JP2022105535A - 抗lag-3抗体及びその使用方法 - Google Patents
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Abstract
Description
本出願は、2016年10月11日に出願された米国仮出願第62/406,766号、2016年11月10日に出願された同第62/420,280号の優先権の利益を主張し、各々は参照により全体が本明細書に組み込まれる。
(a)CDRH1は、DX1YX2X3のアミノ酸配列(配列番号140)を含み、式中
X1は、TまたはNであり、
X2は、IまたはMであり、及び
X3は、H、Y、またはDであり、
(b)CDRH2は、X1IDPANX2X3X4X5X6X7PX8X9QX10のアミノ酸配列(配列番号142)を含み、式中
X1は、E、R、S、またはKであり、
X2は、DまたはGであり、
X3は、NまたはHであり、
X4は、TまたはSであり、
X5は、KまたはHであり、
X6は、YまたはFであり、
X7は、DまたはAであり、
X8は、KまたはRであり、
X9は、FまたはLであり、及び
X10は、GまたはDであり、
(c)CDRH3は、YX1X2X3YX4VGGX5DYのアミノ酸配列(配列番号144)を含み、式中
X1は、Y、F、またはSであり、
X2は、YまたはDであり、
X3は、KまたはRであり、
X4は、DまたはEであり、及び
X5は、FまたはCであり、
(d)CDRL1は、SVSSX1ISSSX2LX3のアミノ酸配列(配列番号147)を含み、式中
X1は、SまたはGであり、
X2は、NまたはTであり、及び
X3は、HまたはYであり、
(e)CDRL2は、GTSNLASのアミノ酸配列(配列番号104)を含み、及び
(f)CDRL3は、QQWX1X2YPX3Tのアミノ酸配列(配列番号149)を含み、式中
X1は、S、N、またはRであり、
X2は、S、T、またはRであり、及び
X3は、F、L、H、またはWである、抗体または単離抗体を提供する。
(a)CDRH1は、DX1YX2X3のアミノ酸配列(配列番号140)を含み、式中
X1は、TまたはNであり、
X2は、IまたはMであり、及び
X3は、H、Y、またはDであり、
(b)CDRH2は、X1IDPANX2X3X4X5X6X7PX8X9QX10のアミノ酸配列(配列番号142)を含み、式中
X1は、E、R、S、またはKであり、
X2は、DまたはGであり、
X3は、NまたはHであり、
X4は、TまたはSであり、
X5は、KまたはHであり、
X6は、YまたはFであり、
X7は、DまたはAであり、
X8は、KまたはRであり、
X9は、FまたはLであり、及び
X10は、GまたはDであり、
(c)CDRH3は、YX1X2X3YX4VGGX5DYのアミノ酸配列(配列番号144)を含み、式中
X1は、Y、F、またはSであり、
X2は、YまたはDであり、
X3は、KまたはRであり、
X4は、DまたはEであり、及び
X5は、FまたはCであり、
(d)CDRL1は、SVSSX1ISSSX2LX3のアミノ酸配列(配列番号147)を含み、式中
X1は、SまたはGであり、
X2は、NまたはTであり、及び
X3は、HまたはYであり、
(e)CDRL2は、GTSNLASのアミノ酸配列(配列番号104)を含み、及び
(f)CDRL3は、QQWX1X2YPX3Tのアミノ酸配列(配列番号149)を含み、式中
X1は、S、N、またはRであり、
X2は、S、T、またはRであり、及び
X3は、F、L、H、またはWである、抗体または単離抗体を提供する。
(a)CDRH1は、DTYIHのアミノ酸配列(配列番号79)を含み、
(b)CDRH2は、EIDPANDNTKYDPKFQGのアミノ酸配列(配列番号90)を含み、
(c)CDRH3は、YYYX1YX2VGGFDYのアミノ酸配列(配列番号146)を含み、式中:X1は、KまたはRであり、及びX2は、DまたはEであり、
(d)CDRL1は、SVSSSISSSNLHのアミノ酸配列(配列番号100)を含み、
(e)CDRL2は、GTSNLASのアミノ酸配列(配列番号104)を含み、及び
(f)CDRL3は、QQWSSYPFTのアミノ酸配列(配列番号105)を含む。
本明細書で使用される場合、「約」及び「およそ」という用語は、数値または数値範囲を修飾するために使用される場合、5%~10%上回り(例えば、最大で5%~10%上回る)、かつ5%~10%下回る(例えば、最大で5%~10%下回る)その値または範囲の偏差が、列挙される値または範囲の意図される意味に留まることを示す。
一態様では、本開示は、LAG-3(例えば、ヒトLAG-3)に特異的に結合し、LAG-3機能を拮抗する、抗体を提供する。例示的抗体のアミノ酸配列は、本明細書の表1~7に記載される。
当業者であれば、N末端EまたはQアミノ酸残基が、ある特定の条件下で、遊離アミノ基の翻訳後の環化によってピログルタミン酸に自発的に変換し、ラクタムを形成できることが理解できるであろう。したがって、ある特定の実施形態では、本開示は、本明細書に開示される抗体重鎖可変領域もしくは軽鎖可変領域(例えば、それぞれ、配列番号56~72及び73~77、)または本明細書に開示される完全長重鎖もしくは軽鎖(例えば、それぞれ、配列番号168~186及び187~191)を含む抗体であって、N末端EまたはQアミノ酸残基が、(例えば、N末端EまたはQ残基の遊離アミノ基の翻訳後の環化の結果として)ピログルタミン酸に変換されている、抗体を提供する。
(a)CDRH1は、DX1YX2X3のアミノ酸配列(配列番号140)を含み、式中
X1は、TまたはNであり、
X2は、IまたはMであり、及び
X3は、H、Y、またはDであり、
(b)CDRH2は、X1IDPANX2X3X4X5X6X7PX8X9QX10のアミノ酸配列(配列番号142)を含み、式中
X1は、E、R、S、またはKであり、
X2は、DまたはGであり、
X3は、NまたはHであり、
X4は、TまたはSであり、
X5は、KまたはHであり、
X6は、YまたはFであり、
X7は、DまたはAであり、
X8は、KまたはRであり、
X9は、FまたはLであり、及び
X10は、GまたはDであり、
(c)CDRH3は、YX1X2X3YX4VGGX5DYのアミノ酸配列(配列番号144)を含み、式中
X1は、Y、F、またはSであり、
X2は、YまたはDであり、
X3は、KまたはRであり、
X4は、DまたはEであり、及び
X5は、FまたはCであり、
(d)CDRL1は、SVSSX1ISSSX2LX3のアミノ酸配列(配列番号147)を含み、式中
X1は、SまたはGであり、
X2は、NまたはTであり、及び
X3は、HまたはYであり、
(e)CDRL2は、GTSNLASのアミノ酸配列(配列番号104)を含み、及び
(f)CDRL3は、QQWX1X2YPX3Tのアミノ酸配列(配列番号149)を含み、式中
X1は、S、N、またはRであり、
X2は、S、T、またはRであり、及び
X3は、F、L、H、またはWである、単離抗体を提供する。
(a)CDRH1は、DTYIHのアミノ酸配列(配列番号79)を含み、
(b)CDRH2は、EIDPANDNTKYDPKFQGのアミノ酸配列(配列番号90)を含み、
(c)CDRH3は、YYYX1YX2VGGFDYのアミノ酸配列(配列番号146)を含み、式中:X1は、KまたはRであり、及びX2は、DまたはEであり、
(d)CDRL1は、SVSSSISSSNLHのアミノ酸配列(配列番号100)を含み、
(e)CDRL2は、GTSNLASのアミノ酸配列(配列番号104)を含み、及び
(f)CDRL3は、QQWSSYPFTのアミノ酸配列(配列番号105)を含む、単離抗体を提供する。
医薬的に許容可能な担体、賦形剤、または安定剤中で所望の純度を有する本明細書に記載の抗LAG-3(例えば、ヒトLAG-3)抗体を含む組成物(例えば、医薬組成物)が本明細書で提供される(Remington’s Pharmaceutical Sciences(1990)Mack Publishing Co.,Easton,PA)。許容可能な担体、賦形剤、または安定剤は、用いられる投与量及び濃度において受容者に対して非毒性であり、リン酸塩、クエン酸塩、及び他の有機酸などの緩衝液、アスコルビン酸及びメチオニンを含む酸化防止剤、保存剤(オクタデシルジメチルベンジル塩化アンモニウム、塩化ヘキサメトニウム、塩化ベンザルコニウム、塩化ベンゼトニウム、フェノール、ブチル、もしくはベンジルアルコール、メチルもしくはプロピルパラベンなどのアルキルパラベン、カテコール、レゾルシノール、シクロヘキサノール、3-ペンタノール、及びm-クレゾールなど)、低分子量(約10個未満の残基)ポリペプチド、血清アルブミン、ゼラチン、もしくは免疫グロブリンなどのタンパク質、ポリビニルピロリドンなどの親水性ポリマー、グリシン、グルタミン、アスパラギン、ヒスチジン、アルギニン、もしくはリシンなどのアミノ酸、モノサッカライド、ジサッカライド、及びグルコース、マンノース、もしくはデキストリンを含む他の炭水化物、EDTAなどのキレート剤、スクロース、マンニトール、トレハロース、もしくはソルビトールなどの糖類、ナトリウムなどの塩形成対イオン、金属複合体(例えば、Zn-タンパク質複合体)、及び/またはTWEEN(登録商標)、PLURONICS(登録商標)、もしくはポリエチレングリコール(PEG)などの非イオン界面活性剤などの緩衝液が挙げられる。
別の態様では、本開示は、本明細書に開示される抗LAG-3(例えば、ヒトLAG-3)抗体を用いた対象の治療方法を提供する。LAG-3(例えば、ヒトLAG-3)機能の阻害から恩恵を受ける対象中の任意の疾患または障害は、本明細書に開示される抗LAG-3(例えば、ヒトLAG-3)抗体を用いて治療することができる。本明細書に開示される抗LAG-3(例えば、ヒトLAG-3)抗体は、腫瘍に対する免疫寛容を阻害するために特に有用であるため、がんを有する対象の免疫療法として使用することができる。例えば、ある特定の実施形態では、本開示は、対象中の抗原に応答してT細胞活性化を増加させる方法であって、本明細書に開示されるように、有効量の抗LAG-3(例えば、ヒトLAG-3)抗体またはその医薬組成物を対象に投与することを含む、方法を提供する。ある特定の実施形態では、本開示は、対象におけるがんの治療方法であって、本明細書に開示されるように、有効量の抗体または医薬組成物を対象に投与することを含む、方法を提供する。
別の態様では、LAG-3(例えば、ヒトLAG-3)抗原に特異的に結合する本明細書に記載の抗体またはその断片(例えば、軽鎖可変領域及び/または重鎖可変領域)をコードするヌクレオチド配列を含むポリヌクレオチド、及びベクター、例えば、宿主細胞(例えば、E.coli及び哺乳動物細胞)において組み換え発現のためのかかるポリヌクレオチドを含むベクターが本明細書で提供される。本明細書で提供される抗体の任意の重鎖及び/または軽鎖をコードするヌクレオチド配列を含むポリヌクレオチド、及びかかるポリヌクレオチド配列を含むベクター、例えば、宿主細胞、例えば、哺乳動物細胞においてそれらの効率的な発現のための発現ベクターが本明細書で提供される。
1つ以上の本明細書に記載の抗体または医薬組成物またはその共役体を含むキットも本明細書で提供される。特定の実施形態では、本明細書で提供される1つ以上の抗体などの本明細書に記載の医薬組成物の成分のうちの1つ以上で充填された1つ以上の容器を含む薬学的パックまたはキットが本明細書で提供される。いくつかの実施形態では、キットは、本明細書に記載の医薬組成物、及び本明細書に記載のものなどの任意の予防または治療剤を含有する。ある特定の実施形態では、キットは、例えば、フィトヘムアグルチニン(PHA)及び/またはホルボールミリステートアセテート(PMA)、または抗CD3抗体及び抗CD28抗体などのTCR複合体刺激抗体などのT細胞マイトジェンを含有し得る。必要に応じて、かかる容器(複数可)と関連して、調合薬または生物学的製剤の製造、使用、または販売を規制する行政機関によって規定された様式の注意書きを含むことができ、この注意書きは、ヒトへの投与のための製造、使用、または販売の機関による承認を反映する。
この項(すなわち、項6)における実施例は、例証として提供されており、限定するものではない。
この実施例は、CD223としても知られるヒトリンパ球活性化遺伝子3(LAG-3)に結合する抗体の生成及び特徴付けを説明する。特に、この実施例は、ヒトLAG-3に特異的に結合し、ヒトLAG-3の機能を阻害するマウス抗体の生成を説明する。
抗LAG-3抗体は、免疫したFabファージディスプレイライブラリーの生成及び選択によって特定した。まず、組み換えヒトLAG-3-Fcタンパク質(R&D Systems、Cat#2319-L3-050)及び組み換えカニクイザルLAG-3-Fcタンパク質(Evitria、特注)で予め免疫した3匹の個々のマウス由来の脾細胞の単一細胞懸濁液から全RNAを精製した。その後、マウスごとに、全RNAをテンプレートとして用いたランダムプライムcDNAによってFabライブラリーを生成し、マウス抗体遺伝子から可変領域を増幅した。重鎖及びカッパ鎖アンプリコンを組み合わせて、ファージミドベクターにクローニングした。3ラウンドの選択を、組み換えLAG-3タンパク質(ヒトLAG-3-Fc、ヒトLAG-3-6His、及び/または30アミノ酸ヒトLAG-3ペプチド)及び/またはカニクイザルLAG-3を発現する細胞に対して実施し、LAG-3特異的Fabファージクローンを特定した。30アミノ酸ヒトLAG-3ペプチドは、GPPAAAPGHPLAPGPHPAAPSSWGPRPRRYのアミノ酸配列(配列番号199)を含むビオチン化ペプチドである。その後、選択したFabクローンのペリプラズム抽出物をELISAまたはフローサイトメトリーによってスクリーニングした。次いで、抗体シーケンシング及びオフ率分析を抗LAG-3 Fabで実施した。
ペリプラズム抽出物からの抗LAG-3 Fabを、フローサイトメトリーを用いて、LAG-3発現細胞への結合について試験した。簡単に言えば、野生型ジャーカット細胞及びヒトLAG-3を発現するジャーカット細胞を、96ウェルU底プレート(Sarstedt)中の試料緩衝液(PBS(Gibco、Cat#10010-015)+0.5%FBS(Gibco、Cat#10270-106))において2×105細胞/ウェルで播種した。22μlの抗LAG-3 Fabペリプラズム抽出物、及び83μlの希釈抗c-myc抗体(Gentaur、クローン#9E10、Cat#04-cmyc-9E10)を室温で30分間インキュベートした。100μlのペリプラズム抽出物/抗c-myc混合物を細胞に添加した後、氷上で1時間インキュベートした。細胞を3回洗浄した後、ヤギ抗マウスAPC(BD Biosciences、Cat#550826)と氷上にて30分間インキュベートした。細胞を3回洗浄した後、FACSマシン(BD Accuri6)で分析した。
抗LAG-3 Fabを、組み換えヒトLAG-3のMHCクラスII発現細胞への結合を遮断する能力について試験した。LAG-3-6His(Acro Biosystems、Cat#LA3-H5222)を、抗Hisビオチン(Genscript、クローン#A00186、Cat#A00613)を6μg/mlで、10μg/mlで4℃にて10分間プレインキュベートした。次いで、この混合物を、抗LAG-3 FabまたはLAG-3に特異的ではない陰性対照Fabの10000ng/ml(図2A)または連続希釈(21170、7056.6、2352.2、784.0、261.3、87.1、29.0、または9.7ng/ml)(図2B)のいずれかと4℃で60分間インキュベートした後、50,000Raji細胞でさらに60分間4℃にてインキュベートした。培養を試料緩衝液(PBS+2%FBS+0.09%アジ化ナトリウム)で2回洗浄した後、試料緩衝液中のストレプトアビジン-PE(Biolegend、Cat#405204)と4℃で30分間インキュベートした。細胞を2回洗浄した後、FACS Fortessaサイトメーター(Becton Dickinson)で分析した。
キメラ抗LAG-3抗体P13B02の機能活性は、StaphylococcusエンテロトキシンA(SEA)で刺激された初代ヒト末梢血単核細胞(PBMC)を用いて試験した。簡単に言えば、凍結保存したヒトPBMC(Research Blood Components)を、96ウェルNUNCLONデルタ定盤(NUNC(商標))における、Normocin(商標)(Invivogen、Cat#ant-nr-1)及び10%熱不活性化FBS(Thermo Fisher Scientific、Cat#26140079)を補充したRPMI1640中で105細胞/ウェルで播種した。細胞を、100ng/mlのSEA(Toxin Technologies、Cat#at101red)及び10μg/mlのP13B02またはアイソタイプ対照抗体で、37℃、5%CO2、及び97%湿度で5日間培養した。澄明化された上清を収集し、分析するまで-80℃で保存した。IL-2レベルは、AlphaLISA(Perkin Elmer、Cat#AL221C)を用いて決定した。
この実施例は、マウス抗体P13B02のヒト化、及びヒト化抗体の特徴付けを説明する。
相同性マッチングを使用して、マウス抗体P13B02のCDRをグラフトするためのヒト受容体フレームワーク領域を選択した。データベース、例えば、ヒト及びマウスの免疫グロブリン遺伝子座由来の生殖系列可変遺伝子のデータベース(IMGTデータベース(the international ImMunoGeneTics information system(登録商標)、Lefranc MP et al.,(1999)Nucleic Acids Res 27(1):209-12、Ruiz M et al.,(2000)Nucleic Acids Res 28(1):219-21、Lefranc MP(2001)Nucleic Acids Res 29(1):207-9、Lefranc MP(2003)Nucleic Acids Res 31(1):307-10、Lefranc MP et al.,(2005)Dev Compo Immunol 29(3):185-203、Kaas Q et al.,(2007)Briefings in Functional Genomics & Proteomics 6(4):253-64)またはVBASE2(Retter I et al.,(2005)Nucleic Acids Res 33,Database issue D671-D674)またはKabatデータベース(Johnson G et al.,(2000)Nucleic Acids Res 28:214-218))または出版物(例えば、Kabat EA et al.,(1991)Sequences of Proteins of Immunological Interest、Fifth Edition、U.S.Department of Health and Human Services、NIH公開番号第91-3242号)(これらは全て、それら全体が参照により本明細書に組み込まれる)は、マウス重鎖及び軽鎖可変領域が属するヒトサブファミリーを特定し、受容体分子として用いるのに最良適合のヒト生殖系列フレームワークを決定するために使用され得る。受容体として使用されるべきこれらのサブファミリー内の重鎖及び軽鎖可変領域配列の選択は、グラフト後の6つのCDRの適切な相対提示の保存に役立つように、配列相同性及び/またはCDR1及びCDR2領域の構造の一致に基づき得る。
抗LAG-3抗体を、フローサイトメトリーを用いて、初代ヒトT細胞への結合について試験した。凍結保存したヒトPBMC(Research Blood Components)を、100ng/mlのSEA(Toxin Technologies、Cat#at101red)の存在下で、T-75フラスコ(Corning)中にNormocinTM(Invivogen、Cat#ant-nr-1)及び10%熱不活性化FBS(Thermo Fisher Scientific、Cat#26140079)を補充したRPMI1640において106細胞/mlで、37℃、5%CO2、及び97%湿度で5日間播種した。その後、培養したPBMCを、96ウェルU底プレート(Nunc)中で105細胞/ウェルで播種した。細胞を10μg/mlの抗LAG-3抗体で氷上にて30分間インキュベートした。細胞を3回洗浄した後、抗CD4-PE/Cy7(Biolegend、クローン#OKT4、Cat#317414)、抗CD8-FITC(Biolegend、クローン#RPA-T8、Cat#301060)、抗CD3-APC(BD Biosciences、クローン#SP34-2、Cat#557597)、LIVE/DEAD(登録商標)Fixable Near-IR死細胞染色(Life Technologies、Cat#L10119)、Fcブロック(BD Biosciences、Cat#422302)、及びヤギ抗ヒトIgG-PE(ThermoFisher、Cat#PA1-74408)でインキュベートした。細胞を氷上で30分間インキュベートし、洗浄し、FACSマシン(BD Canto)で分析した。図6Aに示すように、キメラ抗体P13B02、及び試験した全てのヒト化抗体は、SEAスーパー抗原で刺激された初代CD4+ヒトT細胞への結合を示した。
次に、ヒト化抗LAG-3抗体が架橋組み換えLAG-3-6HisとMHCクラスIIを発現するRaji細胞との間の相互作用を遮断する能力を上記のように調べた。ヒト化抗体P13B02-06、P13B02-07、P13B02-16、P13B02-26、及びP13B02-27(それらは全て、ヒトIgG1定常領域を含む)を、57820、28910、14455、7228、3613、1807、903、452、226、113、及び56ng/mlで試験した(図7A)。ヒト化抗体P13B02-30(IgG1 G1m17 N297A)を、96360、48180、24090、12045、6022、3011、1505、753、376、188、及び94ng/mlで試験した(図7B)。
ヒト化抗体P13B02-30(IgG1)の機能活性は、StaphylococcusエンテロトキシンA(SEA)で刺激された初代ヒトPBMCを用いて評価した。凍結保存したヒトPBMC(Research Blood Components)を、96ウェルNUNCLONデルタ定盤(NUNC(商標))における、Normocin(商標)(Invivogen、Cat#ant-nr-1)及び10%熱不活性化FBS(Thermo Fisher Scientific、Cat#26140079)を補充したRPMI1640中で105細胞/ウェルで播種した。細胞を、100ng/mlのSEA(Toxin Technologies、Cat#at101red)及び10μg/mlのP13B02-30(IgG1)またはアイソタイプ対照抗体で、37℃、5%CO2、及び97%湿度で5日間培養した。澄明化された上清を収集し、分析するまで-80℃で保存した。IL-2レベルは、AlphaLISA(Perkin Elmer、Cat#AL221C)を用いて決定した。
抗LAG-3抗体P13B02-30(IgG1 G1m3 N297A)は、活性化初代腫瘍浸潤リンパ球(TIL)のサイトカイン産生を、単体でまたは抗PD-1抗体と組み合わせて刺激するその能力についてさらに評価した。新鮮な腎細胞癌(RCC)(ステージI)または大腸癌(CRC)(ステージII)腫瘍(UMass Medical School,Worcester,MA)由来の単一細胞懸濁液を機械的な顕微解剖を介して単離した。場合によっては、線維症のレベルに応じて、酵素消化が必要であった(リベラーゼ及びDNAseI、Roche)。細胞を、96ウェルNUNCLONデルタ定盤(NUNC(商標)、Cat#143761)における、Normocin(商標)(Invivogen、Cat#ant-nr-1)、組み換えヒトIL-2(20U/ml、R&D Systems、Cat#202-IL-010)、及び10%熱不活性化FBS(Thermo Fisher Scientific、Cat#26140079)を補充したRPMI1640中で5×104細胞/ウェルで1日間休止した。翌日、試料を遠心分離し、対象となる抗体:P13B02-30(IgG1 G1m3 N297A)を20μg/mlで、及び抗PD-1抗体ペムブロリズマブ(ペムブロ)(Myoderm)を5μg/mlで、及び抗CD3/CD28マイクロビーズ(1:1ビーズ:細胞比)を含む新鮮な培養培地を100μlの最終容量で添加し、37℃、及び5%CO2で3日間インキュベートした。無細胞上清を収集し、分析するまで-80℃で保存した。TNFαレベルは、AlphaLISA(Perkin Elmer、Cat#AL208C)を用いて決定した。
この実施例では、NFAT-ルシフェラーゼレポーター株を使用して、細胞抑制アッセイにおけるLAG-3に対する抗LAG-3抗体P13B02-30(IgG1 G1m3 N297A)の阻害効果を評価した。2つの実験を以下に記載するように実施した。
この実施例では、抗LAG-3抗体P13B02-30のエピトープは、上述のように特徴付けた。
抗LAG-3 F(ab’)2は、FragITキット(Genovis、Cat#A2-FR2-100)を用いてP13B02-30(IgG4 S228P)から生成された。抗LAG-3 F(ab’)2のヒトLAG-3との相互作用は、水素-重水素交換(HDX)質量分析法を用いて研究した。
Claims (147)
- ヒトLAG-3に特異的に結合する単離抗体であって、相補性決定領域CDRH1、CDRH2、及びCDRH3を含む重鎖可変領域、及び相補性決定領域CDRL1、CDRL2、及びCDRL3を含む軽鎖可変領域を含み、
(a)CDRH1は、DX1YX2X3のアミノ酸配列(配列番号140)を含み、式中
X1は、TまたはNであり、
X2は、IまたはMであり、及び
X3は、H、Y、またはDであり、
(b)CDRH2は、X1IDPANX2X3X4X5X6X7PX8X9QX10のアミノ酸配列(配列番号142)を含み、式中
X1は、E、R、S、またはKであり、
X2は、DまたはGであり、
X3は、NまたはHであり、
X4は、TまたはSであり、
X5は、KまたはHであり、
X6は、YまたはFであり、
X7は、DまたはAであり、
X8は、KまたはRであり、
X9は、FまたはLであり、及び
X10は、GまたはDであり、
(c)CDRH3は、YX1X2X3YX4VGGX5DYのアミノ酸配列(配列番号144)を含み、式中
X1は、Y、F、またはSであり、
X2は、YまたはDであり、
X3は、KまたはRであり、
X4は、DまたはEであり、及び
X5は、FまたはCであり、
(d)CDRL1は、SVSSX1ISSSX2LX3のアミノ酸配列(配列番号147)を含み、式中
X1は、SまたはGであり、
X2は、NまたはTであり、及び
X3は、HまたはYであり、
(e)CDRL2は、GTSNLASのアミノ酸配列(配列番号104)を含み、及び
(f)CDRL3は、QQWX1X2YPX3Tのアミノ酸配列(配列番号149)を含み、式中
X1は、S、N、またはRであり、
X2は、S、T、またはRであり、及び
X3は、F、L、H、またはWである、前記単離抗体。 - CDRH1が、DX1YX2X3のアミノ酸配列(配列番号141)を含み、式中:X1が、TまたはNであり、X2が、IまたはMであり、及びX3が、HまたはYである、請求項1に記載の単離抗体。
- CDRH2が、X1IDPANX2X3X4KX5X6PX7FQX8のアミノ酸配列(配列番号143)を含み、式中:X1が、E、R、またはSであり、X2が、DまたはGであり、X3が、NまたはHであり、X4が、TまたはSであり、X5が、YまたはFであり、X6が、DまたはAであり、X7が、KまたはRであり、及びX8が、GまたはDである、請求項1に記載の単離抗体。
- CDRH3が、YX1X2X3YDVGGX4DYのアミノ酸配列(配列番号145)を含み、式中:X1が、Y、F、またはSであり、X2が、YまたはDであり、X3が、KまたはRであり、及びX4が、FまたはCである、請求項1に記載の単離抗体。
- CDRH3が、YYYX1YX2VGGFDYのアミノ酸配列(配列番号146)を含み、式中:X1が、KまたはRであり、及びX2が、DまたはEである、請求項1に記載の単離抗体。
- CDRL1が、SVSSSISSSNLX1のアミノ酸配列(配列番号148)を含み、式中:X1が、HまたはYである、請求項1に記載の単離抗体。
- CDRL3が、QQWX1SYPX2T(配列番号150)のアミノ酸配列を含み、式中:X1が、S、N、またはRであり、及びX2が、F、L、またはHである、請求項1に記載の単離抗体。
- (a)CDRH1が、DTYIHのアミノ酸配列(配列番号79)を含み、
(b)CDRH2が、EIDPANDNTKYDPKFQGのアミノ酸配列(配列番号90)を含み、
(c)CDRH3が、YYYX1YX2VGGFDYのアミノ酸配列(配列番号146)を含み、式中:X1が、KまたはRであり、及びX2が、DまたはEであり、
(d)CDRL1が、SVSSSISSSNLHのアミノ酸配列(配列番号100)を含み、
(e)CDRL2が、GTSNLASのアミノ酸配列(配列番号104)を含み、及び
(f)CDRL3が、QQWSSYPFTのアミノ酸配列(配列番号105)を含む、請求項1に記載の単離抗体。 - CDRH1が、配列番号78~82からなる群から選択されるアミノ酸配列を含む、請求項1~8のいずれか1項に記載の単離抗体。
- CDRH2が、配列番号83~93からなる群から選択されるアミノ酸配列を含む、請求項1~9のいずれか1項に記載の単離抗体。
- CDRH3が、配列番号94~99からなる群から選択されるアミノ酸配列を含む、請求項1~10のいずれか1項に記載の単離抗体。
- CDRL1が、配列番号100~103からなる群から選択されるアミノ酸配列を含む、請求項1~11のいずれか1項に記載の単離抗体。
- CDRL3が、からなる群から選択されるアミノ酸配列を含む 配列番号105~112、請求項1~12のいずれか1項に記載の単離抗体。
- CDRH1、CDRH2、及びCDRH3が、配列番号78、83、及び94、78、85、及び95、78、86、及び96、78、86、及び97、78、91、及び94、78、92、及び96、79、84、及び95、79、88、及び95、79、89、及び95、79、90、及び95、79、90、及び98、79、90、及び99、80、85、及び96、81、87、及び96、または、82、93、及び95にそれぞれ記載のCDRH1、CDRH2、及びCDRH3アミノ酸配列を含む、請求項1~13のいずれか1項に記載の単離抗体。
- CDRL1、CDRL2、及びCDRL3が、配列番号100、104、及び105、100、104、及び106、100、104、及び107、100、104、及び109、100、104、及び110、101、104、及び108、102、104、及び105、102、104、及び112、または、103、104、及び111にそれぞれ記載のCDRL1、CDRL2、及びCDRL3アミノ酸配列を含む、請求項1~14のいずれか1項に記載の単離抗体。
- CDRH1、CDRH2、CDRH3、CDRL1、CDRL2、及びCDRL3が、配列番号78、83、94、100、104、及び105、78、85、95、100、104、及び105、78、86、96、100、104、及び105、78、86、96、100、104、及び109、78、86、96、100、104、及び110、78、86、96、101、104、及び108、78、86、96、103、104、及び111、78、86、97、102、104、及び112、78、91、94、100、104、及び107、78、92、96、100、104、及び105、78、92、96、100、104、及び109、79、84、95、100、104、及び105、79、84、95、100、104、及び106、79、84、95、102、104、及び105、79、88、95、100、104、及び105、79、89、95、100、104、及び105、79、90、95、100、104、及び105、79、90、98、100、104、及び105、79、90、99、100、104、及び105、80、85、96、100、104、及び105、81、87、96、100、104、及び105、81、87、96、100、104、及び107、または、82、93、95、100、104、及び105にそれぞれ記載のアミノ酸配列を含む、請求項1~15のいずれか1項に記載の単離抗体。
- ヒトLAG-3に特異的に結合する単離抗体であって、相補性決定領域CDRH1、CDRH2、及びCDRH3を含む重鎖可変領域、及び相補性決定領域CDRL1、CDRL2、及びCDRL3を含む軽鎖可変領域を含み、CDRH1、CDRH2、CDRH3、CDRL1、CDRL2、及びCDRL3は、配列番号79、90、95、100、104、及び105にそれぞれ記載のアミノ酸配列を含む、前記単離抗体。
- ヒトLAG-3に特異的に結合する単離抗体であって、相補性決定領域CDRH1、CDRH2、及びCDRH3を含む重鎖可変領域、及び相補性決定領域CDRL1、CDRL2、及びCDRL3を含む軽鎖可変領域を含み、CDRH1、CDRH2、CDRH3、CDRL1、CDRL2、及びCDRL3は、配列番号79、90、98、100、104、及び105にそれぞれ記載のアミノ酸配列を含む、前記単離抗体。
- 前記抗体が、配列番号151、222、218、または223の重鎖可変領域配列のフレームワーク領域を含む重鎖可変領域を含む、請求項1~18のいずれか1項に記載の単離抗体。
- 前記抗体が、配列番号151、222、218、または223のアミノ酸配列を含む重鎖可変領域を含む、請求項1~18のいずれか1項に記載の単離抗体。
- 前記抗体が、配列番号56~72、及び220からなる群から選択されるアミノ酸配列に少なくとも75%、80%、85%、90%、95%、または100%同一であるアミノ酸配列を含む重鎖可変領域を含む、請求項1~18のいずれか1項に記載の単離抗体。
- 前記重鎖可変領域が、配列番号56~72、及び220からなる群から選択されるアミノ酸配列を含む、請求項21に記載の単離抗体。
- 前記重鎖可変領域が、配列番号65または220のアミノ酸配列を含む、請求項22に記載の単離抗体。
- 前記抗体が、配列番号168~186、及び225~227からなる群から選択されるアミノ酸配列を含む重鎖を含む、請求項22に記載の単離抗体。
- 前記抗体が、ヒト由来フレームワーク領域を有する重鎖可変領域を含む、請求項1~18のいずれか1項に記載の単離抗体。
- 前記抗体が、ヒト遺伝子によってコードされるアミノ酸配列であるかまたは由来である重鎖可変フレームワーク領域を含み、前記アミノ酸配列が、IGHV1-46*01(配列番号153)、IGHV1-69-2*01(配列番号154)、IGHV1-3*01(配列番号155)、IGHV1-24*01(配列番号156)、IGHV1-2*01(配列番号157)、IGHV1-45*01(配列番号158)、及びIGHV1-18*01(配列番号159)からなる群から選択される、請求項1~18のいずれか1項に記載の単離抗体。
- 前記抗体が、前記アミノ酸配列IGHV1-46*01(配列番号153)由来である重鎖可変フレームワーク領域を含み、前記アミノ酸配列IGHV1-46*01(配列番号153)中の少なくとも1つのアミノ酸が、対応する非ヒト重鎖可変フレームワーク領域中の類似位置におけるアミノ酸で置換される、請求項26に記載の単離抗体。
- 前記アミノ酸置換が、4、5、12、23、27、28、29、30、48、69、71、75、76、80、81、及び94からなる群から選択されるアミノ酸位置であり、前記アミノ酸位置が、Kabatの番号付けシステムにしたがって示される、請求項27に記載の単離抗体。
- 前記アミノ酸置換が、4M、5K、12V、23T、27F、28N、29I、30K、48I、69I、71A、75S、76N、80L、81Q、及び94Tからなる群から選択され、前記アミノ酸置換の位置が、Kabatの番号付けシステムにしたがって示される、請求項28に記載の単離抗体。
- 前記アミノ酸置換が、4、27、28、29、30、69、71、及び94からなる群から選択されるアミノ酸位置であり、前記アミノ酸位置が、Kabatの番号付けシステムにしたがって示される、請求項28または29に記載の単離抗体。
- 前記抗体が、配列番号152または224の軽鎖可変領域配列のフレームワーク領域を含む軽鎖可変領域を含む、請求項1~30のいずれか1項に記載の単離抗体。
- 前記抗体が、配列番号152または224のアミノ酸配列を含む軽鎖可変領域を含む、請求項1~30のいずれか1項に記載の単離抗体。
- 前記抗体が、配列番号73~77、及び221からなる群から選択されるアミノ酸配列に少なくとも75%、80%、85%、90%、95%、または100%同一であるアミノ酸配列を含む軽鎖可変領域を含む、請求項1~30のいずれか1項に記載の単離抗体。
- 前記軽鎖可変領域が、配列番号73~77、及び221からなる群から選択されるアミノ酸配列を含む、請求項33に記載の単離抗体。
- 前記軽鎖可変領域が、配列番号73または221のアミノ酸配列を含む、請求項34に記載の単離抗体。
- 前記抗体が、配列番号187~191、及び228からなる群から選択されるアミノ酸配列を含む軽鎖を含む、請求項34に記載の単離抗体。
- 前記抗体が、ヒト由来フレームワーク領域を有する軽鎖可変領域を含む、請求項1~30のいずれか1項に記載の単離抗体。
- 前記抗体が、ヒト遺伝子によってコードされるアミノ酸配列であるかまたは由来である軽鎖可変フレームワーク領域を含み、前記アミノ酸配列が、IGKV3-20*01(配列番号160)、IGKV3D-15*01(配列番号161)、IGKV3-15*01(配列番号161)、IGKV3D-20*01(配列番号162)、IGKV3D-7*01(配列番号163)、IGKV1-9*01(配列番号164)、及びIGKV3-11*01(配列番号165)からなる群から選択される、請求項1~30のいずれか1項に記載の単離抗体。
- 前記抗体が、前記アミノ酸配列IGKV3-20*01(配列番号160)由来である軽鎖可変フレームワーク領域を含む、請求項38に記載の単離抗体。
- 前記抗体が、前記アミノ酸配列IGKV3-20*01(配列番号160)由来である軽鎖可変フレームワーク領域を含み、前記アミノ酸配列IGKV3-20*01(配列番号160)中の少なくとも1つのアミノ酸が、対応する非ヒト軽鎖可変フレームワーク領域中の類似位置におけるアミノ酸で置換される、請求項38に記載の単離抗体。
- 前記アミノ酸置換が、3、22、36、43、47、58、70、及び71からなる群から選択されるアミノ酸位置であり、前記アミノ酸位置が、Kabatの番号付けシステムにしたがって示される、請求項40に記載の単離抗体。
- 前記アミノ酸置換が、3L、22T、36F、43S、47W、58V、70S、及び71Yからなる群から選択され、前記アミノ酸置換の位置が、Kabatの番号付けシステムにしたがって示される、請求項41に記載の単離抗体。
- 配列番号56~72、及び220からなる群から選択されるアミノ酸配列を含む重鎖可変領域を含む、ヒトLAG-3に特異的に結合する単離抗体。
- 前記重鎖可変領域が、配列番号65または220のアミノ酸配列を含む、請求項43に記載の単離抗体。
- 前記抗体が、配列番号168~186、及び225~227からなる群から選択されるアミノ酸配列を含む重鎖を含む、請求項43に記載の単離抗体。
- 前記抗体が、配列番号168、225、169、226、170、または227のアミノ酸配列を含む重鎖を含む、請求項45に記載の単離抗体。
- 配列番号73~77、及び221からなる群から選択されるアミノ酸配列を含む軽鎖可変領域を含む、ヒトLAG-3に特異的に結合する単離抗体。
- 前記軽鎖可変領域が、配列番号73または221のアミノ酸配列を含む、請求項47に記載の単離抗体。
- 前記抗体が、配列番号187~191、及び228からなる群から選択されるアミノ酸配列を含む軽鎖を含む、請求項47に記載の単離抗体。
- 前記抗体が、配列番号187または228のアミノ酸配列を含む軽鎖を含む、請求項49に記載の単離抗体。
- 重鎖可変領域及び軽鎖可変領域を含み、前記重鎖可変領域及び前記軽鎖可変領域は、配列番号56及び73、56及び74、56及び75、56及び76、56及び77、57及び73、57及び74、57及び75、57及び76、57及び77、58及び73、58及び74、58及び75、58及び76、58及び77、59及び73、59及び74、59及び75、59及び76、59及び77、60及び73、60及び74、60及び75、60及び76、60及び77、61及び77、62及び77、63及び73、64及び73、65及び73、220及び73、65及び221、220及び221、66及び73、67及び73、68及び73、69及び73、70及び73、71及び73、または72及び73にそれぞれ記載のアミノ酸配列を含む、ヒトLAG-3に特異的に結合する単離抗体。
- 前記重鎖可変領域及び前記軽鎖可変領域が、配列番号65及び73、220及び73、65及び221、または220及び221にそれぞれ記載のアミノ酸配列を含む、請求項51に記載の単離抗体。
- 配列番号168または225のアミノ酸配列を含む重鎖、及び配列番号187または228のアミノ酸配列を含む軽鎖を含む、ヒトLAG-3に特異的に結合する単離抗体。
- 配列番号169または226のアミノ酸配列を含む重鎖、及び配列番号187または228のアミノ酸配列を含む軽鎖を含む、ヒトLAG-3に特異的に結合する単離抗体。
- 配列番号170または227のアミノ酸配列を含む重鎖、及び配列番号187または228のアミノ酸配列を含む軽鎖を含む、ヒトLAG-3に特異的に結合する単離抗体。
- 前記抗体が、ヒトIgG1、IgG2、IgG3、IgG4、IgA1、及びIgA2からなる群から選択される重鎖定常領域を含む、請求項1~23、25~44、及び47~52のいずれか1項に記載の単離抗体。
- 前記重鎖定常領域が、IgG1である、請求項1~23、25~44、及び47~52のいずれか1項に記載の単離抗体。
- IgG1のアミノ酸配列が、前記EU番号付けシステムにしたがって番号付けされたN297A突然変異を含む、請求項57に記載の単離抗体。
- 前記抗体が、配列番号194のアミノ酸配列を含む重鎖定常領域を含む、請求項58に記載の単離抗体。
- IgG1のアミノ酸配列が、前記EU番号付けシステムにしたがって番号付けされたN297Q突然変異を含む、請求項57に記載の単離抗体。
- 前記IgG1が、非フコシル化IgG1である、請求項57に記載の単離抗体。
- 前記重鎖定常領域が、IgG4である、請求項1~23、25~44、及び47~52のいずれか1項に記載の単離抗体。
- IgG4のアミノ酸配列が、前記EU番号付けシステムにしたがって番号付けされたS228P突然変異を含む、請求項62に記載の単離抗体。
- 前記抗体が、配列番号196のアミノ酸配列を含む重鎖定常領域を含む、請求項63に記載の単離抗体。
- 前記抗体が、ヒトIgGκ及びIgGλからなる群から選択される軽鎖定常領域を含む、請求項1~35、37~48、51~52、及び56~64のいずれか1項に記載の単離抗体。
- 前記軽鎖定常領域が、IgGκである、請求項1~35、37~48、51~52、及び56~64のいずれか1項に記載の単離抗体。
- 前記抗体が、配列番号198または219のアミノ酸配列を含む軽鎖定常領域を含む、請求項66に記載の単離抗体。
- ヒトLAG-3に結合するために、先行請求項のいずれか1項に記載の抗体と交差競合する、単離抗体。
- 先行請求項のいずれか1項に記載の抗体と同じヒトLAG-3のエピトープに結合する、単離抗体。
- 前記抗体が、配列番号216のアミノ酸配列からなるヒトLAG-3の領域内に位置するエピトープに結合する、先行請求項のいずれか1項に記載の単離抗体。
- 前記抗体が、配列番号215のアミノ酸配列からなるヒトLAG-3の領域内に位置するエピトープに結合する、先行請求項のいずれか1項に記載の単離抗体。
- 前記抗体が、配列番号214のアミノ酸配列からなるヒトLAG-3の領域内に位置するエピトープに結合する、先行請求項のいずれか1項に記載の単離抗体。
- 前記抗体が、配列番号213のアミノ酸配列からなるヒトLAG-3の領域内に位置するエピトープに結合する、先行請求項のいずれか1項に記載の単離抗体。
- 前記抗体が、配列番号212のアミノ酸配列からなるヒトLAG-3の領域内に位置するエピトープに結合する、先行請求項のいずれか1項に記載の単離抗体。
- 前記抗体が、配列番号211のアミノ酸配列からなるヒトLAG-3の領域内に位置するエピトープに結合する、先行請求項のいずれか1項に記載の単離抗体。
- 前記抗体が、ヒト化抗体、マウス抗体、またはキメラ抗体である、先行請求項のいずれか1項に記載の単離抗体。
- 前記抗体が、ヒトLAG-3に拮抗的である、先行請求項のいずれか1項に記載の単離抗体。
- 前記抗体が、ヒトLAG-3の活性を不活性化、低下、または阻害する、請求項77に記載の単離抗体。
- 前記抗体が、MHCクラスIIへのヒトLAG-3の結合を阻害する、請求項77に記載の単離抗体。
- 前記抗体が、ブドウ球菌エンテロトキシンA(SEA)で刺激された末梢血単核細胞(PBMC)によってIL-2産生を誘導する、請求項77に記載の単離抗体。
- 前記抗体が、抗CD3及び抗CD28抗体で刺激された腫瘍浸潤リンパ球(TIL)によってTNFα産生を誘導する、請求項77に記載の単離抗体。
- 細胞毒性剤、細胞増殖抑制剤、毒素、放射性核種、または検出可能な標識と共役した、先行請求項のいずれか1項に記載の単離抗体。
- 先行請求項のいずれか1項に記載の抗体、及び医薬的に許容可能な担体、または賦形剤を含む、医薬組成物。
- 請求項1~82のいずれか1項に記載の抗体の重鎖及び/または軽鎖をコードする、単離ポリヌクレオチド。
- 請求項84に記載のポリヌクレオチドを含む、ベクター。
- 請求項84に記載のポリヌクレオチド、または請求項85に記載のベクターを含む、組み換え宿主細胞。
- ヒトLAG-3に結合する抗体の産生方法であって、
前記ポリヌクレオチドが発現され、前記抗体が産生されるように、請求項86に記載の宿主細胞を培養することを含む、前記方法。 - 対象中の抗原に応答したT細胞活性化の増加方法であって、
有効量の請求項1~83のいずれか1項に記載の抗体または医薬組成物を前記対象に投与することを含む、前記方法。 - 有効量の請求項1~83のいずれか1項に記載の抗体または医薬組成物を前記対象に投与することを含む、対象におけるがんの治療方法。
- 前記抗体または医薬組成物を皮下または静脈内に投与する、請求項88または89に記載の方法。
- 前記抗体または医薬組成物を腫瘍内に投与する、請求項88または89に記載の方法。
- 追加の治療剤を前記対象に投与することをさらに含む、請求項88~91のいずれか1項に記載の方法。
- 前記追加の治療剤が、化学療法剤、放射線療法剤、またはチェックポイント標的剤である、請求項92に記載の方法。
- 前記チェックポイント標的剤が、アンタゴニスト抗PD-1抗体、アンタゴニスト抗PD-L1抗体、アンタゴニスト抗PD-L2抗体、アンタゴニスト抗CTLA-4抗体、アンタゴニスト抗TIM-3抗体、アンタゴニスト抗LAG-3抗体、アンタゴニスト抗CEACAM1抗体、アゴニスト抗GITR抗体、及びアゴニスト抗OX40抗体からなる群から選択される、請求項93に記載の方法。
- 前記追加の治療剤が、抗PD-1抗体であり、必要に応じて、前記抗PD-1抗体が、ペムブロリズマブまたはニボルマブである、請求項92に記載の方法。
- 前記追加の治療剤が、抗PD-L1抗体である、請求項92に記載の方法。
- 前記追加の治療剤が、抗CTLA-4抗体である、請求項92に記載の方法。
- 前記追加の治療剤が、インドールアミン-2,3-ジオキシゲナーゼ(IDO)の阻害剤である、請求項92に記載の方法。
- 前記阻害剤が、エパカドスタット、BMS-986205、インドキシモド、及びNLG919からなる群から選択される、請求項98に記載の方法。
- 前記阻害剤が、エパカドスタットである、請求項99に記載の方法。
- 前記追加の治療剤が、ワクチンである、請求項92に記載の方法。
- 前記ワクチンが、抗原性ペプチドと複合体化された熱ショックタンパク質を含む熱ショックタンパク質ペプチド複合体(HSPPC)を含む、請求項101に記載の方法。
- 前記熱ショックタンパク質が、hsc70であり、かつ、腫瘍関連抗原性ペプチドと複合体を形成する、請求項102に記載の方法。
- 前記熱ショックタンパク質が、gp96であり、かつ、腫瘍関連抗原性ペプチドと複合体を形成し、前記HSPPCが、対象から得られた腫瘍由来である、請求項102に記載の方法。
- CDRH1、CDRH2、及びCDRH3が、配列番号79、90、及び98にそれぞれ記載のアミノ酸配列を含む、請求項1に記載の単離抗体。
- 前記重鎖可変領域が、配列番号65または220のアミノ酸配列に少なくとも75%、80%、85%、90%、95%、97%、98%、または99%同一であるアミノ酸配列を含む、請求項1または105に記載の単離抗体。
- 前記重鎖可変領域が、配列番号65または220のアミノ酸配列に少なくとも98%同一であるアミノ酸配列を含む、請求項1または105に記載の単離抗体。
- 前記重鎖可変領域が、配列番号65または220のアミノ酸配列を含む、請求項1に記載の単離抗体。
- 前記抗体が、配列番号169または226のアミノ酸配列を含む重鎖を含む、請求項1に記載の単離抗体。
- CDRL1、CDRL2、及びCDRL3が、配列番号100、104、及び105にそれぞれ記載のアミノ酸配列を含む、請求項1に記載の単離抗体。
- 前記軽鎖可変領域が、配列番号73または221のアミノ酸配列に少なくとも75%、80%、85%、90%、95%、97%、98%、または99%同一であるアミノ酸配列を含む、請求項1または110に記載の単離抗体。
- 前記軽鎖可変領域が、配列番号73または221のアミノ酸配列に少なくとも98%同一であるアミノ酸配列を含む、請求項1または110に記載の単離抗体。
- 前記軽鎖可変領域が、配列番号73または221のアミノ酸配列を含む、請求項1に記載の単離抗体。
- 前記抗体が、配列番号187または228のアミノ酸配列を含む軽鎖を含む、請求項1に記載の単離抗体。
- 前記重鎖可変領域が、配列番号65または220のアミノ酸配列に少なくとも75%、80%、85%、90%、95%、97%、98%、または99%同一であるアミノ酸配列を含む、請求項18に記載の単離抗体。
- 前記重鎖可変領域が、配列番号65または220のアミノ酸配列に少なくとも98%同一であるアミノ酸配列を含む、請求項18に記載の単離抗体。
- 前記重鎖可変領域が、配列番号65または220のアミノ酸配列を含む、請求項18に記載の単離抗体。
- 前記抗体が、配列番号169または226のアミノ酸配列を含む重鎖を含む、請求項18に記載の単離抗体。
- 前記軽鎖可変領域が、配列番号73または221のアミノ酸配列に少なくとも75%、80%、85%、90%、95%、97%、98%、または99%同一であるアミノ酸配列を含む、請求項18に記載の単離抗体。
- 前記軽鎖可変領域が、配列番号73または221のアミノ酸配列に少なくとも98%同一であるアミノ酸配列を含む、請求項18に記載の単離抗体。
- 前記軽鎖可変領域が、配列番号73または221のアミノ酸配列を含む、請求項18に記載の単離抗体。
- 前記抗体が、配列番号187または228のアミノ酸配列を含む軽鎖を含む、請求項18に記載の単離抗体。
- 前記重鎖可変領域が、配列番号65または220のアミノ酸配列に少なくとも75%、80%、85%、90%、95%、97%、98%、または99%同一であるアミノ酸配列を含み、前記軽鎖可変領域が、配列番号73または221のアミノ酸配列に少なくとも75%、80%、85%、90%、95%、97%、98%、または99%同一であるアミノ酸配列を含む、請求項18に記載の単離抗体。
- 前記重鎖可変領域が、配列番号65または220のアミノ酸配列に少なくとも98%同一であるアミノ酸配列を含み、前記軽鎖可変領域が、配列番号73または221のアミノ酸配列に少なくとも98%同一であるアミノ酸配列を含む、請求項18に記載の単離抗体。
- 前記重鎖可変領域が、配列番号65または220のアミノ酸配列を含む、請求項123または124に記載の単離抗体。
- 前記軽鎖可変領域が、配列番号73または221のアミノ酸配列を含む、請求項123または124に記載の単離抗体。
- 前記重鎖可変領域が、配列番号65または220のアミノ酸配列を含み、前記軽鎖可変領域が、配列番号73または221のアミノ酸配列を含む、請求項18に記載の単離抗体。
- 前記重鎖可変領域が、配列番号220のアミノ酸配列を含み、前記軽鎖可変領域が、配列番号221のアミノ酸配列を含む、請求項127に記載の単離抗体。
- 前記抗体が、配列番号169または226のアミノ酸配列を含む重鎖を含む、請求項127に記載の単離抗体。
- 前記抗体が、配列番号187または228のアミノ酸配列を含む軽鎖を含む、請求項127に記載の単離抗体。
- 前記抗体が、配列番号169または226のアミノ酸配列を含む重鎖、及び配列番号187または228のアミノ酸配列を含む軽鎖を含む、請求項127に記載の単離抗体。
- 前記抗体が、配列番号226のアミノ酸配列を含む重鎖、及び配列番号228のアミノ酸配列を含む軽鎖を含む、請求項131に記載の単離抗体。
- 配列番号65または220のアミノ酸配列を含む重鎖可変領域を含む、ヒトLAG-3に特異的に結合する単離抗体。
- 前記抗体が、配列番号73または221のアミノ酸配列に少なくとも75%、80%、85%、90%、95%、97%、98%、または99%同一であるアミノ酸配列を含む軽鎖可変領域を含む、請求項133に記載の単離抗体。
- 前記抗体が、配列番号73または221のアミノ酸配列に少なくとも98%同一であるアミノ酸配列を含む軽鎖可変領域を含む、請求項133に記載の単離抗体。
- 配列番号73または221のアミノ酸配列を含む軽鎖可変領域を含む、ヒトLAG-3に特異的に結合する単離抗体。
- 前記抗体が、配列番号65または220のアミノ酸配列に少なくとも75%、80%、85%、90%、95%、97%、98%、または99%同一であるアミノ酸配列を含む重鎖可変領域を含む、請求項136に記載の単離抗体。
- 前記抗体が、配列番号65または220のアミノ酸配列に少なくとも98%同一であるアミノ酸配列を含む重鎖可変領域を含む、請求項136に記載の単離抗体。
- 前記重鎖可変領域のN末端アミノ酸残基が、ピログルタミン酸である、請求項1~18、31~42、47~50、56~82、105~107、110~116、119~124、126、及び136~138のいずれか1項に記載の単離抗体。
- 前記軽鎖可変領域のN末端アミノ酸残基が、ピログルタミン酸である、請求項1~30、43~46、56~82、105~112、115~120、123~125、及び133~135のいずれか1項に記載の単離抗体。
- 配列番号220中のXが、ピログルタミン酸である、請求項21~24、37~46、56~82、106~108、115~117、123~125、127~135、137、及び138のいずれか1項に記載の単離抗体。
- 配列番号221中のXが、ピログルタミン酸である、請求項33~36、47~50、52、56~82、111~113、119~121、123、124、126~132、及び134~138のいずれか1項に記載の単離抗体。
- (a)配列番号220中のXが、Qであり、配列番号221中のXが、Eまたはピログルタミン酸であり、または
(b)配列番号220中のXが、ピログルタミン酸であり、配列番号221中のXが、ピログルタミン酸である、請求項51、52、56~82、123~132、134、135、137、及び138のいずれか1項に記載の単離抗体。 - 前記配列番号226中のXが、ピログルタミン酸である、請求項24、31~42、45、46、54、62~82、109、118、129、131、及び132のいずれか1項に記載の単離抗体。
- 前記配列番号228中のXが、ピログルタミン酸である、請求項36、49、50、53~55、62~82、114、122、及び130~132のいずれか1項に記載の単離抗体。
- (a)配列番号226中のXが、Qであり、配列番号228中のXが、Eまたはピログルタミン酸であり、または
(b)配列番号226中のXが、ピログルタミン酸であり、配列番号228中のXが、ピログルタミン酸である、請求項54、68~82、131、及び132のいずれか1項に記載の単離抗体。 - 前記重鎖が、非グリコシル化される、請求項1~82、及び105~146のいずれか1項に記載の単離抗体。
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