JP2014514334A - Cd8+制御性t細胞を生成するための寛容原性合成ナノキャリア - Google Patents
Cd8+制御性t細胞を生成するための寛容原性合成ナノキャリア Download PDFInfo
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Abstract
Description
本出願は、米国特許法第119条の下で、2011年4月29日に出願された米国仮特許出願第61/480,946号、2011年7月29日に出願された同第61/513,514号、2011年9月6日に出願された同第61/531,147号、2011年9月6日に出願された同第61/531,153号、2011年9月6日に出願された同第61/531,164号、2011年9月6日に出願された同第61/531,168号、2011年9月6日に出願された同第61/531,175号、2011年9月6日に出願された同第61/531,180号、2011年9月6日に出願された同第61/531,194号、2011年9月6日に出願された同第61/531,204号、2011年9月6日に出願された同第61/531,209号、2011年9月6日に出願された同第61/531,215号の利益を主張するものであり、これらの仮特許出願のそれぞれの内容全体が、参照により本明細書に援用される。
免疫抑制剤および抗原のMHCクラスI拘束性および/またはMHCクラスII拘束性エピトープを含む合成ナノキャリア組成物が本明細書に提供される。このような組成物は、制御性細胞の生成、制御性表現型へのCD8+T細胞の変換などによる、エピトープの認識の結果として直接、並びに他の免疫細胞および免疫応答に対する更なる寛容原性効果をもたらすサイトカインの生成によって間接的に、寛容原性免疫効果を提供することができる。実施例に示されるように、本明細書に提供される合成ナノキャリアを用いて、CD8+制御性T細胞を生成するのに成功した。このような細胞の生成は、様々な疾病、疾患または病態の治療または予防に有用性を有し得る抗原特異的な寛容原性免疫応答を生成する本発明の組成物の能力を裏付けるものである。更に、本発明の組成物は、例えば、対象とする免疫細胞への標的化した送達を可能にすることによって、より標的化した免疫効果を可能にし得る。従って、本組成物および方法により、より標的を絞った(directed manner)免疫抑制を得ることができる。これは、オフターゲット(off−target)作用および/または毒性を軽減するのに役立ち得る。
「投与する(administering)」または「投与(administration)」は、薬理学的に有用な方法で被験体に材料を提供することを意味する。
CD8+制御性T細胞の生成をもたらす、免疫抑制剤およびMHCクラスI拘束性および/またはMHCクラスII拘束性エピトープを含む合成ナノキャリア組成物の投与を含む寛容原性方法、および関連する組成物が本明細書に提供される。提供される方法は、治療用タンパク質および/または移植可能な移植片の投与も含み得る。従って、提供される組成物は、治療用タンパク質および/または移植可能な移植片も含み得る。組成物は、寛容原性免疫応答(例えば、CD8+制御性T細胞の生成)が必要とされる被験体に投与され得る。このような被験体は、炎症性疾患、自己免疫疾患、アレルギー、臓器若しくは組織拒絶反応または移植片対宿主病に罹患しているかまたは罹患するリスクがある被験体を含む。このような被験体は、被験体が望ましくない免疫応答を起こしたかまたは起こすことが予測される治療用タンパク質を投与されたか、投与されているかまたは投与される予定である被験体も含む。このような被験体は、移植を行ったかまたは移植を行う予定である被験体も含む。
合成ナノキャリアは、当該技術分野において公知の様々な方法を用いて調製され得る。例えば、合成ナノキャリアは、ナノ析出(nanoprecipitation)、流体チャネルを用いたフローフォーカシング(flow focusing)、噴霧乾燥、単一および二重乳化溶媒蒸発、溶媒抽出、相分離、ミリング、マイクロエマルジョン法、マイクロ加工、ナノ加工(nanofabrication)、犠牲層、単純コアセルベーションおよび複合コアセルベーション、並びに当業者に周知の他の方法のような方法によって形成され得る。その代わりにまたはそれに加えて、単分散半導体ナノ材料、伝導性ナノ材料、磁性ナノ材料、有機ナノ材料、および他のナノ材料のための水性および有機溶媒合成が、記載されている(Pellegrino et al.,2005,Small,1:48;Murray et al.,2000,Ann.Rev.Mat.Sci.,30:545;およびTrindade et al.,2001,Chem.Mat.,13:3843)。更なる方法が、文献に記載されている(例えば、Doubrow,Ed.,“Microcapsules and Nanoparticles in Medicine and Pharmacy,” CRC Press,Boca Raton,1992;Mathiowitz et al.,1987,J.Control.Release,5:13;Mathiowitz et al.,1987,Reactive Polymers,6:275;およびMathiowitz et al.,1988,J.Appl.Polymer Sci.,35:755;米国特許第5578325号明細書および同第6007845号明細書;P.Paolicelli et al.,“Surface−modified PLGA−based Nanoparticles that can Efficiently Associate and Deliver Virus−like Particles” Nanomedicine.5(6):843−853(2010)を参照されたい)。
材料
オボアルブミンタンパク質のTおよびB細胞エピトープであることが知られている17アミノ酸のペプチドであるオボアルブミンペプチド323−339を、Bachem Americas Inc.(3132 Kashiwa Street,Torrance CA 90505;パーツ番号4065609)から購入した。ラパマイシンを、TSZ CHEM(185 Wilson Street,Framingham,MA 01702;製品カタログ番号R1017)から購入した。3:1のラクチド:グリコリド比および0.75dL/gの固有粘度を有するPLGAを、SurModics Pharmaceuticals(756 Tom Martin Drive,Birmingham,AL 35211;製品コード7525 DLG 7A)から購入した。ポリビニルアルコール(85〜89%加水分解されたもの)を、EMD Chemicals(製品番号1.41350.1001)から購入した。
溶液1:希塩酸水溶液中20mg/mLのオボアルブミンペプチド323−339。オボアルブミンペプチドを0.13Mの塩酸溶液に室温で溶解させることによって溶液を調製した。
溶液2:塩化メチレン中50mg/mLのラパマイシン。ラパマイシンを純粋な塩化メチレンに溶解させることによって溶液を調製した。
溶液3:塩化メチレン中100mg/mLのPLGA。PLGAを純粋な塩化メチレンに溶解させることによって溶液を調製した。
溶液4:100mMのpH8のリン酸緩衝液中50mg/mLのポリビニルアルコール。
第1の油中水型エマルジョンをまず調製した。溶液1(0.2mL)、溶液2(0.2mL)、および溶液3(1.0mL)を、小型の圧力管中で組み合わせて、Branson Digital Sonifier 250を用いて、50%の振幅で40秒間、超音波で分解することによって、W1/O1を調製した。次に、溶液4(3.0mL)を、第1のW1/O1エマルジョンと組み合わせて、10秒間ボルテックスし、Branson Digital Sonifier 250を用いて、30%の振幅で60秒間、超音波で分解することによって、第2のエマルジョン(W1/O1/W2)を調製した。
第1の油中水型エマルジョンをまず調製した。0.13Mの塩酸溶液(0.2mL)、溶液2(0.2mL)、および溶液3(1.0mL)を、小型の圧力管中で組み合わせて、Branson Digital Sonifier 250を用いて、50%の振幅で40秒間、超音波で分解することによって、W1/O1を調製した。次に、溶液4(3.0mL)を、第1のW1/O1エマルジョンと組み合わせて、10秒間ボルテックスし、Branson Digital Sonifier 250を用いて、30%の振幅で60秒間、超音波で分解することによって、第2のエマルジョン(W1/O1/W2)を調製した。
約3mgの合成ナノキャリアを収集し、遠心分離して、上清を合成ナノキャリアペレットから分離した。アセトニトリルをペレットに加え、試料を超音波で分解し、遠心分離して、あらゆる不溶性材料を除去した。上清およびペレットをRP−HPLCに注入し、278nmでの吸光度を読み取った。ペレットに見られたμgを用いて、取り込み%(負荷)を計算し、上清およびペレットのμgを用いて、回収された合計μgを計算した。
約3mgの合成ナノキャリアを収集し、遠心分離して、上清を合成ナノキャリアペレットから分離した。トリフルオロエタノールをペレットに加え、試料を超音波で分解して、ポリマーを溶解させ、0.2%のトリフルオロ酢酸を加え、試料を超音波で分解し、次に、遠心分離して、あらゆる不溶性材料を除去した。上清およびペレットをRP−HPLCに注入し、吸光度を215nmで読み取った。ペレットに見られたμgを用いて、取り込み%(負荷)を計算し、上清およびペレットのμgを用いて、回収された合計μgを計算した。
このアッセイには、免疫優性(immune−dominant)オボアルブミン(323−339)に特異的なトランスジェニックT細胞受容体を有するOTIIマウスの使用が含まれていた。抗原特異的なtDCを生成するために、CD11c+脾細胞を単離し、オボアルブミン(323−339)ペプチドをインビトロで1μg/mlでまたは抗原なしで加えた。次に、可溶性またはナノキャリア封入ラパマイシンを、2時間にわたってDCに加え、次に、それを十分に洗浄して、遊離ラパマイシンを培養物から除去した。精製されたレスポンダーCD4+CD25−細胞を、OTIIマウスから単離し、10:1のT対DC比でtDCに加えた。次に、tDCとOTII T細胞との混合物を4〜5日間培養し、Treg細胞(CD4+CD25highFoxP3+)の頻度を、図1に示されるようにフローサイトメトリーによって分析した。アイソタイプコントロールに基づいて領域を選択した。
メソ多孔質SiO2ナノ粒子コアを、ゾル・ゲル法によって生成する。ヘキサデシルトリメチルアンモニウムブロミド(CTAB)(0.5g)を、脱イオン水(500mL)に溶解させ、次に、2MのNaOH水溶液(3.5mL)を、CTAB溶液に加える。溶液を30分間撹拌し、次に、テトラエトキシシラン(TEOS)(2.5mL)を溶液に加える。得られたゲルを、80℃の温度で3時間撹拌する。生じる白色の沈殿物を、ろ過によって捕捉した後、脱イオン水で洗浄し、室温で乾燥させる。次に、残っている界面活性剤を、HClのエタノール溶液中で一晩懸濁させることによって粒子から抽出する。粒子を、エタノールで洗浄し、遠心分離し、超音波処理により再分散させる。この洗浄手順を更に2回繰り返す。
リポソームを、薄膜水和(thin film hydration)を用いて形成する。1,2−ジパルミトイル−sn−グリセロ−3−ホスホコリン(DPPC)(32μmol)、コレステロール(32μmol)、およびシクロスポリンA(6.4μmol)を、純粋なクロロホルム(3mL)に溶解させる。この脂質溶液を、50mLの丸底フラスコに加え、溶媒を、60℃の温度でロータリーエバポレータにおいて蒸発させる。次に、フラスコを、窒素ガスでフラッシュして、残りの溶媒を除去する。リン酸緩衝生理食塩水(2mL)および5つのガラスビーズをフラスコに加え、60℃で1時間振とうすることによって脂質膜を水和して、懸濁液を形成する。懸濁液を小型の圧力管に移し、各パルス間に30秒の遅延を伴う30秒のパルスの4回のサイクルにわたって、60℃で、超音波で分解する。次に、懸濁液を室温で2時間そのままにしておき、完全に水和させる。リポソームを、遠心分離によって洗浄した後、新鮮なリン酸緩衝生理食塩水に再懸濁させる。
PLGA−ラパマイシンコンジュゲートの調製:
酸性末端基を有するPLGAポリマー(7525 DLG1A、酸価0.46mmol/g、Lakeshore Biomaterials;5g、2.3mmol、1.0当量)を、30mLのジクロロメタン(DCM)に溶解させる。N,N−ジシクロヘキシルカルボジイミド(1.2当量、2.8mmol、0.57g)を加えた後、ラパマイシン(1.0当量、2.3mmol、2.1g)および4−ジメチルアミノピリジン(DMAP)(2.0当量、4.6mmol、0.56g)を加える。混合物を室温で2日間撹拌する。次に、混合物をろ過して、不溶性ジシクロヘキシル尿素を除去する。ろ液を、約10mLの体積に濃縮し、100mLのイソプロピルアルコール(IPA)に加えて、PLGA−ラパマイシンコンジュゲートを析出させる。IPA層を除去し、次に、ポリマーを、50mLのIPAおよび50mLのメチルt−ブチルエーテル(MTBE)で洗浄する。次に、ポリマーを、35Cで2日間、真空下で乾燥させて、白色の固体としてPLGA−ラパマイシン(約6.5g)を得る。
PLGA−ラパマイシンを含有するナノキャリアを、実施例1に記載される手順に従って、以下のとおりに調製する:
溶液1:希塩酸水溶液中20mg/mLのオボアルブミンペプチド323−339。オボアルブミンペプチドを0.13Mの塩酸溶液に室温で溶解させることによって溶液を調製する。溶液2:塩化メチレン中100mg/mLのPLGA−ラパマイシン。LGA−ラパマイシンを純粋な塩化メチレンに溶解させることによって溶液を調製する。溶液3:塩化メチレン中100mg/mLのPLA−PEG。PLA−PEGを純粋な塩化メチレンに溶解させることによって溶液を調製する。溶液4:100mMのpH8のリン酸緩衝液中50mg/mLのポリビニルアルコール。
HS−PEG−ラパマイシンの調製:
乾燥DMF中のPEG酸ジスルフィド(1.0当量)、ラパマイシン(2.0〜2.5当量)、DCC(2.5当量)およびDMAP(3.0当量)の溶液を、室温で一晩撹拌する。不溶性ジシクロヘキシル尿素を、ろ過によって除去し、ろ液をイソプロピルアルコール(IPA)に加えて、PEG−ジスルフィド−ジ−ラパマイシンエステルを析出させ、IPAで洗浄し、乾燥させる。次に、ポリマーを、DMF中のトリス(2−カルボキシエチル)ホスフィン塩酸塩で処理して、PEGジスルフィドを還元して、チオールPEGラパマイシンエステル(HS−PEG−ラパマイシン)にする。得られたポリマーを、IPAからの沈殿によって回収し、上述されるように乾燥させ、H NMRおよびGPCによって分析する。
500mLの1mMのHAuCl4の水溶液を、凝縮器を備えた1Lの丸底フラスコ中で激しく撹拌しながら、10分間加熱還流させる。次に、50mLの40mMのクエン酸三ナトリウムの溶液を、撹拌溶液に素早く加える。得られた濃いワインレッドの溶液を、25〜30分間還流状態に保ち、熱を取り除いて、溶液を室温に冷ます。次に、溶液を、0.8μmの薄膜フィルタを通してろ過して、AuNC溶液を得る。AuNCを、可視分光法および透過電子顕微鏡法を用いて特性評価する。AuNCは、直径が約20nmであり、クエン酸塩でキャッピングされ、520nmでピーク吸収を有する。
150μlのHS−PEG−ラパマイシン(10mMのpH9.0の炭酸緩衝液中10μΜ)の溶液を、1mLの20nmの直径のクエン酸塩でキャッピングされた金ナノキャリア(1.16nM)に加えて、2500:1のチオール対金のモル比を得る。混合物を、アルゴン下で、室温で1時間撹拌して、金ナノキャリア上でチオールとクエン酸塩との完全な交換を可能にする。次に、表面におけるPEG−ラパマイシンと複合したAuNCを、12,000gで30分間の遠心分離によって精製する。上清をデカントし、次に、AuNC−S−PEG−ラパマイシンを含有するペレットを、1×PBS緩衝液で洗浄する。次に、精製された金−PEG−ラパマイシンナノキャリアを、更なる分析およびバイオアッセイのために、好適な緩衝液に再懸濁させる。
メソ多孔質SiO2ナノ粒子コアを、ゾル・ゲル法によって生成する。ヘキサデシルトリメチルアンモニウムブロミド(CTAB)(0.5g)を、脱イオン水(500mL)に溶解させ、次に、2MのNaOH水溶液(3.5mL)を、CTAB溶液に加える。溶液を30分間撹拌し、次に、テトラエトキシシラン(TEOS)(2.5mL)を溶液に加える。得られたゲルを、80℃の温度で3時間撹拌する。生じる白色の沈殿物を、ろ過によって捕捉した後、脱イオン水で洗浄し、室温で乾燥させる。次に、残っている界面活性剤を、HClのエタノール溶液中で一晩懸濁させることによって粒子から抽出する。粒子を、エタノールで洗浄し、遠心分離し、超音波処理により再分散させる。この洗浄手順を更に2回繰り返す。
リポソームを、薄膜水和によって形成する。1,2−ジパルミトイル−sn−グリセロ−3−ホスホコリン(DPPC)(32μmol)、コレステロール(32μmol)、およびラパマイシン(6.4μmol)を、純粋なクロロホルム(3mL)に溶解させる。この脂質溶液を、10mLのガラス管に加え、溶媒を窒素ガス流下で除去し、真空下で6時間乾燥させる。過剰量のオボアルブミンを含有する2.0mlの25mMのMOPS緩衝液(pH8.5)による薄膜の水和によって、多重膜ベシクルを得る。脂質薄膜が管表面から剥がれるまで、管をボルテックスする。多重膜ベシクルを単層膜へと分解するために、10回のサイクルの凍結(液体窒素)および解凍(30℃の水浴)を行う。次に、試料を25mMのMOPS緩衝液(pH8.5)中で1mlまで希釈する。200nmの細孔のポリカーボネートフィルタに試料を10回通すことによって、得られたリポソームのサイズを、押出しによって均一にする。次に、得られたリポソームを、更なる分析およびバイオアッセイのために使用する。
工程1。L−フェニルアラニンエチルエステル(L−PAE)で修飾されたポリ(γ−グルタミン酸)(γ−PGA)の調製:4.7mmol単位のγ−PGA(Mn=300kD)を、0.3NのNaHCO3水溶液(50mL)に溶解させる。L−PAE(4.7mmol)およびEDC.HCl(4.7mmol)を溶液に加え、4Cで30分間撹拌する。次に、溶液を24時間撹拌しながら室温に維持する。低分子量の化学物質を、50kDのMWCOを有する透析膜を用いて透析によって除去する。得られたγ−PGA−グラフト−L−PAEは、凍結乾燥によって得られる。
EPO封入γ−PGAナノ粒子を調製するために、0.25〜4mgのEPOを、1mLのPBS(pH7.4)に溶解させ、1mLのγ−PGA−グラフト−L−PAE(DMSO中10mg/mL)をEPO溶液に加える。得られた溶液を、14,000×gで15分間遠心分離し、PBSで繰り返しすすぐ。次に、得られたEPO封入γ−PGAナノ粒子を、更なる分析およびバイオアッセイのためにPBS(5mg/mL)に再懸濁させる。
工程1。金NC(AuNC)の形成:500mLの1mMのHAuCl4の水溶液を、凝縮器を備えた1Lの丸底フラスコ中で激しく撹拌しながら、10分間加熱還流させる。次に、50mLの40mMのクエン酸三ナトリウムの溶液を、撹拌溶液に素早く加える。得られた濃いワインレッドの溶液を、25〜30分間還流状態に保ち、熱を取り除いて、溶液を室温に冷ます。次に、溶液を、0.8μmの薄膜フィルタを通してろ過して、AuNC溶液を得る。AuNCを、可視分光法および透過電子顕微鏡法を用いて特性評価する。AuNCは、直径が約20nmであり、クエン酸塩でキャッピングされ、520nmでピーク吸収を有する。
本発明の組成物を、リン酸緩衝生理食塩水(PBS)に溶解させ、500μgの組成物を含有する0.1〜0.2mlで雌のLewisラットに筋肉注射する。ラットの対照群には、0.1〜0.2mlのPBSを投与する。注射の9〜10日後、脾臓およびリンパ節を、ラットから採取し、組織を40μmのナイロンのセルストレーナー(cell strainer)に通して浸軟させることによって単細胞懸濁液を得る。関連するモノクローナル抗体の適切な希釈でPBS(1%のFCS)中で試料を染色する。プロピジウムヨージド染色細胞は、分析から除外する。試料をLSR2フローサイトメータ(BD Biosciences,USA)で取得し、FACS Divaソフトウェアを用いて分析する。マーカーCD8、CD25およびFoxP3の発現を細胞において分析する。CD8+CD25+FoxP3+細胞の存在は、Treg細胞の誘導を示唆する。
Balb/cマウスに、MHCクラスI拘束性および/またはMHCクラスII拘束性エピトープを含む自己抗原を投与し、CD8+制御性T細胞増殖のレベルを評価する。その後、エピトープを含む自己抗原またはその部分および免疫抑制剤を含む本発明の組成物を、用量依存的に皮下投与する。寛容原性免疫応答を示す増加によって、CD8+制御性T細胞増殖のレベルを再度評価する。
免疫抑制剤および骨髄細胞から得られるかまたはそれに由来する抗原を含む少なくとも106個の合成ナノキャリアの集団を、被験体が骨髄移植を受ける4週間前に、被験体に皮下投与する。被験体が移植を受けた後、被験体における望ましい免疫応答の生成を、移植を受けた後の最初の1週間は1日1回、その後、次の3週間にわたって週に1回、その後、次の11ヶ月間にわたって月に1回評価する。評価の一環として、CD8+制御性T細胞計数を行い、骨髄移植または合成ナノキャリアを被験体に投与する前に行ったCD8+制御性T細胞計数と比較する。最初の1年間、維持投与量の合成ナノキャリアを、被験体に2ヶ月に1回(bi−monthly)投与する。被験体は、骨髄移植に特異的なより高いまたは望ましいレベルのCD8+制御性T細胞を示すことが予測される。
本明細書に記載されるように、被験体が合成ナノキャリア(NC)を投与された後に被験体から得られる生体試料、例えば、末梢血から、CD8+Tregsを単離する。通常、生体試料を、投与されたNCがCD8+Tregsを誘導するのに十分な期間後に被験体から得る。陰性および/または陽性選択によって、生体試料、例えば、全血から、CD8+Tregsを単離する。
ナノキャリア
オボアルブミンタンパク質のTおよびB細胞エピトープであることが知られている17アミノ酸のペプチドであるオボアルブミンペプチド323−339を、Bachem Americas Inc.(3132 Kashiwa Street,Torrance CA 90505;パーツ番号4065609)から購入した。3:1のラクチド:グリコリド比および0.75dL/gの固有粘度を有するPLGAを、SurModics Pharmaceuticals(756 Tom Martin Drive,Birmingham,AL 35211;製品コード7525 DLG 7A)から購入した。約5,000DaのPEGブロックと約20,000DaのPLAブロックとのPLA−PEGブロックコポリマーを合成した。ポリビニルアルコール(85〜89%加水分解されたもの)を、EMD Chemicals(製品番号1.41350.1001)から購入した。
溶液1:希塩酸水溶液中20mg/mLのオボアルブミンペプチド323−339。オボアルブミンペプチドを0.13Mの塩酸溶液に室温で溶解させることによって溶液を調製した。溶液2:塩化メチレン中100mg/mLのPLGA。PLGAを純粋な塩化メチレンに溶解させることによって溶液を調製した。溶液3:塩化メチレン中100mg/mLのPLA−PEG。PLA−PEGを純粋な塩化メチレンに溶解させることによって、溶液を調製した。溶液4:100mMのpH8のリン酸緩衝液中50mg/mLのポリビニルアルコール。第1の油中水型エマルジョンをまず調製した。溶液1(0.2mL)、溶液2(0.75mL)、および溶液3(0.25mL)を、小型の圧力管中で組み合わせて、Branson Digital Sonifier 250を用いて、50%の振幅で40秒間、超音波で分解することによって、W1/O1を調製した。次に、溶液4(3.0mL)を、第1のW1/O1エマルジョンと組み合わせて、10秒間ボルテックスし、Branson Digital Sonifier 250を用いて、30%の振幅で60秒間、超音波で分解することによって、第2のエマルジョン(W1/O1/W2)を調製した。
ナノキャリアを解凍し、平衡化した。初期希釈は、10倍ストック溶液であり、これを、OVA323−339中100μg/mlの濃度に、即ち1倍溶液へと更に希釈した。この1倍溶液を、静脈注射当たり200μlで注射に使用した。動物をOVAタンパク質(OVA)で免疫化し、OVA323−339ペプチドで処理した。免疫化経路は以下のとおりであった:免疫学的にナイーブな雌のBalb/Cマウスのそれぞれにつき400μlで、10μgのOVA+4mgのミョウバンの腹腔内投与。実験群は、それぞれ5匹の動物からなっていた。脾臓細胞を、CFSEまたはCTOを用いて抗原で再度刺激して、Ag特異的な増殖の量を測定した。
オボアルブミン反応性IL−10を分泌するCD8+T細胞の頻度を、フローサイトメトリーによって計算した。脾細胞を、オボアルブミンタンパク質とともに、5%のCO2の37℃の完全培地において3日間培養した。3日目に、標準的な方法およびキットを用いた細胞内染色によって、細胞が異なるサイトカインを分泌する能力について細胞をアッセイした。簡潔に述べると、細胞を、ホルボールミリスチン酸アセテート(PMA)およびイオノマイシンで2時間にわたって再度刺激し、タンパク質輸送を更に4時間ブロックした。抗体の非特異的な結合を、抗CD16/32抗体でブロックし、次に、CD8、TCR、CD122およびCXCR5を特に認識する共役された抗体で細胞を染色した。パラホルムアルデヒドによる固定の後、細胞を透過化して、モノクローナル抗体を細胞に導入させ、細胞内エピトープ(サイトカイン)を標識した。CD8+TCR+CD122+CXCR5+IL−10+細胞の割合を測定した。
図2は、OVA323−339および免疫抑制剤を含む合成ナノキャリアで処理された動物被験体からの洗浄試料におけるCD8+制御性T細胞の生成におけるナノキャリアの有効性を示す。
ナノキャリア
オボアルブミンペプチドの代わりにMHCクラスI拘束性ペプチドSINFEKL(配列番号944)を用いて、上記の実施例(実施例15)と同様にナノキャリアを調製する。
ナノキャリアを解凍し、平衡化する。初期希釈は、10倍ストック溶液であり、これを、ペプチド中100μg/mlの濃度に、即ち1倍溶液へと更に希釈する。この1倍溶液を、静脈注射当たり200μlで注射に使用する。動物を、ペプチドを含むタンパク質で免疫化し、ペプチドで処理する。免疫化経路は以下のとおりである:免疫学的にナイーブな雌のBalb/Cマウスのそれぞれにつき400μlで、10μgのペプチド+4mgのミョウバンの腹腔内投与。実験群は、それぞれ5匹の動物からなる。脾臓細胞を、CFSEまたはCTOを用いて抗原で再度刺激して、Ag特異的な増殖の量を測定する。
タンパク質反応性IL−10を分泌するCD8+T細胞の頻度を、フローサイトメトリーによって計算する。脾細胞を、タンパク質とともに5%のCO2で37Cの完全培地において3日間培養する。3日目に、標準的な方法およびキットを用いた細胞内染色によって、細胞が異なるサイトカインを分泌する能力について細胞をアッセイする。簡潔に述べると、細胞を、ホルボールミリスチン酸アセテート(PMA)およびイオノマイシンで2時間にわたって再度刺激し、タンパク質輸送を更に4時間ブロックする。抗体の非特異的な結合を、抗CD16/32抗体でブロックし、次に、CD8、TCR、CD122およびCXCR5を特に認識する共役された抗体で細胞を染色する。パラホルムアルデヒドによる固定の後、細胞を透過化して、モノクローナル抗体を細胞に導入させ、細胞内エピトープ(サイトカイン)を標識する。CD8+TCR+CD122+CXCR5+IL−10+細胞の割合を測定する。
Claims (68)
- (i)免疫抑制剤に結合された合成ナノキャリアの第1の集団と、
(ii)抗原のMHCクラスI拘束性および/またはMHCクラスII拘束性エピトープに結合された合成ナノキャリアの第2の集団と
を含む組成物を被験体に投与する工程を含む方法であって、
前記組成物が、前記被験体における抗原特異的なCD8+制御性T細胞を生成するのに有効な量である方法。 - (i)免疫抑制剤に結合された合成ナノキャリアの第1の集団と、
(ii)抗原のMHCクラスI拘束性および/またはMHCクラスII拘束性に結合された合成ナノキャリアの第2の集団と
を含む組成物を投与することによって、被験体における抗原特異的なCD8+制御性T細胞を生成する工程を含む方法。 - 一体人以上の被験体における抗原特異的なCD8+制御性T細胞を生成することが既に示されたプロトコルに従って組成物を被験体に投与する工程を含む方法であって;
前記組成物が:
(i)免疫抑制剤に結合された合成ナノキャリアの第1の集団と、
(ii)抗原のMHCクラスI拘束性および/またはMHCクラスII拘束性エピトープに結合された合成ナノキャリアの第2の集団と
を含む方法。 - 前記第1の集団および前記第2の集団が同じ集団である、請求項1〜3のいずれか一項に記載の方法。
- 前記被験体を提供または同定する工程を更に含む、請求項1〜4のいずれか一項に記載の方法。
- 前記抗原が、治療用タンパク質、自己抗原またはアレルゲンであるか、或いは炎症性疾患、自己免疫疾患、臓器若しくは組織拒絶反応または移植片対宿主病と関連する、請求項1〜5のいずれか一項に記載の方法。
- 前記組成物の前記投与の前および/または前記投与の後に、前記被験体における抗原特異的なCD8+制御性T細胞の生成を評価する工程を更に含む、請求項1〜6のいずれか一項に記載の方法。
- 前記被験体が、炎症性疾患、自己免疫疾患、アレルギー、臓器若しくは組織拒絶反応または移植片対宿主病に罹患しているかまたは罹患するリスクがある、請求項1〜7のいずれか一項に記載の方法。
- 前記被験体が、移植を行ったかまたは移植を行う予定である、請求項1〜7のいずれか一項に記載の方法。
- 前記被験体が、前記被験体に投与されているかまたは投与される予定である治療用タンパク質に対する望ましくない免疫応答を有するかまたは有するリスクがある、請求項1〜7のいずれか一項に記載の方法。
- 移植可能な移植片または治療用タンパク質を前記被験体に投与する工程を更に含む、請求項1〜10のいずれか一項に記載の方法。
- 合成ナノキャリアの前記第1の集団および第2の集団を含む1つ以上の維持投与量の前記組成物が、前記被験体に投与される、請求項1〜11のいずれか一項に記載の方法。
- 前記合成ナノキャリアの前記投与が、静脈内、腹腔内、経粘膜、経口、皮下、経肺、鼻腔内、皮内または筋肉内投与によって行われる、請求項1〜12のいずれか一項に記載の方法。
- 前記合成ナノキャリアの前記投与が、吸入或いは静脈内、皮下または経粘膜投与によって行われる、請求項1〜13のいずれか一項に記載の方法。
- 前記移植可能な移植片または治療用タンパク質の前記投与は、前記治療用タンパク質が1個以上の細胞として提供される場合、非経口、動脈内、鼻腔内または静脈内投与によって、或いはリンパ節または前眼房への注射によって、或いは対象とする臓器または組織への局所投与によって行われる、請求項1〜14のいずれか一項に記載の方法。
- 前記生成された抗原特異的なCD8+制御性T細胞を収集する工程を更に含む、請求項1〜15のいずれか一項に記載の方法。
- 前記免疫抑制剤が、スタチン、mTOR阻害剤、TGF−βシグナル伝達剤、コルチコステロイド、ミトコンドリア機能の阻害剤、P38阻害剤、NF−κβ阻害剤、アデノシン受容体アゴニスト、プロスタグランジンE2アゴニスト、ホスホジエステラーゼ4阻害剤、HDAC阻害剤またはプロテアソーム阻害剤を含む、請求項1〜16のいずれか一項に記載の方法。
- 前記mTOR阻害剤がラパマイシンである、請求項17に記載の方法。
- 前記免疫抑制剤および/またはエピトープの負荷が、合成ナノキャリアの前記第1および/または第2の集団全体を平均して、0.0001%〜50%(重量/重量)である、請求項1〜18のいずれか一項に記載の方法。
- 前記免疫抑制剤および/またはエピトープの負荷が、合成ナノキャリアの前記第1および/または第2の集団全体を平均して、0.1%〜10%である、請求項19に記載の方法。
- 前記第1の集団および/または第2の集団の前記合成ナノキャリアが、脂質ナノ粒子、ポリマーナノ粒子、金属ナノ粒子、界面活性剤ベースのエマルジョン、デンドリマー、バッキーボール、ナノワイヤ、ウイルス様粒子またはペプチド若しくはタンパク質粒子を含む、請求項1〜20のいずれか一項に記載の方法。
- 前記第1の集団および/または第2の集団の前記合成ナノキャリアが、脂質ナノ粒子を含む、請求項21に記載の方法。
- 前記第1の集団および/または第2の集団の前記合成ナノキャリアが、リポソームを含む、請求項22に記載の方法。
- 前記第1の集団および/または第2の集団の前記合成ナノキャリアが、金属ナノ粒子を含む、請求項21に記載の方法。
- 前記金属ナノ粒子が金ナノ粒子を含む、請求項24に記載の方法。
- 前記第1の集団および/または第2の集団の前記合成ナノキャリアが、ポリマーナノ粒子を含む、請求項21に記載の方法。
- 前記ポリマーナノ粒子が、非メトキシ末端プルロニックポリマーであるポリマーを含む、請求項26に記載の方法。
- 前記ポリマーナノ粒子が、ポリエステル、ポリエーテルに結合されたポリエステル、ポリアミノ酸、ポリカーボネート、ポリアセタール、ポリケタール、多糖、ポリエチルオキサゾリンまたはポリエチレンイミンを含む、請求項26または27に記載の方法。
- 前記ポリエステルが、ポリ(乳酸)、ポリ(グリコール酸)、ポリ(乳酸−コ−グリコール酸)またはポリカプロラクトンを含む、請求項28に記載の方法。
- 前記ポリマーナノ粒子が、ポリエステルおよびポリエーテルに結合されたポリエステルを含む、請求項28または29に記載の方法。
- 前記ポリエーテルが、ポリエチレングリコールまたはポリプロピレングリコールを含む、請求項28〜30のいずれか一項に記載の方法。
- 前記第1および/または第2の集団の前記合成ナノキャリアの動的光散乱を用いて得られる粒度分布の平均が、100nmを超える直径である、請求項1〜31のいずれか一項に記載の方法。
- 前記直径が、150nmを超える、請求項32に記載の方法。
- 前記直径が、200nmを超える、請求項33に記載の方法。
- 前記直径が、250nmを超える、請求項34に記載の方法。
- 前記直径が、300nmを超える、請求項35に記載の方法。
- 前記第1の集団および/または第2の集団の前記合成ナノキャリアのアスペクト比が、1:1、1:1.2、1:1.5、1:2、1:3、1:5、1:7または1:10を超える、請求項1〜36のいずれか一項に記載の方法。
- 前記収集された抗原特異的なCD8+制御性T細胞を含む剤形を作製する工程を更に含む、請求項16〜37のいずれか一項に記載の方法。
- 前記収集された抗原特異的なCD8+制御性T細胞を被験体が投与に利用できるようにするかまたは剤形を被験体が投与に利用できるようにする工程を更に含む、請求項16〜38のいずれか一項に記載の方法。
- 移植可能な移植片または治療用タンパク質を、前記収集された抗原特異的なCD8+制御性T細胞または剤形に含める工程を更に含む、請求項16〜39のいずれか一項に記載の方法。
- 請求項1〜40のいずれか一項に記載の方法に従って生成される単離された抗原特異的なCD8+制御性T細胞を含む組成物。
- 薬学的に許容できる賦形剤を更に含む、請求項41に記載の組成物。
- 移植可能な移植片または治療用タンパク質を更に含む、請求項41または42に記載の組成物。
- 請求項41〜43のいずれか一項に記載の組成物を含む剤形。
- (i)免疫抑制剤に結合された合成ナノキャリアの第1の集団を生成する工程と、
(ii)抗原のMHCクラスI拘束性および/またはMHCクラスII拘束性エピトープに結合された合成ナノキャリアの第2の集団を生成する工程と
を含む方法。 - 前記第1の集団および第2の集団が同じ集団である、請求項45に記載の方法。
- 合成ナノキャリアの前記第1の集団および第2の集団を含む剤形を作製する工程を更に含む、請求項45または46に記載の方法。
- 合成ナノキャリアの前記第1の集団および第2の集団を含む組成物または前記剤形を、被験体が投与に利用できるようにする工程を更に含む、請求項45〜47のいずれか一項に記載の方法。
- 合成ナノキャリアの前記第1の集団および第2の集団を含む組成物による、抗原特異的なCD8+制御性T細胞の生成を評価する工程を更に含む、請求項45〜48のいずれか一項に記載の方法。
- 前記組成物が、抗原特異的なCD8+制御性T細胞を生成するのに有効な量である、請求項45〜49のいずれか一項に記載の方法。
- 生成される合成ナノキャリアの前記第1の集団および第2の集団が、請求項1〜43のいずれか一項に記載されるとおりである、請求項45〜50のいずれか一項に記載の方法。
- 組成物または剤形を生成するためのプロセスであって:
(i)合成ナノキャリアの第1の集団を免疫抑制剤に結合する工程と、
(ii)合成ナノキャリアの第2の集団を、抗原のMHCクラスI拘束性および/またはMHCクラスII拘束性エピトープに結合する工程と
を含むプロセス。 - 請求項45〜52のいずれか一項に記載の方法において規定される工程を含む、請求項52に記載のプロセス。
- 請求項1〜43のいずれか一項に記載の組成物。
- 請求項54に記載の組成物の剤形。
- 請求項45〜52のいずれか一項に記載の方法またはプロセスによって得られる組成物または剤形。
- 治療または予防に使用するための、請求項41〜43および54のいずれか一項に記載の組成物または請求項44に記載の剤形。
- 被験体における抗原特異的なCD8+制御性T細胞を生成する方法、アレルギー、自己免疫疾患、炎症性疾患、臓器若しくは組織拒絶反応または移植片対宿主病の治療または予防或いは請求項1〜40のいずれか一項に記載の方法に使用するための、請求項41〜43、54および56のいずれか一項に記載の組成物または請求項44または55に記載の剤形。
- 被験体における抗原特異的なCD8+制御性T細胞を生成する方法、アレルギー、自己免疫疾患、炎症性疾患、臓器若しくは組織拒絶反応または移植片対宿主病の治療または予防或いは請求項1〜40のいずれか一項に記載の方法に使用するための薬剤の製造のための、請求項41〜43、54および56のいずれか一項に記載の組成物または請求項44または55に記載の剤形の使用。
- 請求項56〜58のいずれか一項に記載の組成物を含む剤形。
- 治療または予防に使用するための、単離された抗原特異的なCD8+制御性T細胞を含む組成物であって、前記単離された抗原特異的なCD8+制御性T細胞が:
(a)(i)免疫抑制剤に結合された合成ナノキャリアの第1の集団と、(ii)抗原のMHCクラスI拘束性および/またはMHCクラスII拘束性エピトープに結合された合成ナノキャリアの第2の集団とを含む組成物を投与することによって、被験体における抗原特異的なCD8+制御性T細胞を生成する工程と;(b)前記生成された抗原特異的なCD8+制御性T細胞を収集する工程とを含むプロセスによって得られる組成物。 - 請求項41〜43のいずれか一項に記載されるとおりである、請求項61に記載の組成物。
- 治療または予防に使用するための、(i)免疫抑制剤に結合された合成ナノキャリアの第1の集団と、(ii)抗原のMHCクラスI拘束性および/またはMHCクラスII拘束性エピトープに結合された合成ナノキャリアの第2の集団とを含む組成物。
- 請求項1〜40のいずれか一項に記載されるとおりである、請求項63に記載の組成物。
- 治療または予防に使用するための、請求項41〜43、61および62のいずれか一項または請求項1〜40および56のいずれか一項に記載の組成物、または請求項44に記載の剤形。
- 被験体における寛容原性免疫応答を促進するかまたは抗原特異的なCD8+制御性T細胞を生成するのに使用するための、請求項41〜43、61および62のいずれか一項または請求項1〜40および56のいずれか一項に記載の組成物、または請求項44に記載の剤形。
- 被験体における寛容原性免疫応答を促進するかまたは抗原特異的なCD8+制御性T細胞を生成するのに使用するための薬剤の製造のための、請求項41〜43、61および62のいずれか一項または請求項1〜40および56のいずれか一項に記載の組成物、または請求項44に記載の剤形の使用。
- 請求項56〜58および61〜66のいずれか一項に記載の組成物を含む剤形。
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