tggctgtagg cctcgtagat 60
gtgaaagtaa cccagagctc gagatatcta gtcaaaagga cgggagagaa agtttttctg 120
gaatgtgtcc aggatatgga ccatgaaaat atgttctggt atcgacaaga cccaggtctg 180
gggctacggc tgatctattt ctcatatgat gttaaaatga aagaaaaagg agatattcct 240
gaggggtaca gtgtctctag agagaagaag gagcgcttct ccctgattct ggagtccgcc 300
agcaccaacc agacatctat gtacctctgt gccagcagct taggggcgac aggggctaat 360
gaaaaactgt tttttggcag tggaacccag ctctctgtct tggaggacct gaacaaggtg 420
ttcccacccg aggtcgctgt gtttgagcca tcagaagcag agatctccca cacccaaaag 480
gccacactgg tgtgcctggc cacaggcttc ttccctgacc acgtggagct gagctggtgg 540
gtgaatggga aggaggtgca cagtggggtc agcacggacc cgcagcccct caaggagcag 600
cccgccctca atgactccag atactgcctg agcagccgcc tgagggtctc ggccaccttc 660
tggcagaacc cccgcaacca cttccgctgt caagtccagt tctacgggct ctcggagaat 720
gacgagtgga cccaggatag ggccaaaccc gtcacccaga tcgtcagcgc cgaggcctgg 780
ggtagagcag actgtggctt tacctcggtg tcctaccagc aaggggtcct gtctgccacc 840
atcctctatg agatcctgct agggaaggcc accctgtatg ctgtgctggt cagcgccctt 900
gtgttgatgg ccatggtcaa gagaaaggat ttc 933
<210> 48
<211> 933
<212> DNA
<213> 人类
<400> 48
atgctgagtc ttctgctcct tctcctggga ctaggctctg tgttcagtgc tgtcatctct 60
caaaagccaa gcagggatat ctgtcaacgt ggaacctccc tgacgatcca gtgtcaagtc 120
gatagccaag tcaccatgat gttctggtac cgtcagcaac ctggacagag cctgacactg 180
atcgcaactg caaatcaggg ctctgaggcc acatatgaga gtggatttgt cattgacaag 240
tttcccatca gccgcccaaa cctaacattc tcaactctga ctgtgagcaa catgagccct 300
gaagacagca gcatatatct ctgcagcgtt ggggcggggc aaggacctta cacagatacg 360
cagtattttg gcccaggcac ccggctgaca gtgctcgagg acctgaaaaa cgtgttccca 420
cccgaggtcg ctgtgtttga gccatcagaa gcagagatct cccacaccca aaaggccaca 480
ctggtgtgcc tggccacagg cttctacccc gaccacgtgg agctgagctg gtgggtgaat 540
gggaaggagg tgcacagtgg ggtcagcaca gacccgcagc ccctcaagga gcagcccgcc 600
ctcaatgact ccagatactg cctgagcagc cgcctgaggg tctcggccac cttctggcag 660
aacccccgca accacttccg ctgtcaagtc cagttctacg ggctctcgga gaatgacgag 720
tggacccagg atagggccaa acctgtcacc cagatcgtca gcgccgaggc ctggggtaga 780
gcagactgtg gcttcacctc cgagtcttac cagcaagggg tcctgtctgc caccatcctc 840
tatgagatct tgctagggaa ggccaccttg tatgccgtgc tggtcagtgc cctcgtgctg 900
atggccatgg tcaagagaaa ggattccaga ggc 933
<210> 49
<211> 936
<212> DNA
<213> 人类
<400> 49
atgagcatcg gcctcctgtg ctgtgtggcc ttttctctcc tgtgggcaag tccagtgaat 60
gctggtgtca ctcagacccc aaaattccag gtcctgaaga caggacagag catgacactg 120
cagtgtgccc aggatatgaa ccataactcc atgtactggt atcgacaaga cccaggcatg 180
ggactgaggc tgatttatta ctcagcttct gagggtacca ctgacaaagg agaagtcccc 240
aatggctaca atgtctccag attaaacaaa cgggagttct cgctcaggct ggagtcggct 300
gctccctccc agacatctgt gtacttctgt gccagcagtg aggtgacagg gggatacaat 360
gagcagttct tcgggccagg gacacggctc accgtgctag aggacctgaa aaacgtgttc 420
ccacccgagg tcgctgtgtt tgagccatca gaagcagaga tctcccacac ccaaaaggcc 480
acactggtgt gcctggccac aggcttctac cccgaccacg tggagctgag ctggtgggtg 540
aatgggaagg aggtgcacag tggggtcagc acagacccgc agcccctcaa ggagcagccc 600
gccctcaatg actccagata ctgcctgagc agccgcctga gggtctcggc caccttctgg 660
cagaaccccc gcaaccactt ccgctgtcaa gtccagttct acgggctctc ggagaatgac 720
gagtggaccc aggatagggc caaacctgtc acccagatcg tcagcgccga ggcctggggt 780
agagcagact gtggcttcac ctccgagtct taccagcaag gggtcctgtc tgccaccatc 840
ctctatgaga tcttgctagg gaaggccacc ttgtatgccg tgctggtcag tgccctcgtg 900
ctgatggcca tggtcaagag aaaggattcc agaggc 936
<210> 50
<211> 921
<212> DNA
<213> 人类
<400> 50
atgctgagtc ttctgctcct tctcctggga ctaggctctg tgttcagtgc tgtcatctct 60
caaaagccaa gcagggatat ctgtcaacgt ggaacctccc tgacgatcca gtgtcaagtc 120
gatagccaag tcaccatgat gttctggtac cgtcagcaac ctggacagag cctgacactg 180
atcgcaactg caaatcaggg ctctgaggcc acatatgaga gtggatttgt cattgacaag 240
tttcccatca gccgcccaaa cctaacattc tcaactctga ctgtgagcaa catgagccct 300
gaagacagca gcatatatct ctgcagcgtt gaaggcaggg gttacgagca gtacttcggg 360
ccgggcacca ggctcacggt cacagaggac ctgaaaaacg tgttcccacc cgaggtcgct 420
gtgtttgagc catcagaagc agagatctcc cacacccaaa aggccacact ggtgtgcctg 480
gccacaggct tctaccccga ccacgtggag ctgagctggt gggtgaatgg gaaggaggtg 540
cacagtgggg tcagcacaga cccgcagccc ctcaaggagc agcccgccct caatgactcc 600
agatactgcc tgagcagccg cctgagggtc tcggccacct tctggcagaa cccccgcaac 660
cacttccgct gtcaagtcca gttctacggg ctctcggaga atgacgagtg gacccaggat 720
agggccaaac ctgtcaccca gatcgtcagc gccgaggcct ggggtagagc agactgtggc 780
ttcacctccg agtcttacca gcaaggggtc ctgtctgcca ccatcctcta tgagatcttg 840
ctagggaagg ccaccttgta tgccgtgctg gtcagtgccc tcgtgctgat ggccatggtc 900
aagagaaagg attccagagg c 921
<210> 51
<211> 930
<212> DNA
<213> 人类
<400> 51
atgcagtggg ccctagcggt gcttctagct ttcctgtctc ctgccagtca gaaatcttcc 60
aacttggaag ggagaacgaa gtcagtcatc aggcagactg ggtcatctgc tgaaatcact 120
tgtgatcttg ctgaaggaag taccggctac atccactggt acctacacca ggaggggaag 180
gccccacagc gtcttctgta ctatgactcc tacacctcca gcgttgtgtt ggaatcagga 240
atcagcccag ggaagtatga tacttatgga agcacaagga agaacttgag aatgatactg 300
cgaaatctta ttgaaaatga ctctggagtc tattactgtg ccacctggga aactcaagag 360
ttgggcaaaa aaatcaaggt atttggtccc ggaacaaagc ttatcattac agataaacaa 420
cttgatgcag atgtttcccc caagcccact atttttcttc cttcaattgc tgaaacaaag 480
ctccagaagg ctggaacata cctttgtctt cttgagaaat ttttccctga tgttattaag 540
atacattggc aagaaaagaa gagcaacacg attctgggat cccaggaggg gaacaccatg 600
aagactaacg acacatacat gaaatttagc tggttaacgg tgccagaaaa gtcactggac 660
aaagaacaca gatgtatcgt cagacatgag aataataaaa acggagttga tcaagaaatt 720
atctttcctc caataaagac agatgtcatc acaatggatc ccaaagacaa ttgttcaaaa 780
gatgcaaatg atacactact gctgcagctc acaaacacct ctgcatatta catgtacctc 840
ctcctgctcc tcaagagtgt ggtctatttt gccatcatca cctgctgtct gcttagaaga 900
acggctttct gctgcaatgg agagaaatca 930
<210> 52
<211> 885
<212> DNA
<213> 人类
<400> 52
atgctgttct ccagcctgct gtgtgtattt gtggccttca gctactctgg atcaagtgtg 60
gcccagaagg ttactcaagc ccagtcatca gtatccatgc cagtgaggaa agcagtcacc 120
ctgaactgcc tgtatgaaac aagttggtgg tcatattata ttttttggta caagcaactt 180
cccagcaaag agatgatttt ccttattcgc cagggttctg atgaacagaa tgcaaaaagt 240
ggtcgctatt ctgtcaactt caagaaagca gtgaaatccg tcgccttaac catttcagcc 300
ttacagctag aagattcagc aaagtacttt tgtgctcttg gggtccaagc cctcctaccc 360
atactggggg ataccaccga taaactcatc tttggaaaag gaacccgtgt gactgtggaa 420
ccaagaagtc agcctcatac caaaccatcc gtttttgtca tgaaaaatgg aacaaatgtc 480
gcttgtctgg tgaaggaatt ctaccccaag gatataagaa taaatctcgt gtcatccaag 540
aagataacag agtttgatcc tgctattgtc atctctccca gtgggaagta caatgctgtc 600
aagcttggta aatatgaaga ttcaaattca gtgacatgtt cagttcaaca cgacaataaa 660
actgtgcact ccactgactt tgaagtgaag acagattcta cagatcacgt aaaaccaaag 720
gaaactgaaa acacaaagca accttcaaag agctgccata aacccaaagc catagttcat 780
accgagaagg tgaacatgat gtccctcaca gtgcttgggc tacgaatgct gtttgcaaag 840
actgttgccg tcaattttct cttgactgcc aagttatttt tcttg 885
<210> 53
<211> 22
<212> DNA
<213> 人类
<400> 53
ctcggcaggc cgagccacgg gc 22
<210> 54
<211> 22
<212> DNA
<213> 人类
<400> 54
gcccgtggct cggcctgccg ag 22
<210> 55
<211> 27
<212> DNA
<213> 人工序列
<220>
<223> 具有限制性位点的引物
<400> 55
ctcgagatgt ctcgctccgt ggcctta 27
<210> 56
<211> 32
<212> DNA
<213> 人工序列
<220>
<223> 具有限制性位点的引物
<400> 56
gtgtgagttt tgtcgctagc ctgggggacc tg 32
<210> 57
<211> 32
<212> DNA
<213> 人工序列
<220>
<223> 具有限制性位点的引物
<400> 57
caggtccccc aggctagcga caaaactcac ac 32
<210> 58
<211> 31
<212> DNA
<213> 人工序列
<220>
<223> 具有限制性位点的引物
<400> 58
gcggccgctc atttacccgg agacagggag a 31
Claims (27)
1.一种分离表达T细胞受体的T细胞的方法,所述T细胞受体能够特异性结合由与MR1分子关联的癌细胞呈递的抗原,所述方法包含以下步骤:
a.提供T细胞制剂;然后
b.在接触步骤中使所述T细胞制剂与表达MR1的癌细胞接触;
c.在分离步骤中将与所述癌细胞特异性反应的T细胞分离。
2.根据权利要求1所述的方法,其中所述接触步骤包含扩增步骤,其中所述分离的T细胞制剂在所述表达MR1的癌细胞的存在下扩增。
3.根据权利要求1或2所述的方法,其中所述扩增步骤在IL-2和/或IL-7和/或IL-15的存在下进行。
4.根据前述权利要求中任一项所述的方法,其中所述分离步骤包含利用对CD3、CD69、CD137、CD150和/或ICOS的细胞表面标记物具有特异性的配体染色所述T细胞制剂,特别是其中所述分离步骤包括选定CD3+CD137+、和/或CD3+ CD69+、和/或CD3+ CD150+、和/或CD3+ICOS+ T细胞,之后进行流式细胞术分析和细胞分选,特别是通过使用FACS或磁分离进行细胞分选。
5.根据前述权利要求中任一项所述的方法,其中所述对细胞表面标记物具有特异性的配体是抗体或类抗体分子。
6.根据前述权利要求中任一项所述的方法,其中所述分离步骤包含选定这样一种T细胞,当用表达MR1的细胞刺激时,与用不表达MR1的细胞刺激相比,其从选自IFN-γ和/或GM-CSF的细胞因子释放两倍的表达量。
7.根据前述权利要求中任一项所述的方法,还包括确定用于编码在所述分离步骤中分离的T细胞的T细胞受体的核酸序列。
8.一种制备表达T细胞受体的MR1T细胞制剂的方法,所述T细胞受体能够结合由与MR1分子关联的癌细胞呈递的抗原,所述方法包括以下步骤:
a.提供从患者获得的肿瘤样品;
b.将所述肿瘤样品与以下物质接触:
i.多个T细胞克隆,其中每个T细胞克隆的特征在于具有MR1T细胞受体,其能够特异性地结合由与MR1分子关联的癌细胞呈递的抗原;或者
ii.从MR1T细胞受体分子中分离的多个被标记和多聚化的可溶性TCR。
c.识别与所述肿瘤样品特异性反应的MR1T细胞受体;
d.提供T细胞制剂;
e.将一核酸表达构建体引入所述T细胞制剂从而产生转基因T细胞制剂,所述核酸构建体编码在所述T细胞克隆上表达的MR1反应性T细胞受体分子,其在步骤c中被识别出与所述肿瘤样品特异性反应。
9.根据权利要求8所述的方法,其中所述T细胞制剂是从同一患者处获得(自体过继性T细胞疗法)。
10.根据权利要求8所述的方法,其中所述T细胞制剂从另一个受试者获得,特别是HLA匹配的受试者(同种异体过继性T细胞疗法)。
11.根据权利要求8所述的方法,其中从所述患者获得的所述T细胞制剂是从患者的外周血中获得,特别是其中所述T细胞制剂是通过选定PBMC来表达一种或多种选自CD4、CD8、CD27、CD45RA和CD57的T细胞标记物获得的,特别是选定CD3+ CD4+、或CD3+ CD8+、或CD3+CD27+ CD45RA+、或CD3+ CD27+CD45RA-、或CD3+ CD27- CD45RA-、或CD3+ CD57-或CD3+ CD57+T细胞。
12.根据权利要求8所述的方法,其中从所述患者获得的所述T细胞制剂是经过肿瘤活检接着体外扩增后获得。
13.一种通过权利要求8至12所述的任一方法获得的MR1特异性T细胞制剂,所述制剂用于治疗或预防癌症的方法,特别是治疗或预防通过MR1表达来表征的癌症的方法。
14.一种表达载体,所述表达载体包含编码以下物质的核酸序列:
a.功能性T细胞受体异二聚体;
或
b.T细胞受体α链,所述T细胞受体α链能够与T细胞受体β链一起形成功能性T细胞受体异二聚体;和/或
c.T细胞受体β链,所述T细胞受体β链能够与T细胞受体α链一起形成功能性T细胞受体异二聚体;
或
d.T细胞受体γ链,所述T细胞受体γ链能够与T细胞受体δ链一起形成功能性T细胞受体异二聚体;和/或
e.T细胞受体δ链,所述T细胞受体δ链能够与T细胞受体γ链一起形成功能性T细胞受体异二聚体,
其中所述T细胞受体异二聚体与MR1分子特异性结合,其中所述MR1分子在肿瘤细胞上表达并呈递肿瘤相关抗原,以及特别是所述核酸序列:
i.即是或包含选自SEQ ID NO.027至SEQ ID NO.038的核酸序列、和/或编码选自SEQID NO.001至SEQ ID NO.012的氨基酸序列;和/或
ii.即是或包含选自SEQ ID NO.039至SEQ ID NO.050的核酸序列和/或编码选自SEQID NO.013至SEQ ID NO.024的氨基酸序列;
或
iii.即是或包含SEQ ID NO.051的核酸序列和/或编码SEQ ID NO.025的氨基酸序列;
和/或
iv.即是或包含SEQ ID NO.052的核酸序列和/或编码SEQ ID NO.026的氨基酸序列。
15.一种分离的与MR1分子结合的T细胞受体蛋白异二聚体,其中所述MR1分子在肿瘤细胞上表达,特别是其中所述T细胞受体蛋白异二聚体已通过根据权利要求1至7中任一项所述的方法鉴别。
16.根据权利要求15所述的分离的与MR1分子结合的T细胞受体蛋白异二聚体,其中所述MR1分子呈递肿瘤相关抗原。
17.根据权利要求15或16所述的分离的T细胞受体蛋白异二聚体,其中所述分离的T细胞受体蛋白包含选自SEQ ID NO.001至SEQ ID NO.012的氨基酸序列和选自SEQ ID NO.013至SEQ ID NO.024的氨基酸序列、或SEQ ID NO.025和SEQ ID NO.026的氨基酸序列。
18.根据权利要求17所述的分离的T细胞受体蛋白异二聚体,其中所述分离的T细胞受体蛋白包含一对选自以下序列的氨基酸序列:
a.SEQ ID NO.001和SEQ ID NO.023;
b.SEQ ID NO.002和SEQ ID NO.022;
c.SEQ ID NO.003和SEQ ID NO.021;
d.SEQ ID NO.004和SEQ ID NO.020;
e.SEQ ID NO.005和SEQ ID NO.019;
f.SEQ ID NO.006和SEQ ID NO.017;
g.SEQ ID NO.007和SEQ ID NO.018;
h.SEQ ID NO.008和SEQ ID NO.016;
i.SEQ ID NO.009和SEQ ID NO.015;
j.SEQ ID NO.010和SEQ ID NO.014;
k.SEQ ID NO.011和SEQ ID NO.013;
l.SEQ ID NO.012和SEQ ID NO.024;或
m.SEQ ID NO.025和SEQ ID NO.026。
19.一种重组细胞,所述重组细胞包含根据权利要求14所述的表达载体或根据权利要求15至18中的任一项所述的T细胞受体蛋白异二聚体,其中所述重组细胞是从如下地方获取的T细胞:
a.外周血;或
b.肿瘤浸润淋巴细胞。
20.根据权利要求18.a的重组细胞,所述重组细胞用于治疗或预防癌症的方法,特别是治疗或预防通过MR1表达来表征的癌症的方法。
21.根据权利要求20所述的用于治疗或预防癌症的方法的重组细胞,其中所述细胞通过过继性T细胞免疫疗法施用。
22.核酸序列的集合,其中所述集合的每个序列促进哺乳动物细胞中不同T细胞受体α链、T细胞受体β链或T细胞受体α链和β链组合的表达,其中所述组合能够与呈递癌抗原的MR1分子特异性结合。
23.根据权利要求22所述的核酸序列集合,其中所述集合包含选自SEQ ID NO.027至SEQ ID NO.052的序列和/或包含编码选自SEQ ID NO.001至SEQ ID NO.026的T细胞受体分子(或构成α、β、γ或δ链的T细胞受体)的序列。
24.一种重组T细胞集合,其中所述集合的每个细胞作为转基因体表达能够与呈递癌抗原的MR1分子特异性结合的T细胞受体。
25.根据权利要求24所述的T细胞集合,其中所述集合包含含有根据权利要求15至18所述的T细胞受体分子的细胞。
26.一种用于癌症治疗的核酸表达载体,所述核酸表达载体包含通过哺乳动物细胞中能够运作的启动子序列控制的编码MR1的核酸序列。
27.根据权利要求26所述的表达MR1的用于癌症治疗的表达核酸表达载体,其中所述表达MR1的核酸表达载体在给施用以下物质之前、同时或之后施用:
a.一种重组细胞,所述重组细胞包含根据权利要求14所述的表达载体或根据权利要求15至18中的任一项所述的T细胞受体蛋白异二聚体,和/或
b.一种通过权利要求8至12所述的任一项的方法获得的MR1特异性T细胞制剂,和/或
c.一种根据权利要求14所述的表达载体。
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