KR20200071079A - 공동-자극을 위한 신규한 플랫폼, 신규한 car 설계 및 입양 세포 치료를 위한 다른 향상 - Google Patents
공동-자극을 위한 신규한 플랫폼, 신규한 car 설계 및 입양 세포 치료를 위한 다른 향상 Download PDFInfo
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Abstract
Description
도 2는 CD28 또는 41BB는 부재하나, NF-κB 자극 분자 (NEMO 및/또는 K13, 또는 그의 돌연변이체)를 발현하는 CAR을 도시하는 본 개시내용의 실시형태와 2세대 CAR 생물학적 활성 및 구조를 비교하는 도식을 도시한다.
도 3은 mNEMO-K270A, hNEMO-K277A에 의한 NF-κB의 강한 활성화 및 hNEMO-K277I 및 hNEMO-K277G 돌연변이체에 의한 약한 활성화를 도시한다.
도 4는 MPL을 표적화하고 161-scFv 표적화 도메인을 사용하는 이중특이적 T 세포 관여 인자의 활성을 도시한다. HEL-pLENTI-hGluc 및 T 세포를 4℃에서 2시간 동안 다음 상청액 배지 단독 및 pLENTI-161-StreptagII-CD3-Myc-His-P02 (042517-P02-SC)와 함께 별도로 사전 인큐베이션하였다. 인큐베이션 후, 세포를 37℃에서 4시간 동안 1:1 또는 5:1의 E:T 비로 U-바닥 96-웰 플레이트에서 공동 배양하였다. 50 μl의 세포+상청액/웰을 삼중 반복실험으로 하여 384웰로 옮겼다. 15 ul의 CTZ 분석 완충액 (1:100)을 사용하여 hGLuc 분석을 수행하였다.
도 5a 내지 도 5c는 TRAC 좌위로 표적화된 CRISPR/Cas9-매개 TFP 유전자 및 TRAC 발현을 회복시키기 위한 전략을 도시한다. 상부, TRAC 제1 엑손의 5 '말단 (회색), TRAC gRNA (청색) 및 해당 PAM 서열 (적색)을 갖는 a, Top, TRAC 좌위. 2개의 청색 화살표는 예측된 Cas9 이중 가닥 파손을 나타낸다. 하부, TRAC 좌위로의 CRISPR/Cas9-표적화된 혼입. 표적화 작제물 (AAV)은 스플라이싱 수용체 (SA), 이어서 F2A 코딩 서열, TFP 유전자 및 폴리A 서열을 포함하고, 이는 TRAC 좌위 (LHA 및 RHA, 좌 및 우 상동성 아암)와 상동성인 서열에 측접해 있다. 혼입되면, 내인성 TCRα 프로모터는 TFP 발현을 유도하고, TRAC 좌위는 분리된다. B) 표적화 작제물은 TFP를 발현하고, 2A 서열을 통해 TRAC (TCRα 불변 사슬)를 공동 발현한다. C) 표적화 작제물은 TFP를 발현하고, RHA에 존재하는 제1 엑손과 프레임 내에 존재하는 신호 펩타이드를 2A 서열을 통해 공동 발현하여, TCRα 프로모터는 TFP 발현뿐만 아니라, TCRα 가변 영역 (TRAV)이 부재하는 TRAC; TRAJ, TCRα 결합 영역; 2A, 자가 절단 2A 서열 발현을 유도한다. pA: SV40/β-글로빈 폴리A 서열.
도 6a 내지 도 6e는 Ab-TCR을 TRAC 좌위로 유도하기 위해 카세트 표적화를 위한 다양한 작제물 설계를 도시한다.
도 7a 내지 도 7f는 cTCR (SIR)을 TRAC 좌위로 유도하기 위해 카세트 표적화를 위한 다양한 작제물 설계를 도시한다.
도 8a 내지 도 8d는 cTCR (SIR) 및 TCR을 TRAC 좌위로 유도하기 위해 카세트 표적화를 위한 다양한 작제물 설계를 도시한다.
도 9a 내지 도 9d는 단일 사슬 cTCR (SIR)을 TRAC 좌위로 유도하기 위해 카세트 표적화를 위한 다양한 작제물 설계를 도시한다.
Claims (69)
- 면역 세포 또는 그의 면역 세포 집합으로서, (i) 적어도 하나의 비천연 발생 면역 수용체 및 (ii) NF-κB 신호전달 경로를 선택적으로(selectively) 활성화시키는 적어도 하나의 비천연 발생 제제를 발현하는, 면역 세포 또는 그의 면역 세포 집합.
- 제1항에 있어서, 적어도 하나의 비천연 발생 면역 수용체는 적어도 하나의 항원-결합 도메인 및 적어도 하나의 막관통 도메인을 포함하는, 면역 세포 또는 그의 면역 세포 집합.
- 제1항에 있어서, 적어도 하나의 비천연 발생 면역 수용체는 적어도 하나의 TCR 관련 신호전달 모듈을 채용할 수 있는, 면역 세포 또는 그의 면역 세포 집합.
- 제1항에 있어서, 적어도 하나의 비천연 발생 면역 수용체는 키메라 항원 수용체 (CAR) 또는 재조합 TCR인, 면역 세포 또는 그의 면역 세포 집합.
- 제2항에 있어서, 적어도 하나의 비천연 발생 면역 수용체의 적어도 하나의 항원-결합 도메인은 CD5; CD19; CD123; CD22; CD30; CD171; CS1 (CD2 하위세트 1, CRACC, MPL, SLAMF7, CD319, 및 19A24로도 지칭됨); C형 렉틴-유사 분자-1 (CLL-1 또는 CLECL1); CD33; 상피 성장 인자 수용체 변이체 III (EGFRviii); 강글리오사이드 G2 (GD2); 강글리오사이드 GD3 (aNeu5Ac(2-8)aNeu5Ac(2-3)bDGalp(l-4)bDGlcp(l-l)Cer); TNF 수용체 패밀리 구성원 B 세포 성숙 (BCMA); Tn 항원 ((Tn Ag) 또는 (GalNAcα-Ser/Thr)); 전립선-특이적 막 항원 (PSMA); 수용체 티로신 키나제-유사 고아 수용체 1 (ROR1); Fms 유사 티로신 키나제 3 (FLT3); 종양-관련 당단백질 72 (TAG72); CD38; CD44v6; 조혈 전구체 상이 아닌 급성 백혈병 또는 림프종 상에 발현되는 글리코실화된 CD43 에피토프, 비 조혈암 상에 발현되는 글리코실화된 CD43 에피토프, 종양태아성 항원 (CEA); 상피 세포 부착 분자 (EPCAM); B7H3 (CD276); KIT (CD117); 인터루킨-13 (Interleukin-13) 수용체 하위단위 알파-2 (IL-13Ra2 또는 CD213A2); 메소텔린 (Mesothelin); 인터루킨 11 수용체 알파 (IL-llRa); 전립선 줄기세포 항원 (PSCA); 세린 프로테아제 21 (테스티신 (Testisin) 또는 PRSS21); 혈관내피 성장 인자 수용체 2 (VEGFR2); 루이스(Y) 항원; CD24; 혈소판 유래 성장 인자 수용체 베타 (PDGFR-베타); 단계-특이적 배아 항원-4 (SSEA-4); CD20; 엽산 수용체 알파 (FRa 또는 FR1); 엽산 수용체 베타 (FRb); 수용체 티로신-단백질 키나제 ERBB2 (Her2/neu); 세포 표면 결합 뮤신 1 (Mucin 1, cell surface associated) (MUC1); 상피 성장 인자 수용체 (EGFR); 신경 세포 부착 분자 (NCAM); 프로스타제 (Prostase); 전립선 산성 포스파타제 (PAP); 돌연변이 연장 인자 2 (ELF2M); 에프린 B2 (Ephrin B2); 섬유아세포 활성화 단백질 알파 (FAP); 인슐린-유사 성장 인자 1 수용체 (IGF-I 수용체), 탄산무수화효소 IX (CAlX); 프로테아좀 (Proteasome) (프로좀 (Prosome), 마크로파인 (Macropain)) 하위단위, 베타 유형, 9 (LMP2); 당단백질 100 (gpl00); 중단점 클러스터 영역 (BCR) 및 아벨슨 (Abelson) 쥣과동물 백혈병 바이러스 암유전자 상동체 1 (Abl) (bcr-abl)로 이루어진 암유전자 융합 단백질; 티로시나제 (Tyrosinase); 에프린 유형-A 수용체 2 (EphA2); 시알릴 루이스 부착 분자 (sLe); 강글리오사이드 GM3 (aNeu5Ac(2-3)bDClalp(l-4)bDGlcp(l-1)Cer); 트랜스글루타미나제 5 (transglutaminase 5) (TGS5); 고분자량-흑색종 관련 항원 (HMWMAA); o-아세틸-GD2 강글리오사이드 (OAcGD2); 종양 내피 마커 1 (TEM1/CD248); 종양 내피 마커 7-관련 (TEM7R); 클라우딘 6 (Claudin 6)(CLDN6); 갑상선 자극 호르몬 수용체 (TSHR); G 단백질 연결 수용체 클래스 C 그룹 5, 구성원 D (GPRC5D); 염색체 X 오픈 리딩 프레임 61 (CXORF61); CD97; CD179a; 역형성 림프종 키나제 (ALK); 폴리시알산; 태반-특이적 1 (PLAC1); globoH 글리코세라마이드 (GloboH)의 육당류 부분; 포유류 샘 분화 항원 (NY-BR-1); 유로플라킨 2 (uroplakin 2) (UPK2); A형 간염 바이러스 세포 수용체 1 (HAVCR1); 아드레날린수용체 베타 3 (adrenoceptor beta 3) (ADRB3); 파넥신 3 (pannexin 3) (PANX3); G 단백질 연결 수용체 20 (GPR20); 림프구 항원 6 복합체, 좌위 K 9 (LY6K); 후각 수용체 51E2 (OR51E2); TCR 감마 대체 리딩 프레임 단백질 (TARP); 빌름스 종양 단백질 (Wilms tumor protein) (WT1); 암/고환 항원 1 (NY-ESO-1); 암/고환 항원 2 (LAGE-1a); 흑색종-관련 항원 1 (MAGE-A1); 염색체 12p에 위치한 ETS 전좌-변이체 유전자 6 (ETV6-AML); 정자 단백질 17 (SPA17); X 항원 패밀리, 구성원 lA (XAGEl); 안지오포이에틴 (angiopoietin)-결합 세포 표면 수용체 2 (Tie 2); 흑색종 고환암 항원-1 (MAD-CT-1); 흑색종 고환암 항원-2 (MAD-CT-2); Fos-관련 항원 1; 종양 단백질 p53 (p53); p53 돌연변이체; 프로스테인 (prostein); 서바이빈 (survivin); 텔로머라제 (telomerase); 전립선 암종 종양 항원-1 (PCT A-1 또는 갈렉틴 8 (Galectin 8)), T 세포 1에 의해 인식되는 흑색종 항원 (MelanA 또는 MARTI); 랫트 육종 (Ras) 돌연변이체; 인간 텔로머라제 역전사효소 (hTERT); 육종 전좌 중단점; 아폽토시스의 흑색종 억제제 (ML-IAP); ERG (막관통 프로테아제, 세린 2 (TMPRSS2) ETS 융합 유전자); N-아세틸 글루코사미닐-트랜스퍼라제 V (NA17); 쌍 형성 box 단백질 Pax-3 (PAX3); 안드로겐 수용체 (androgen receptor); 사이클린 Bl (Cyclin B1); v-myc 조류 골수세포증 바이러스 암유전자 신경아세포 유래 상동체 (MYCN); Ras 상동체 패밀리 구성원 C (RhoC); 티로시나제-관련 단백질 2 (TRP-2); 시토크롬 P450 lB 1 (CYPlB 1); CCCTC-결합 인자 (아연 핑거 단백질 (Zinc finger protein))-유사 (BORIS 또는 Brother of the Regulator oflmprinted Sites), T 세포 3에 의해 인식되는 편평 세포 암종 항원 (SART3); 쌍 형성 box 단백질 Pax-5 (PAX5); 프로아크로신 (proacrosin) 결합 단백질 sp32 (OY-TESl); 림프구-특이적 단백질 티로신 키나제 (LCK); A 키나제 고정 단백질 4 (AKAP-4); 활액 육종, X 중단점 2 (SSX2); 진행된 최종 당화 산물의 수용체 (RAGE-1); 신장 산재 인자 1 (renal ubiquitous 1) (RUl); 신장 산재 인자 2 (RU2); 레구메인 (legumain); 인간 유두종 바이러스 E6 (HPV E6); 인간 유두종 바이러스 E7 (HPV E7); 장내 카복실 에스테라제; 돌연변이 열 충격 단백질 70-2 (mut hsp70-2); CD79a; CD79b; CD72; 백혈구-관련 면역글로불린-유사 수용체 1 (LAIRl); IgA 수용체의 Fc 단편 (FCAR 또는 CD89); 백혈구 면역글로불린-유사 수용체 서브패밀리 A 구성원 2 (LILRA2); CD300 분자-유사 패밀리 구성원 f (CD300LF); C형 렉틴 도메인 패밀리 12 구성원 A (CLEC12A); 골수 기질 세포 항원 2 (BST2); EGF-유사 모듈-포함 뮤신-유사 호르몬 수용체-유사 2 (EMR2); 림프구 항원 75 (LY75); 글리피칸-3 (GPC3); Fc 수용체-유사 5 (FCRL5); 및 면역글로불린 람다-유사 폴리펩타이드 1 (IGLLl), MPL, 비오틴, c-MYC 에피토프 Tag, CD34, LAMP1 TROP2, GFR알파4, CDH17, CDH6, NYBR1, CDH19, CD200R, Slea (CA19.9; 시알릴 루이스 항원); 푸코실-GM1, PTK7, gpNMB, CDH1-CD324, DLL3, CD276/B7H3, IL11Ra, IL13Ra2, CD179b-IGLl1, TCR감마-델타, NKG2D, CD32 (FCGR2A), Tn ag, Tim1-/HVCR1, CSF2RA (GM-CSFR-알파), TGF베타R2, Lews Ag, TCR-베타1 사슬, TCR-베타2 사슬, TCR-감마 사슬, TCR-델타 사슬, FITC, 황체형성 호르몬 수용체 (LHR), 여포 자극 호르몬 수용체 (FSHR), 성샘자극 호르몬 수용체 (CGHR 또는 GR), CCR4, GD3, SLAMF6, SLAMF4, HIV1 외피 당단백질, HTLV1-Tax, CMV pp65, EBV-EBNA3c, KSHV K8.1, KSHV-gH, A형 인플루엔자 혈구응집소 (influenza A hemagglutinin) (HA), GAD, PDL1, 구아닐릴 사이클라제 C (GCC), 데스모글레인 3 (desmoglein 3) (Dsg3)에 대한 자기항체, 데스모글레인 1 (Dsg1)에 대한 자기항체, HLA, HLA-A, HLA-A2, HLA-B, HLA-C, HLA-DP, HLA-DM, HLA-DOA, HLA-DOB, HLA-DQ, HLA-DR, HLA-G, IgE, CD99, Ras G12V, 조직 인자 1 (TF1), AFP, GPRC5D, 클라우딘18.2 (CLD18A2 또는 CLDN18A.2), P-당단백질, STEAP1, Liv1, 넥틴-4 (Nectin-4), 크립토 (Cripto), gpA33, BST1/CD157, 낮은 전도도 염화물 채널, 및 TNT 항체에 의해 인식되는 항원으로 이루어진 군으로부터 선택되는 항원에 결합하는, 면역 세포 또는 그의 면역 세포 집합.
- 제1항에 있어서, NF-κB 경로를 선택적으로 활성화시킬 수 있는 적어도 하나의 비천연 발생 제제는 vFLIP K13, K13-opt, NEMO 돌연변이체, NEMO-융합 단백질, IKK1-S176E-S180E, IKK2-S177E-S181E, RIP, IKKα, IKKβ, Tcl-1, MyD88-L265, 임의의 NF-κB 활성화 단백질 또는 단백질 단편, NF-κB 경로의 억제제 중 임의의 억제제, NF-κB를 선택적으로 활성화시킬 수 있는 임의의 유전자 편집 시스템, 이들의 임의의 상동체 또는 변이체 및 이들의 임의의 조합으로 이루어진 군으로부터 선택되는, 면역 세포 또는 그의 면역 세포 집합.
- 제1항에 있어서, NF-κB 경로를 선택적으로 활성화시킬 수 있는 적어도 하나의 비천연 발생 제제는 비 바이러스 유래인, 면역 세포 또는 그의 면역 세포 집합.
- 제1항에 있어서, NF-κB 경로를 선택적으로 활성화시킬 수 있는 적어도 하나의 비천연 발생 제제는 유전자 편집 시스템인, 면역 세포 또는 그의 면역 세포 집합.
- 제1항에 있어서, NF-κB 경로를 선택적으로 활성화시킬 수 있는 적어도 하나의 비천연 발생 제제는 NEMO/IKKγ의 올리고머화를 유도하는, 면역 세포 또는 그의 면역 세포 집합.
- 제1항에 있어서, NF-κB 경로를 선택적으로 활성화시킬 수 있는 적어도 하나의 비천연 발생 제제는 IKK 복합체의 활성화를 유도하는, 면역 세포 또는 그의 면역 세포 집합.
- 제1항에 있어서, NF-κB 경로를 선택적으로 활성화시킬 수 있는 적어도 하나의 비천연 발생 제제는 AKT 경로를 활성화시키지 않는, 면역 세포 또는 그의 면역 세포 집합.
- 제1항에 있어서, NF-κB 경로를 선택적으로 활성화시킬 수 있는 적어도 하나의 비천연 발생 제제는 항시적 또는 유도성 방식으로 발현되는, 면역 세포 또는 그의 면역 세포 집합.
- 제1항에 있어서, NF-κB 경로를 선택적으로 활성화시킬 수 있는 적어도 하나의 비천연 발생 제제는 일시적으로 발현되는, 면역 세포 또는 그의 면역 세포 집합.
- 제1항에 있어서, NF-κB 경로를 선택적으로 활성화시킬 수 있는 적어도 하나의 비천연 발생 제제는 안정하게 발현되는, 면역 세포 또는 그의 면역 세포 집합.
- 제1항에 있어서, NF-κB 경로를 선택적으로 활성화시킬 수 있는 적어도 하나의 비천연 발생 제제의 활성은 세포와 화합물의 접촉을 통해 번역 후 제어되는, 면역 세포 또는 그의 면역 세포 집합.
- 제1항에 있어서, NF-κB 경로를 선택적으로 활성화시킬 수 있는 적어도 하나의 비천연 발생 제제는 스위치 도메인의 하나 이상의 카피를 갖는 융합 작제물(fusion construct)로서 발현되는, 면역 세포 또는 그의 면역 세포 집합.
- 제9항에 있어서, NF-κB 경로를 선택적으로 활성화시킬 수 있는 적어도 하나의 비천연 발생 제제의 활성은 스위치 도메인의 이량체화의 이량체화를 유도하는 화합물의 치료 유효량의 투여에 의해 번역 후 수준에서 제어되는, 면역 세포 또는 그의 면역 세포 집합.
- 제16항 또는 제17항에 있어서, 스위치 도메인은 FKBP12 도메인의 하나 이상의 카피를 포함하는, 면역 세포 또는 그의 면역 세포 집합.
- 제15항에 있어서, 화합물은 AP20187 또는 리미두시드 (Rimiducid) 또는 그의 상동체인, 면역 세포 또는 그의 면역 세포 집합.
- 제1항에 있어서, 면역 세포는 T-림프구 (T 세포), CAR-T 세포, TCR-발현 T 세포, 종양 침윤 림프구 (TIL), 조직 상재 림프구, 줄기세포, 유도된 전능성 줄기세포 또는 자연 살해 (NK) 세포인, 면역 세포 또는 그의 면역 세포 집합.
- 제1항에 있어서, 면역 세포는 기능성 고유 T 세포 수용체 (TCR) 신호전달 복합체 및/또는 β2 마이크로글로불린이 부재하도록 조작되는, 면역 세포 또는 그의 면역 세포 집합.
- 제1항 및 제21항에 있어서, 적어도 하나의 비천연 발생 면역 수용체 및/또는 NF-κB 신호전달 경로를 선택적으로 활성화시킬 수 있는 적어도 하나의 제제의 발현이 TCR 유전자의 내인성 조절 요소/프로모터의 제어 하에 있도록 적어도 하나의 비천연 발생 면역 수용체 및/또는 NF-κB 신호전달 경로를 선택적으로 활성화시킬 수 있는 적어도 하나의 제제는 내인성 TCR 유전자 내에 클로닝되는, 면역 세포 또는 그의 면역 세포 집합.
- 제1항에 있어서, 암, 감염성 질병, 면역 질병 및 알레르기 질병의 군으로부터 선택되는 질병의 예방 및 치료에 사용되는, 면역 세포 또는 그의 면역 세포 집합.
- 제1항에 있어서, 적어도 하나의 비천연 발생 면역 수용체를 인코딩하고, NF-κB 신호전달 경로를 선택적으로 활성화시킬 수 있는 적어도 하나의 비천연 발생 제제를 인코딩하는 적어도 하나의 폴리뉴클레오타이드는 단일 프로모터로부터 발현되는, 면역 세포 또는 그의 면역 세포 집합.
- 제1항에 있어서, 적어도 하나의 비천연 발생 면역 수용체 및 NF-κB 신호전달 경로를 선택적으로 활성화시킬 수 있는 적어도 하나의 비천연 발생 제제를 인코딩하는 적어도 하나의 폴리뉴클레오타이드는 2개 이상의 개별 프로모터를 사용하여 발현되는, 면역 세포 또는 그의 면역 세포 집합.
- 제24항 또는 제25항에 있어서, 적어도 하나의 폴리뉴클레오타이드는, 제1 및 제2 핵산 코딩 서열의 발현시 비천연 발생 면역 수용체 및 NF-κB를 선택적으로 활성화시킬 수 있는 비천연 발생 제제는 물리적 또는 화학적으로 연결되지 않도록, NF-κB를 선택적으로 활성화시킬 수 있는 비천연 발생 제제를 인코딩하는 제2 핵산 서열로부터 분리된 적어도 하나의 비천연 발생 면역 수용체를 인코딩하는 제1 핵산 코딩 서열을 포함하는, 면역 세포 또는 그의 면역 세포 집합.
- 제24항 또는 제25항에 있어서, 적어도 하나의 비천연 발생 면역 수용체 및/또는 적어도 하나의 NF-κB를 선택적으로 활성화시킬 수 있는 비천연 발생 제제가 TCR 유전자의 내인성 조절 요소/프로모터의 제어 하에 있도록 적어도 하나의 비천연 발생 면역 수용체 및/또는 NF-κB 코딩 폴리뉴클레오타이드(들)를 선택적으로 활성화시킬 수 있는 적어도 하나의 비천연 발생 제제는 내인성 TCR 유전자 내에 클로닝되는, 면역 세포 또는 그의 면역 세포 집합.
- 제21항 또는 제27항에 있어서, TCR 유전자의 하나 이상의 불변 사슬이 기능적으로 재 발현되는, 면역 세포 또는 그의 면역 세포 집합.
- 적어도 하나의 비천연 발생 면역 수용체를 인코딩하는 적어도 하나의 재조합 폴리뉴클레오타이드로서,
(a) 일부 또는 전체 막관통 및/또는 세포질 도메인 및 임의적으로(optionally) 내인성 단백질의 세포외 도메인을 인코딩하는 제1 핵산 도메인으로서, 내인성 단백질은 림프구의 표면에 발현되고, 림프구의 활성화 및/또는 증식을 촉발시키는 제1 핵산 도메인;
(b) 임의적으로 폴리뉴클레오타이드 링커;
(c) 제1 핵산 도메인에 작동 가능하게 연결된 제2 핵산 도메인으로서, 제2 핵산 도메인은 하나 이상의 비천연 TCR 항원 결합 도메인(들)을 인코딩하는 제2 핵산 도메인;
(d) 공자극 도메인을 인코딩하는 임의적 제3 핵산 도메인; 및
(e) 보조 모듈을 인코딩하는 추가의 임의적 핵산 도메인
을 포함하는, 적어도 하나의 재조합 폴리뉴클레오타이드. - a) 비천연 발생 면역 수용체를 인코딩하는 제1 핵산; 및
b) 선택적 NF-κB 활성화제를 포함하는 보조 모듈을 인코딩하는 제2 핵산
을 포함하는, 적어도 하나의 재조합 폴리뉴클레오타이드. - 제30항에 있어서, 제1 핵산 및 제2 핵산은 절단 가능한 펩타이드 링커를 인코딩하는 올리고뉴클레오타이드 링커에 의해 분리되는, 적어도 하나의 재조합 폴리뉴클레오타이드.
- 제30항에 있어서, 제1 핵산 및 제2 핵산이 개별 벡터로부터 발현되도록 2개의 재조합 폴리뉴클레오타이드를 포함하는, 적어도 하나의 재조합 폴리뉴클레오타이드.
- 제30항에 있어서, 선택적 NF-κB 활성화제는 비천연 발생 선택적 NF-κB 활성화제인, 적어도 하나의 재조합 폴리뉴클레오타이드.
- 제30항에 있어서, 비천연 발생 면역 수용체는 CAR, Ab-TCR, TFP, cTCR, SIR 및 재조합 TCR로 이루어진 군으로부터 선택되는, 적어도 하나의 폴리뉴클레오타이드.
- 제30항에 있어서, 비천연 발생 면역 수용체는 (i) 세포외 항원 특이적 도메인, (ii) 막관통 도메인, 및 (iii) 면역수용체 티로신-기반 활성화 모티프 (ITAM)를 포함하는 임의적 세포내 신호전달 도메인을 포함하고, (iii)은 비천연 발생 면역 수용체의 C 말단에 위치하는, 적어도 하나의 폴리뉴클레오타이드.
- 제30항에 있어서, 제1 및 제2 핵산 서열의 발현시 비천연 발생 면역 수용체 및 선택적 NF-κB 활성화제 폴리펩타이드는 물리적 또는 화학적으로 연결되지 않은, 적어도 하나의 폴리뉴클레오타이드.
- 제35항에 있어서, 세포외 항원-특이적 도메인은 CD5; CD19; CD123; CD22; CD30; CD171; CS1 (CD2 하위세트 1, CRACC, MPL, SLAMF7, CD319, 및 19A24로도 지칭됨); C형 렉틴-유사 분자-1 (CLL-1 또는 CLECL1); CD33; 상피 성장 인자 수용체 변이체 III (EGFRviii); 강글리오사이드 G2 (GD2); 강글리오사이드 GD3 (aNeu5Ac(2-8)aNeu5Ac(2-3)bDGalp(l-4)bDGlcp(l-l)Cer); TNF 수용체 패밀리 구성원 B 세포 성숙 (BCMA); Tn 항원 ((Tn Ag) 또는 (GalNAcα-Ser/Thr)); 전립선-특이적 막 항원 (PSMA); 수용체 티로신 키나제-유사 고아 수용체 1 (ROR1); Fms 유사 티로신 키나제 3 (FLT3); 종양-관련 당단백질 72 (TAG72); CD38; CD44v6; 조혈 전구체 상이 아닌 급성 백혈병 또는 림프종 상에 발현되는 글리코실화된 CD43 에피토프, 비 조혈암 상에 발현되는 글리코실화된 CD43 에피토프, 종양태아성 항원 (CEA); 상피 세포 부착 분자 (EPCAM); B7H3 (CD276); KIT (CD117); 인터루킨-13 수용체 하위단위 알파-2 (IL-13Ra2 또는 CD213A2); 메소텔린; 인터루킨 11 수용체 알파 (IL-llRa); 전립선 줄기세포 항원 (PSCA); 세린 프로테아제 21 (테스티신 또는 PRSS21); 혈관내피 성장 인자 수용체 2 (VEGFR2); 루이스(Y) 항원; CD24; 혈소판 유래 성장 인자 수용체 베타 (PDGFR-베타); 단계-특이적 배아 항원-4 (SSEA-4); CD20; 엽산 수용체 알파 (FRa 또는 FR1); 엽산 수용체 베타 (FRb); 수용체 티로신-단백질 키나제 ERBB2 (Her2/neu); 뮤신 1, 세포 표면 결합 (MUC1); AFP/MHC 복합체; 상피 성장 인자 수용체 (EGFR); 신경 세포 부착 분자 (NCAM); 프로스타제; 전립선 산성 포스파타제 (PAP); 돌연변이 연장 인자 2 (ELF2M); 에프린 B2; 섬유아세포 활성화 단백질 알파 (FAP); 인슐린-유사 성장 인자 1 수용체 (IGF-I 수용체), 탄산무수화효소 IX (CAlX); 프로테아좀 (프로좀, 마크로파인) 하위단위, 베타 유형, 9 (LMP2); 당단백질 100 (gpl00); 중단점 클러스터 영역 (BCR) 및 아벨슨 쥣과동물 백혈병 바이러스 암유전자 상동체 1 (Abl) (bcr-abl)로 이루어진 암유전자 융합 단백질; 티로시나제; 에프린 유형-A 수용체 2 (EphA2); 시알릴 루이스 부착 분자 (sLe); 강글리오사이드 GM3 (aNeu5Ac(2-3)bDClalp(l-4)bDGlcp(l-1)Cer); 트랜스글루타미나제 5 (TGS5); 고분자량-흑색종 관련 항원 (HMWMAA); o-아세틸-GD2 강글리오사이드 (OAcGD2); 종양 내피 마커 1 (TEM1/CD248); 종양 내피 마커 7-관련 (TEM7R); 클라우딘 6 (CLDN6); 갑상선 자극 호르몬 수용체 (TSHR); G 단백질 연결 수용체 클래스 C 그룹 5, 구성원 D (GPRC5D); 염색체 X 오픈 리딩 프레임 61 (CXORF61); CD97; CD179a; 역형성 림프종 키나제 (ALK); 폴리시알산; 태반-특이적 1 (PLAC1); globoH 글리코세라마이드 (GloboH)의 육당류 부분; 포유류 샘 분화 항원 (NY-BR-1); 유로플라킨 2 (UPK2); A형 간염 바이러스 세포 수용체 1 (HAVCR1); 아드레날린수용체 베타 3 (ADRB3); 파넥신 3 (PANX3); G 단백질 연결 수용체 20 (GPR20); 림프구 항원 6 복합체, 좌위 K 9 (LY6K); 후각 수용체 51E2 (OR51E2); TCR 감마 대체 리딩 프레임 단백질 (TARP); 빌름스 종양 단백질 (WT1); WT1/MHC I 복합체; 암/고환 항원 1 (NY-ESO-1); NY-ESO-1/MHC I 복합체, 암/고환 항원 2 (LAGE-1a); 흑색종-관련 항원 1 (MAGE-A1); 염색체 12p에 위치한 ETS 전좌-변이체 유전자 6 (ETV6-AML); 정자 단백질 17 (SPA17); X 항원 패밀리, 구성원 lA (XAGEl); 안지오포이에틴-결합 세포 표면 수용체 2 (Tie 2); 흑색종 고환암 항원-1 (MAD-CT-1); 흑색종 고환암 항원-2 (MAD-CT-2); Fos-관련 항원 1; 종양 단백질 p53 (p53); p53 돌연변이체; 프로스테인; 서바이빈; 텔로머라제; 전립선 암종 종양 항원-1 (PCT A-1 또는 갈렉틴 8), T 세포 1에 의해 인식되는 흑색종 항원 (MelanA 또는 MARTI); 랫트 육종 (Ras) 돌연변이체; 인간 텔로머라제 역전사효소 (hTERT); 육종 전좌 중단점; 아폽토시스의 흑색종 억제제 (ML-IAP); ERG (막관통 프로테아제, 세린 2 (TMPRSS2) ETS 융합 유전자); N-아세틸 글루코사미닐-트랜스퍼라제 V (NA17); 쌍 형성 box 단백질 Pax-3 (PAX3); 안드로겐 수용체; 사이클린 Bl; v-myc 조류 골수세포증 바이러스 암유전자 신경아세포 유래 상동체 (MYCN); Ras 상동체 패밀리 구성원 C (RhoC); 티로시나제-관련 단백질 2 (TRP-2); 시토크롬 P450 lB 1 (CYPlB 1); CCCTC-결합 인자 (아연 핑거 단백질)-유사 (BORIS 또는 Brother of the Regulator oflmprinted Sites), T 세포 3에 의해 인식되는 편평 세포 암종 항원 (SART3); 쌍 형성 box 단백질 Pax-5 (PAX5); 프로아크로신 결합 단백질 sp32 (OY-TESl); 림프구-특이적 단백질 티로신 키나제 (LCK); A 키나제 고정 단백질 4 (AKAP-4); 활액 육종, X 중단점 2 (SSX2); 진행된 최종 당화 산물의 수용체 (RAGE-1); 신장 산재 인자 1 (RUl); 신장 산재 인자 2 (RU2); 레구메인; 인간 유두종 바이러스 E6 (HPV E6); HPV E6/MHC I 복합체; 인간 유두종 바이러스 E7 (HPV E7); HPV E7/MHC I 복합체; AFP/MHC I 복합체; Ras/MHC I 복합체; 장내 카복실 에스테라제; 돌연변이 열 충격 단백질 70-2 (mut hsp70-2); CD79a; CD79b; CD72; 백혈구-관련 면역글로불린-유사 수용체 1 (LAIRl); IgA 수용체의 Fc 단편 (FCAR 또는 CD89); 백혈구 면역글로불린-유사 수용체 서브패밀리 A 구성원 2 (LILRA2); CD300 분자-유사 패밀리 구성원 f (CD300LF); C형 렉틴 도메인 패밀리 12 구성원 A (CLEC12A); 골수 기질 세포 항원 2 (BST2); EGF-유사 모듈-포함 뮤신-유사 호르몬 수용체-유사 2 (EMR2); 림프구 항원 75 (LY75); 글리피칸-3 (GPC3); Fc 수용체-유사 5 (FCRL5); 및 면역글로불린 람다-유사 폴리펩타이드 1 (IGLLl), MPL, 비오틴, c-MYC 에피토프 Tag, CD34, LAMP1 TROP2, GFR알파4, CDH17, CDH6, NYBR1, CDH19, CD200R, Slea (CA19.9; 시알릴 루이스 항원); 푸코실-GM1, PTK7, gpNMB, CDH1-CD324, DLL3, CD276/B7H3, IL11Ra, IL13Ra2, CD179b-IGLl1, TCR감마-델타, NKG2D, CD32 (FCGR2A), Tn ag, Tim1-/HVCR1, CSF2RA (GM-CSFR-알파), TGF베타R2, Lews Ag, TCR-베타1 사슬, TCR-베타2 사슬, TCR-감마 사슬, TCR-델타 사슬, FITC, 황체형성 호르몬 수용체 (LHR), 여포 자극 호르몬 수용체 (FSHR), 성샘자극 호르몬 수용체 (CGHR 또는 GR), CCR4, GD3, SLAMF6, SLAMF4, HIV1 외피 당단백질, HTLV1-Tax, CMV pp65, EBV-EBNA3c, KSHV K8.1, KSHV-gH, A형 인플루엔자 혈구응집소 (HA), GAD, PDL1, 구아닐릴 사이클라제 C (GCC), 데스모글레인 3 (Dsg3)에 대한 자기항체, 데스모글레인 1 (Dsg1)에 대한 자기항체, HLA, HLA-A, HLA-A2, HLA-B, HLA-C, HLA-DP, HLA-DM, HLA-DOA, HLA-DOB, HLA-DQ, HLA-DR, HLA-G, IgE, CD99, Ras G12V, 조직 인자 1 (TF1), AFP, GPRC5D, 클라우딘18.2 (CLD18A2 또는 CLDN18A.2), P-당단백질, STEAP1, Liv1, 넥틴-4, 크립토, gpA33, BST1/CD157, 낮은 전도도 염화물 채널, 및 TNT 항체에 의해 인식되는 항원 중 임의의 하나에 결합하는, 적어도 하나의 폴리뉴클레오타이드.
- 제30항에 있어서, 선택적 NF-κB 활성화제는 vFLIP K13, NEMO 돌연변이체, NEMO-융합 단백질, IKK1-S176E-S180E, IKK2-S177E-S181E, RIP, FKBPx2-RIP-ID, IKK1, FKBPx2-IKKα, IKK2, FKBPx2-IKK2, Tcl-1, MyD88-L265, 임의의 NF-κB 활성화 단백질 또는 단백질 단편, NF-κB 경로의 억제제 중 임의의 억제제, NF-κB를 선택적으로 활성화시킬 수 있는 유전자 편집 시스템, NF-κB를 선택적으로 활성화시키는 RNA 간섭 시스템 및 이들의 임의의 조합으로 이루어진 군으로부터 선택되는, 적어도 하나의 폴리뉴클레오타이드.
- 제37항에 있어서, 선택적 NF-κB 활성화제는 FKBP 도메인의 하나 이상의 카피를 갖는 융합 작제물로서 발현되는, 적어도 하나의 폴리뉴클레오타이드.
- 제35항에 있어서, 세포외 항원 특이적 도메인은 다음으로 이루어진 군으로부터 선택되는, 폴리뉴클레오타이드:
-소정의 표적 항원에 특이적인 항체 또는 그의 단편의 중쇄의 가변 영역 (vH);
-소정의 표적 항원에 특이적인 항체 또는 그의 단편의 경쇄의 가변 영역 (vL);
-소정의 표적 항원에 특이적인 단일 사슬 가변 단편 (scFv) 또는 그의 단편;
-소정의 표적 항원에 특이적인 항체 단편 (예를 들어, Fv, Fab, (Fab')2);
-소정의 표적 항원에 특이적인 단일 도메인 항체 (SDAB) 단편;
-소정의 표적 항원에 특이적인 낙타과 vHH 도메인;
-소정의 표적 항원에 특이적인 비면역글로불린 항원 결합 스캐폴드;
-소정의 표적 항원에 특이적인 수용체 또는 그의 단편;
-소정의 표적 항원에 특이적인 리간드 또는 그의 단편;
-하나 이상의 소정의 표적 항원에 특이적인 이중특이적-항체, -항체 단편, -scFV, -vHH, -SDAB, -비면역글로불린 항원 결합 스캐폴드, -수용체 또는 -리간드; 및
- 자기항원 또는 그의 단편. - 제30항 내지 제40항 중 어느 한 항의 적어도 하나의 폴리뉴클레오타이드를 포함하는 적어도 하나의 벡터.
- 제41항에 있어서, 벡터는 DNA 벡터, RNA 벡터, 플라스미드, 렌티바이러스 벡터, 아데노바이러스 벡터, AAV 벡터, 레트로바이러스 벡터, 바큘로바이러스 벡터, 슬리핑 뷰티 (sleeping beauty) 트랜스포손 벡터, 및 피기백 트랜스포손 벡터로 이루어진 군으로부터 선택되는, 적어도 하나의 벡터.
- 제30항 내지 제40항 중 어느 한 항의 적어도 하나의 재조합 폴리뉴클레오타이드를 포함하는 면역 효과기 세포 또는 줄기세포.
- 제41항의 적어도 하나의 벡터를 포함하는 면역 효과기 세포 또는 줄기세포.
- 제42항의 적어도 하나의 벡터를 포함하는 면역 효과기 세포 또는 줄기세포.
- 제41항의 적어도 하나의 벡터를 포함하는 항원 제시 세포.
- 제43항 내지 제45항 중 어느 한 항에 있어서, 면역 효과기 세포는 인간 T 세포, 인간 NKT 세포 또는 합성 T 세포, NK 세포, 또는 면역 효과기 세포를 생성할 수 있는 줄기세포이고, 임의적으로, T 세포는 디아글리세롤 키나제 (DGK) 및/또는 Ikaros 결핍 및/또는 Brd4 결핍인, 면역 효과기 세포 또는 줄기세포.
- (i) 발현 면역 세포의 수명(life span)을 연장하고, (ii) 면역 세포의 증식을 자극하고, (iii) 면역 세포에 의한 사이토카인 생성을 자극하고, (iv) 면역 세포에 의한 항원 제시를 증대시키고, (v) 아폽토시스로부터 면역 세포를 보호하기 위한 방법으로서, 선택적 NF-κB 활성화제 또는 NF-κB 특이적 자극 폴리펩타이드를 인코딩하는 폴리뉴클레오타이드로 면역 세포를 형질감염시키거나 형질전환시키는 단계를 포함하는, 방법.
- 제48항에 있어서, 선택적 NF-κB 활성화제 또는 NF-κB 특이적 자극 폴리펩타이드는 vFLIP K13, K13-opt, NEMO 돌연변이체, NEMO-융합 단백질, IKK1-S176E-S180E, IKK2-S177E-S181E, RIP, IKKα, IKKβ, Tcl-1, MyD88-L265, 임의의 NF-κB 활성화 단백질 또는 단백질 단편, NF-κB 경로의 억제제 중 임의의 억제제, 이들의 임의의 상동체 또는 변이체 및 이들의 임의의 조합으로 이루어진 군으로부터 선택되는, 방법.
- 제49항에 있어서, 선택적 NF-κB 활성화제 또는 NF-κB 특이적 자극 폴리펩타이드는 항시적 또는 유도성 방식으로 발현되는, 방법.
- 제50항에 있어서, 선택적 NF-κB 활성화제 또는 NF-κB 특이적 자극 폴리펩타이드는 T 세포와 화합물의 접촉을 통해 번역 후 제어되는, 방법.
- 제50항에 있어서, 선택적 NF-κB 활성화제 또는 NF-κB 특이적 자극 폴리펩타이드는 FKBP 도메인의 하나 이상의 카피를 갖는 융합 작제물로서 발현되는, 방법.
- 제52항에 있어서, 선택적 NF-κB 활성화제 또는 NF-κB 특이적 자극 폴리펩타이드의 활성은 FKBP 도메인의 이량체화를 유도하는 화합물의 치료 유효량의 투여에 의해 번역 후 수준에서 제어되는, 방법.
- 제51항에 있어서, 상기 화합물은 AP20187 또는 리미두시드인, 방법.
- 비천연 발생 면역 수용체-발현 면역 효과기 세포를 제조하는 방법으로서, 비천연 발생 면역 수용체가 발현되는 조건 하에서, 제41항의 적어도 하나의 벡터 또는 제29항의 적어도 하나의 재조합 폴리뉴클레오타이드를 면역 효과기 세포 또는 면역 효과기 세포를 생성할 수 있는 조혈모세포 또는 전구 세포 내에 도입시키는 단계를 포함하며, 면역 효과기 세포는 NFkB 특이적 자극 폴리펩타이드가 부재하는 CAR-T 세포와 비교하여, (i) 연장된 수명, (ii) 개선된 T 세포 증식, 및/또는 (iii) 감소된 아폽토시스를 포함하는, 방법.
- 제55항에 있어서,
a) 면역 효과기 세포의 집합을 제공하는 단계; 및
b) 상기 집합으로부터 T 조절 세포를 제거함으로써, T 조절-고갈 세포의 집합을 제공하는 단계
를 추가로 포함하고;
단계 a) 및 b)는 벡터 또는 CAR 및/또는 NFkB 특이적 자극 폴리펩타이드를 인코딩하는 재조합 폴리뉴클레오타이드를 상기 집합에 도입시키기 전에 수행되는, 방법. - 제56항에 있어서, T 조절 세포는 항-CD25 항체, 또는 항-GITR 항체를 사용하여 세포 집합으로부터 제거되는, 방법.
- 제55항에 있어서,
a) 면역 효과기 세포의 집합을 제공하는 단계; 및
b) P-당단백질 (P-gp 또는 Pgp; MDR1, ABCB1, CD243)-양성 세포를 상기 집합으로부터 다량화함(enriching)으로써, P-당단백질 (P-gp 또는 Pgp; MDR1, ABCB1, CD243)-다량화된 세포의 집합을 제공하는 단계
를 추가로 포함하고;
단계 a) 및 b)는 벡터 또는 CAR 및/또는 NFkB 특이적 자극 폴리펩타이드를 인코딩하는 재조합 폴리뉴클레오타이드의 도입 전 또는 후에 수행되는, 방법. - 제58항에 있어서, P-당단백질 양성 세포는
i) P-당단백질 특이적 항체 중 하나 또는 그의 칵테일을 사용한 면역선택 단계,
ii) P-당단백질의 기질인 하나 이상의 형광 염료, 테트라메틸로다민 메틸 에스테르 (TMRM), 아드리아마이신 (Adriamycin) 및 액티노마이신-D)로 P-당단백질이 펌프로서 활성인 조건 하에서 염색하고, 염료로 덜 염색된 세포를 다량화하는 단계,
iii) P-당단백질의 기질, 예컨대 TH9402, 2-(4,5-디브로모-6-아미노-3-이미노-3H-크산텐-9-일)-벤조산 메틸 에스테르 하이드로클로라이드, 2-(4,5-디브로모-6-아미노-3-이미노-3H-크산텐-9-일)-벤조산 에틸 에스테르 하이드로클로라이드, 2-(4,5-디브로모-6-아미노-3-이미노-3H-크산텐-9-일)-벤조산 옥틸 에스테르 하이드로클로라이드, 2-(4,5-디브로모-6-아미노-3-이미노-3H-크산텐-9-일)-벤조산 n-부틸 에스테르 하이드로클로라이드, 2-(6-에틸 아미노-3-에틸 이미노-3H-크산텐-9-일)-벤조산 n-부틸 에스테르 하이드로클로라이드, 또는 이들의 유도체 또는 이들의 조합 중 임의의 하나 이상의 광독성 화합물에 저항성인 세포의 선택 단계, 및
iv) P-당단백질의 기질, 예컨대 빈크리스틴 (vincristine), 빈블라스틴 (vinblastine), 탁솔 (taxol), 파클리탁셀 (paclitaxel), 미톡산트론 (mitoxantrone), 에토포시드 (etoposide), 아드리아마이신, 다우노루비신 (daunorubicin) 및 액티노마이신-D의 세포독성 화합물에 저항성인 세포의 선택 단계
로 이루어진 군으로부터 선택되는 방법 중 임의의 하나 이상을 사용하여 다량화되는, 방법. - RNA-조작된 세포의 집합을 생성하는 방법으로서, 시험관내 전사된 RNA 또는 RNA들 또는 합성 RNA 또는 RNA들을 세포 또는 세포의 집합 내에 도입시키는 단계를 포함하고, RNA 또는 RNA들은 제30항의 재조합 폴리뉴클레오타이드 또는 폴리뉴클레오타이드들을 포함하는, 방법.
- 대상체에서 항-질병 면역을 제공하는 방법으로서, 제43항 내지 제47항 중 어느 한 항의 면역 효과기 세포 또는 면역 효과기 세포를 생성할 수 있는 줄기세포의 유효량을 대상체에 투여하는 단계를 포함하고, 세포는 자가유래 T 세포 또는 동종이계 T 세포, 또는 자가유래 NKT 세포 또는 동종이계 NKT 세포 또는 면역 효과기 세포를 생성할 수 있는 자가유래 또는 동종이계 조혈모세포 또는 자가유래 또는 동종이계 iPSC인, 방법.
- 제61항에 있어서, 동종이계 T 세포 또는 동종이계 NKT 세포 또는 조혈모세포 또는 iPSC는 기능성 TCR 또는 기능성 HLA의 발현이 부재하거나, 그의 발현이 낮은, 방법.
- 비천연 발생 면역 수용체 및 선택적 NFkB 활성화제를 포함하는 면역 효과기 세포 또는 면역 효과기 세포를 생성할 수 있는 줄기세포를 포함하는 조성물로서, 비천연 발생 면역 수용체는 관련된 질병-관련 항원에 결합하는 항원 결합 도메인을 포함하고, 상기 질병-관련 항원은 CD5, CD19; CD123; CD22; CD30; CD171; CS-1 (CD2 하위세트 1, CRACC, SLAMF7, CD319, 및 19A24로도 지칭됨); C형 렉틴-유사 분자-1 (CLL-1 또는 CLECL1); CD33; 상피 성장 인자 수용체 변이체 III (EGFRviii); 강글리오사이드 G2 (GD2); 강글리오사이드 GD3 (aNeu5Ac(2-8)aNeu5Ac(2-3)bDGalp(l-4)bDGlcp(l-l)Cer); TNF 수용체 패밀리 구성원 B 세포 성숙 (BCMA); Tn 항원 ((Tn Ag) 또는 (GalNAcα-Ser/Thr)); 전립선-특이적 막 항원 (PSMA); 수용체 티로신 키나제-유사 고아 수용체 1 (ROR1); FmsLike 티로신 키나제 3 (FLT3); 종양-관련 당단백질 72 (TAG72); CD38; CD44v6; 조혈 전구체 상이 아닌 급성 백혈병 또는 림프종 상에 발현되는 글리코실화된 CD43 에피토프, 비 조혈암 상에 발현되는 글리코실화된 CD43 에피토프, 종양태아성 항원 (CEA); 상피 세포 부착 분자 (EPCAM); B7H3 (CD276); KIT (CD117); 인터루킨-13 수용체 하위단위 알파-2 (IL-13Ra2 또는 CD213A2); 메소텔린; 인터루킨 11 수용체 알파 (IL-llRa); 전립선 줄기세포 항원 (PSCA); 세린 프로테아제 21 (테스티신 또는 PRSS21); 혈관내피 성장 인자 수용체 2 (VEGFR2); 루이스(Y) 항원; CD24; 혈소판 유래 성장 인자 수용체 베타 (PDGFR-베타); 단계-특이적 배아 항원-4 (SSEA-4); CD20; 엽산 수용체 알파; 수용체 티로신-단백질 키나제 ERBB2 (Her2/neu); 뮤신 1, 세포 표면 결합 (MUC1); 상피 성장 인자 수용체 (EGFR); 신경 세포 부착 분자 (NCAM); 프로스타제; 전립선 산성 포스파타제 (PAP); 돌연변이 연장 인자 2 (ELF2M); 에프린 B2; 섬유아세포 활성화 단백질 알파 (FAP); 인슐린-유사 성장 인자 1 수용체 (IGF-I 수용체), 탄산무수화효소 IX (CAlX); 프로테아좀 (프로좀, 마크로파인) 하위단위, 베타 유형, 9 (LMP2); 당단백질 100 (gpl00); 중단점 클러스터 영역 (BCR) 및 아벨슨 쥣과동물 백혈병 바이러스 암유전자 상동체 1 (Abl) (bcr-abl)로 이루어진 암유전자 융합 단백질; 티로시나제; 에프린 유형-A 수용체 2 (EphA2); 푸코실 GM1; 시알릴 루이스 부착 분자 (sLe); 강글리오사이드 GM3 (aNeu5Ac(2-3)bDClalp(l-4)bDGlcp(l-1)Cer); 트랜스글루타미나제 5 (TGS5); 고분자량-흑색종관련 항원 (HMWMAA); o-아세틸-GD2 강글리오사이드 (OAcGD2); 종양 내피 마커 1 (TEM1/CD248); 종양 내피 마커 7-관련 (TEM7R); 클라우딘 6 (CLDN6); 갑상선 자극 호르몬 수용체 (TSHR); G 단백질 연결 수용체 클래스 C 그룹 5, 구성원 D (GPRC5D); 염색체 X 오픈 리딩 프레임 61 (CXORF61); CD97; CD179a; 역형성 림프종 키나제 (ALK); 폴리시알산; 태반-특이적 1 (PLAC1); globoH 글리코세라마이드 (GloboH)의 육당류 부분; 포유류 샘 분화 항원 (NY-BR-1); 유로플라킨 2 (UPK2); A형 간염 바이러스 세포 수용체 1 (HAVCR1); 아드레날린수용체 베타 3 (ADRB3); 파넥신 3 (PANX3); G 단백질 연결 수용체 20 (GPR20); 림프구 항원 6 복합체, 좌위 K 9 (LY6K); 후각 수용체 51E2 (OR51E2); TCR 감마 대체 리딩 프레임 단백질 (TARP); 빌름스 종양 단백질 (WT1); 암/고환 항원 1 (NY-ESO-1); 암/고환 항원 2 (LAGE-1a); 흑색종-관련 항원 1 (MAGE-A1); 염색체 12p에 위치한 ETS 전좌-변이체 유전자 6 (ETV6-AML); 정자 단백질 17 (SPA17); X 항원 패밀리, 구성원 lA (XAGEl); 안지오포이에틴-결합 세포 표면 수용체 2 (Tie 2); 흑색종 고환암 항원-1 (MAD-CT-1); 흑색종 고환암 항원-2 (MAD-CT-2); Fos-관련 항원 1; 종양 단백질 p53 (p53); p53 돌연변이체; 프로스테인; 서바이빙 (surviving); 텔로머라제; 전립선 암종 종양 항원-1 (PCT A-1 또는 갈렉틴 8), T 세포 1에 의해 인식되는 흑색종 항원 (MelanA 또는 MARTI); 랫트 육종 (Ras) 돌연변이체; 인간 텔로머라제 역전사효소 (hTERT); 육종 전좌 중단점; 아폽토시스의 흑색종 억제제 (ML-IAP); ERG (막관통 프로테아제, 세린 2 (TMPRSS2) ETS 융합 유전자); N-아세틸 글루코사미닐-트랜스퍼라제 V (NA17); 쌍 형성 box 단백질 Pax-3 (PAX3); 안드로겐 수용체; 사이클린 Bl; v-myc 조류 골수세포증 바이러스 암유전자 신경아세포 유래 상동체 (MYCN); Ras 상동체 패밀리 구성원 C (RhoC); 티로시나제-관련 단백질 2 (TRP-2); 시토크롬 P450 lB 1 (CYPlB 1); CCCTC-결합 인자 (아연 핑거 단백질)-유사 (BORIS 또는 Brother of the Regulator oflmprinted Sites), T 세포 3에 의해 인식되는 편평 세포 암종 항원 (SART3); 쌍 형성 box 단백질 Pax-5 (PAX5); 프로아크로신 결합 단백질 sp32 (OY-TESl); 림프구-특이적 단백질 티로신 키나제 (LCK); A 키나제 고정 단백질 4 (AKAP-4); 활액 육종, X 중단점 2 (SSX2); 진행된 최종 당화 산물의 수용체 (RAGE-1); 신장 산재 인자 1 (RUl); 신장 산재 인자 2 (RU2); 레구메인; 인간 유두종 바이러스 E6 (HPV E6); 인간 유두종 바이러스 E7 (HPV E7); 장내 카복실 에스테라제; 돌연변이 열 충격 단백질 70-2 (mut hsp70-2); CD79a; CD79b; CD72; 백혈구-관련 면역글로불린-유사 수용체 1 (LAIRl); IgA 수용체의 Fc 단편 (FCAR 또는 CD89); 백혈구 면역글로불린-유사 수용체 서브패밀리 A 구성원 2 (LILRA2); CD300 분자-유사 패밀리 구성원 f (CD300LF); C형 렉틴 도메인 패밀리 12 구성원 A (CLEC12A); 골수 기질 세포 항원 2 (BST2); EGF-유사 모듈-포함 뮤신-유사 호르몬 수용체-유사 2 (EMR2); 림프구 항원 75 (LY75); 글리피칸-3 (GPC3); Fc 수용체-유사 5 (FCRL5); 및 면역글로불린 람다-유사 폴리펩타이드 1 (IGLLl), MPL, 비오틴, c-MYC 에피토프 Tag, CD34, LAMP1 TROP2, GFR알파4, CDH17, CDH6, NYBR1, CDH19, CD200R, Slea (CA19.9; 시알릴 루이스 항원) 푸코실-GM1, PTK7, gpNMB, CDH1-CD324, DLL3, CD276/B7H3, IL11Ra, IL13Ra2, CD179b-IGLl1, ALK TCR감마-델타, NKG2D, CD32 (FCGR2A), CSPG4-HMW-MAA, Tim1-/HVCR1, CSF2RA (GM-CSFR-알파), TGF베타R2, VEGFR2/KDR, Lews Ag, TCR-베타1 사슬, TCR-베타2 사슬, TCR-감마 사슬, TCR-델타 사슬, FITC, 황체형성 호르몬 수용체 (LHR), 여포 자극 호르몬 수용체 (FSHR), 융모막 성샘자극 호르몬 수용체 (CGHR), CCR4, SLAMF6, SLAMF4, HIV1 외피 당단백질, HTLV1-Tax, CMV pp65, EBV-EBNA3c, A형 인플루엔자 혈구응집소 (HA), GAD, PDL1, 구아닐릴 사이클라제 C (GCC), KSHV-K8.1 단백질, KSHV-gH 단백질, 데스모글레인 3에 대한 자기항체 (Dsg3), 데스모글레인 1에 대한 자기항체 (Dsg1), HLA, HLA-A, HLA-A2, HLA-B, HLA-C, HLA-DP, HLA-DM, HLA-DOA, HLA-DOB, HLA-DQ, HLA-DR, HLA-G, IGE, CD99, RAS G12V, 조직 인자 1 (TF1), AFP, GPRC5D, 클라우딘18.2 (CLD18A2 또는 CLDN18A.2)), P-당단백질, STEAP1, LIV1, 넥틴-4, 크립토, GPA33, BST1/CD157, 낮은 전도도 염화물 채널, 및 TNT 항체에 의해 인식되는 항원으로 이루어진 군으로부터 선택되는, 조성물.
- 대상체에서 질병-관련 항원의 발현과 관련된 질병을 치료하거나 예방하는 방법으로서, 비천연 발생 면역 수용체 및 선택적 NFkB 활성화제를 포함하는 면역 효과기 세포의 유효량을 대상체에 투여함으로써, 대상체를 치료하거나, 대상체에서 질병을 예방하는 단계를 포함하고, 비천연 발생 면역 수용체는 관련된 질병-관련 항원에 결합하는 항원 결합 도메인을 포함하고, 상기 질병-관련 항원은 CD5, CD19; CD123; CD22; CD30; CD171; CS-1 (CD2 하위세트 1, CRACC, SLAMF7, CD319, 및 19A24로도 지칭됨); C형 렉틴-유사 분자-1 (CLL-1 또는 CLECL1); CD33; 상피 성장 인자 수용체 변이체 III (EGFRviii); 강글리오사이드 G2 (GD2); 강글리오사이드 GD3 (aNeu5Ac(2-8)aNeu5Ac(2-3)bDGalp(l-4)bDGlcp(l-l)Cer); TNF 수용체 패밀리 구성원 B 세포 성숙 (BCMA); Tn 항원 ((Tn Ag) 또는 (GalNAcα-Ser/Thr)); 전립선-특이적 막 항원 (PSMA); 수용체 티로신 키나제-유사 고아 수용체 1 (ROR1); FmsLike 티로신 키나제 3 (FLT3); 종양-관련 당단백질 72 (TAG72); CD38; CD44v6; 조혈 전구체 상이 아닌 급성 백혈병 또는 림프종 상에 발현되는 글리코실화된 CD43 에피토프, 비 조혈암 상에 발현되는 글리코실화된 CD43 에피토프, 종양태아성 항원 (CEA); 상피 세포 부착 분자 (EPCAM); B7H3 (CD276); KIT (CD117); 인터루킨-13 수용체 하위단위 알파-2 (IL-13Ra2 또는 CD213A2); 메소텔린; 인터루킨 11 수용체 알파 (IL-llRa); 전립선 줄기세포 항원 (PSCA); 세린 프로테아제 21 (테스티신 또는 PRSS21); 혈관내피 성장 인자 수용체 2 (VEGFR2); 루이스(Y) 항원; CD24; 혈소판 유래 성장 인자 수용체 베타 (PDGFR-베타); 단계-특이적 배아 항원-4 (SSEA-4); CD20; 엽산 수용체 알파; 수용체 티로신-단백질 키나제 ERBB2 (Her2/neu); 뮤신 1, 세포 표면 결합 (MUC1); 상피 성장 인자 수용체 (EGFR); 신경 세포 부착 분자 (NCAM); 프로스타제; 전립선 산성 포스파타제 (PAP); 돌연변이 연장 인자 2 (ELF2M); 에프린 B2; 섬유아세포 활성화 단백질 알파 (FAP); 인슐린-유사 성장 인자 1 수용체 (IGF-I 수용체), 탄산무수화효소 IX (CAlX); 프로테아좀 (프로좀, 마크로파인) 하위단위, 베타 유형, 9 (LMP2); 당단백질 100 (gpl00); 중단점 클러스터 영역 (BCR) 및 아벨슨 쥣과동물 백혈병 바이러스 암유전자 상동체 1 (Abl) (bcr-abl)로 이루어진 암유전자 융합 단백질; 티로시나제; 에프린 유형-A 수용체 2 (EphA2); 푸코실 GM1; 시알릴 루이스 부착 분자 (sLe); 강글리오사이드 GM3 (aNeu5Ac(2-3)bDClalp(l-4)bDGlcp(l-1)Cer); 트랜스글루타미나제 5 (TGS5); 고분자량-흑색종관련 항원 (HMWMAA); o-아세틸-GD2 강글리오사이드 (OAcGD2); 종양 내피 마커 1 (TEM1/CD248); 종양 내피 마커 7-관련 (TEM7R); 클라우딘 6 (CLDN6); 갑상선 자극 호르몬 수용체 (TSHR); G 단백질 연결 수용체 클래스 C 그룹 5, 구성원 D (GPRC5D); 염색체 X 오픈 리딩 프레임 61 (CXORF61); CD97; CD179a; 역형성 림프종 키나제 (ALK); 폴리시알산; 태반-특이적 1 (PLAC1); globoH 글리코세라마이드 (GloboH)의 육당류 부분; 포유류 샘 분화 항원 (NY-BR-1); 유로플라킨 2 (UPK2); A형 간염 바이러스 세포 수용체 1 (HAVCR1); 아드레날린수용체 베타 3 (ADRB3); 파넥신 3 (PANX3); G 단백질 연결 수용체 20 (GPR20); 림프구 항원 6 복합체, 좌위 K 9 (LY6K); 후각 수용체 51E2 (OR51E2); TCR 감마 대체 리딩 프레임 단백질 (TARP); 빌름스 종양 단백질 (WT1); 암/고환 항원 1 (NY-ESO-1); 암/고환 항원 2 (LAGE-1a); 흑색종-관련 항원 1 (MAGE-A1); 염색체 12p에 위치한 ETS 전좌-변이체 유전자 6 (ETV6-AML); 정자 단백질 17 (SPA17); X 항원 패밀리, 구성원 lA (XAGEl); 안지오포이에틴-결합 세포 표면 수용체 2 (Tie 2); 흑색종 고환암 항원-1 (MAD-CT-1); 흑색종 고환암 항원-2 (MAD-CT-2); Fos-관련 항원 1; 종양 단백질 p53 (p53); p53 돌연변이체; 프로스테인; 서바이빙; 텔로머라제; 전립선 암종 종양 항원-1 (PCT A-1 또는 갈렉틴 8), T 세포 1에 의해 인식되는 흑색종 항원 (MelanA 또는 MARTI); 랫트 육종 (Ras) 돌연변이체; 인간 텔로머라제 역전사효소 (hTERT); 육종 전좌 중단점; 아폽토시스의 흑색종 억제제 (ML-IAP); ERG (막관통 프로테아제, 세린 2 (TMPRSS2) ETS 융합 유전자); N-아세틸 글루코사미닐-트랜스퍼라제 V (NA17); 쌍 형성 box 단백질 Pax-3 (PAX3); 안드로겐 수용체; 사이클린 Bl; v-myc 조류 골수세포증 바이러스 암유전자 신경아세포 유래 상동체 (MYCN); Ras 상동체 패밀리 구성원 C (RhoC); 티로시나제-관련 단백질 2 (TRP-2); 시토크롬 P450 lB 1 (CYPlB 1); CCCTC-결합 인자 (아연 핑거 단백질)-유사 (BORIS 또는 Brother of the Regulator oflmprinted Sites), T 세포 3에 의해 인식되는 편평 세포 암종 항원 (SART3); 쌍 형성 box 단백질 Pax-5 (PAX5); 프로아크로신 결합 단백질 sp32 (OY-TESl); 림프구-특이적 단백질 티로신 키나제 (LCK); A 키나제 고정 단백질 4 (AKAP-4); 활액 육종, X 중단점 2 (SSX2); 진행된 최종 당화 산물의 수용체 (RAGE-1); 신장 산재 인자 1 (RUl); 신장 산재 인자 2 (RU2); 레구메인; 인간 유두종 바이러스 E6 (HPV E6); 인간 유두종 바이러스 E7 (HPV E7); 장내 카복실 에스테라제; 돌연변이 열 충격 단백질 70-2 (mut hsp70-2); CD79a; CD79b; CD72; 백혈구-관련 면역글로불린-유사 수용체 1 (LAIRl); IgA 수용체의 Fc 단편 (FCAR 또는 CD89); 백혈구 면역글로불린-유사 수용체 서브패밀리 A 구성원 2 (LILRA2); CD300 분자-유사 패밀리 구성원 f (CD300LF); C형 렉틴 도메인 패밀리 12 구성원 A (CLEC12A); 골수 기질 세포 항원 2 (BST2); EGF-유사 모듈-포함 뮤신-유사 호르몬 수용체-유사 2 (EMR2); 림프구 항원 75 (LY75); 글리피칸-3 (GPC3); Fc 수용체-유사 5 (FCRL5); 및 면역글로불린 람다-유사 폴리펩타이드 1 (IGLLl), MPL, 비오틴, c-MYC 에피토프 Tag, CD34, LAMP1 TROP2, GFR알파4, CDH17, CDH6, NYBR1, CDH19, CD200R, Slea (CA19.9; 시알릴 루이스 항원) 푸코실-GM1, PTK7, gpNMB, CDH1-CD324, DLL3, CD276/B7H3, IL11Ra, IL13Ra2, CD179b-IGLl1, ALK TCR감마-델타, NKG2D, CD32 (FCGR2A), CSPG4-HMW-MAA, Tim1-/HVCR1, CSF2RA (GM-CSFR-알파), TGF베타R2, VEGFR2/KDR, Lews Ag, TCR-베타1 사슬, TCR-베타2 사슬, TCR-감마 사슬, TCR-델타 사슬, FITC, 황체형성 호르몬 수용체 (LHR), 여포 자극 호르몬 수용체 (FSHR), 융모막 성샘자극 호르몬 수용체 (CGHR), CCR4, SLAMF6, SLAMF4, HIV1 외피 당단백질, HTLV1-Tax, CMV pp65, EBV-EBNA3c, A형 인플루엔자 혈구응집소 (HA), GAD, PDL1, 구아닐릴 사이클라제 C (GCC), KSHV-K8.1 단백질, KSHV-gH 단백질, 데스모글레인 3에 대한 자기항체 (Dsg3), 데스모글레인 1에 대한 자기항체 (Dsg1), HLA, HLA-A, HLA-A2, HLA-B, HLA-C, HLA-DP, HLA-DM, HLA-DOA, HLA-DOB, HLA-DQ, HLA-DR, HLA-G, IGE, CD99, RAS G12V, 조직 인자 1 (TF1), AFP, GPRC5D, 클라우딘18.2 (CLD18A2 또는 CLDN18A.2)), P-당단백질, STEAP1, LIV1, 넥틴-4, 크립토, GPA33, BST1/CD157, 낮은 전도도 염화물 채널, 및 TNT 항체에 의해 인식되는 항원으로 이루어진 군으로부터 선택되는, 방법.
- 제63항 또는 제64항에 있어서, 질병 관련 항원의 발현과 관련된 질병은 증식성 질병, 전암성 병태, 암, 및 질병 관련 항원의 발현과 관련된 비 암 관련 적응증으로 이루어진 군으로부터 선택되는, 용도 또는 방법.
- 제65항에 있어서, 암은 만성 림프구성 백혈병 (CLL), 급성 백혈병, 급성 림프성 백혈병 (ALL), B 세포 급성 림프성 백혈병 (B-ALL), T 세포 급성 림프성 백혈병 (T-ALL), 만성 골수성 백혈병 (CML), B 세포 전림프구성 백혈병, 아구성 형질세포양 수지상 세포 신생물, 버킷 림프종 (Burkitt's lymphoma), 미만성 거대 B 세포 림프종, 1차 삼출 림프종, 여포성 림프종, 모세포 백혈병, 소세포 또는 거대 세포 여포성 림프종, 악성 림프 증식성 병태, MALT 림프종, 외투 세포 림프종, 변연부 림프종, 다발성 골수종, 골수이형성 및 골수이형성 증후군, 비호지킨 림프종 (non-Hodgkin's lymphoma), 호지킨 림프종, 형질모세포성 림프종, 형질세포양 수지상 세포 신생물, 왈덴스트룀 마크로글로불린혈증 (Waldenstrom macroglobulinemia), 또는 백혈병 전증 중 하나 이상으로부터 선택되는 혈액암인, 용도 또는 방법.
- 제65항에 있어서, 암은 결장암, 직장 암, 신장 세포 암종, 간 암, 폐의 비소세포 암종, 소장암, 식도암, 흑색종, 골암, 췌장암, 피부 암, 두경부암, 피부 또는 안내 악성 흑색종, 자궁 암, 난소 암, 직장 암, 항문 영역의 암, 위 암, 고환 암, 자궁 암, 자궁관암, 자궁내막 암종, 자궁경부 암종, 질 암종, 외음부 암종, 호지킨 질병, 비호지킨 림프종, 내분비계암, 갑상선암, 부갑상선암, 부신암, 연조직 육종, 요도암, 음경암, 소아 고형 종양, 방광암, 신장 또는 요관의 암, 신우 암종, 중추신경계 (CNS)의 신생물, 1차 CNS 림프종, 혈관신생 종양, 척추 종양, 뇌줄기신경아교종, 뇌하수체선종, 카포시 육종, 메르켈세포암 (Merkel cell cancer), 표피암, 편평 세포 암, T 세포 림프종, 환경 유발 암, 상기 암의 조합, 및 상기 암의 전이성 병변으로 이루어진 군으로부터 선택되는, 용도 또는 방법.
- 제65항에 있어서, 질병은 다음에 제한되는 것은 아니나, HIV1, HIV2, HTLV1, 엡스타인 바르 바이러스 (EBV), 사이토메갈로바이러스 (CMV), 아데노바이러스, 아데노-관련 바이러스, BK 바이러스, 인간 포진바이러스 6, 인간 포진바이러스 8 인플루엔자 바이러스, 파라인플루엔자 바이러스, 조류 독감 바이러스, MERS 및 SARS 코로나바이러스, 크림 반도 콩고 유행성 출혈열 바이러스, 리노 바이러스, 엔테로바이러스, 뎅기열 바이러스, 웨스트 나일 바이러스, 에볼라 바이러스, 마르부르크 바이러스, 랏사열 바이러스, 지카 바이러스, RSV, 홍역 바이러스, 유행성 이하선염 바이러스, 리노 바이러스, 수두 바이러스, 단순 포진 바이러스 1 및 2, 수두 대상포진 바이러스, HIV-1, HTLV1, 간염 바이러스, 엔테로바이러스, B형 간염 바이러스, C형 간염 바이러스, 니파 및 리프트밸리열 바이러스, 일본뇌염 바이러스, 메르켈 세포 폴리오마바이러스를 포함하는 바이러스에 의한 감염과 관련되거나, 결핵균, 비정형 마이코박테리아 종, 폐포자충, 톡소포자충증, 리케차, 노카르디아, 아스페르길루스, 무코르, 또는 칸디다에 의한 감염과 관련되는, 용도 또는 방법.
- 제65항에 있어서, 질병은 다음에 제한되는 것은 아니나, 진성 당뇨병, 다발성 경화증, 류머티스 관절염, 심상성천포창, 강직성 척추염, 하시모토 갑상선염, SLE, 사르코이드증, 피부경화증, 혼합결합조직병, 이식편대숙주병 또는 알츠하이머병을 포함하는 면역 또는 퇴행성 질병인, 용도 또는 방법.
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CN (1) | CN111629734A (ko) |
AU (1) | AU2018338647A1 (ko) |
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EA (1) | EA202090839A1 (ko) |
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Cited By (1)
Publication number | Priority date | Publication date | Assignee | Title |
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KR20230120362A (ko) | 2022-02-09 | 2023-08-17 | 한림대학교 산학협력단 | 항-cd20을 포함하는 키메릭 항원 수용체를 유효성분으로 포함하는 암의 예방 또는 치료용 약학적 조성물 및 이의 제조 방법 |
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IL273201A (en) | 2020-04-30 |
JP2021500861A (ja) | 2021-01-14 |
AU2018338647A1 (en) | 2020-05-07 |
JP2023145589A (ja) | 2023-10-11 |
EA202090839A1 (ru) | 2021-02-04 |
CA3075806A1 (en) | 2019-04-04 |
ZA202205717B (en) | 2024-05-30 |
MX2020004185A (es) | 2021-01-08 |
CN111629734A (zh) | 2020-09-04 |
BR112020005938A2 (pt) | 2020-11-17 |
SG11202002321YA (en) | 2020-04-29 |
EP3687553A1 (en) | 2020-08-05 |
US20230140802A1 (en) | 2023-05-04 |
WO2019067805A1 (en) | 2019-04-04 |
EP3687553A4 (en) | 2022-01-05 |
ZA202002046B (en) | 2022-10-26 |
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