KR20120025014A - 신경 및 뇌 종양에 대한 신규 면역요법 - Google Patents
신경 및 뇌 종양에 대한 신규 면역요법 Download PDFInfo
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Abstract
Description
도 1a 및 1b는 교모 세포종 표본 GB1006에서 종양 관련 펩티드 (TUMAPs) TP-001을 및 교모 세포종 표본 GB6003에서 PTP-002를 식별하는 ESI-액체 크로마토그래피 질량 스펙트럼을 보여준다.
[도 2]
도 2는 표 1에 나와 있는 교모 세포종 관련 펩티드 유전자 PTPRZ1의 mRNA 발현 프로필을 나타낸 것이다. 이 유전자의 발현은 정상 조직에서는 완전히 없거나 또는 아주 낮은 데에 비해 교모 세포종 표본에서는 강하게 증가되어 나타난다 (GB1006T에서 GB1011T; NCH359T와 NCH361T).
[도 3]
도 3은 유식세포분석에 의해 결정된 PTP-002에 의한 시험관내 자극 후의 건강한 HLA-A*0201 기증의 PTP-002-특정 CD8 양성 T 세포 대표적인 예를 보여준다. CD8 양성 T 세포는 건강한 기증 인간 PBMC에서 단리되고 시험관내에서 분자적으로 정의된 공동-자극 분자와 A*0201/PTP-002 (좌측 도면) 또는 비관련 A*0201 펩티드 (우측 도면)이 적재되어 있는 "인공 항원 제시 세포"(aAPC)를 사용하여 프라임된다 (Walter et al., 2003). 3번의 자극 싸이클을 거친 후, 펩티드-반응 세포의 탐지는 PTP-002-플러스 비관련 펩티드 테트라머로 염색을 하여 이루어진다. 세포는 CD8 양성 림프구 집단에 게이트되었고 (gated) 비율은 이 집단 중에서 테트라머-양성 세포의 빈도를 나타낸다.
[도 4]
도 4는 본 발명의 펩티드와 HLA-A*2010의 친화력을 나타낸다. HLA 클래스 I 펩티드와 바이러스 마커 펩티드 HBV-001의 해리 상수 (KD)는 ELISA 기반 분석에 의해 측정된다 (실시예 4 참조).
Claims (16)
- 서열번호 5의 서열 또는 이의 변이체를 포함하는 펩티드로서, 상기 펩티드가 전장 PTPRZ1(단백질 타이로신 포스파타아제 수용체-타입 제타1) 폴리펩티드가 아니고, 상기 변이체가 서열번호 5의 아미노산 서열에서,
i) 두번째 아미노산 잔기가 메싸이오닌, 아홉번째 아미노산 잔기가 류신으로 치환된 변이체;
ii) 두번째 아미노산 잔기가 류신, 아홉번째 아미노산 잔기가 류신으로 치환된 변이체;
iii) 네번째 아미노산 잔기가 글루탐산, 여덟번째 아미노산 잔기가 라이신으로 치환된 변이체;
iv) 첫번째 아미노산 잔기가 아이소류신, 세번째 아미노산 잔기가 알라닌, 네번째 아미노산 잔기가 글라이신, 다섯번째 아미노산 잔기가 아이소류신, 일곱번째 아미노산 잔기가 알라닌, 여덟번째 아미노산 잔기가 글루탐산으로 치환된 변이체;
v) 첫번째 아미노산 잔기가 류신, 세번째 아미노산 잔기가 타이로신, 네번째 아미노산 잔기가 프롤린, 다섯번째 아미노산 잔기가 라이신, 여섯번째 아미노산 잔기가 류신, 일곱번째 아미노산 잔기가 타이로신으로 치환된 변이체;
vi) 첫번째 아미노산 잔기가 페닐알라닌, 세번째 아미노산 잔기가 프롤린, 네번째 아미노산 잔기가 쓰레오닌, 다섯번째 아미노산 잔기가 타이로신, 여섯번째 아미노산 잔기가 쓰레오닌, 일곱번째 아미노산 잔기가 히스티딘으로 치환된 변이체;
vii) 첫번째 아미노산 잔기가 메싸이오닌, 세번째 아미노산 잔기가 메싸이오닌, 다섯번째 아미노산 잔기가 아스파라긴으로 치환된 변이체;
viii) 첫번째 아미노산 잔기가 타이로신, 세번째 아미노산 잔기가 세린, 다섯번째 아미노산 잔기가 페닐 알라닌으로 치환된 변이체; 및
ix) 다섯 번째 아미노산 잔기가 발린으로 치환된 변이체로 이루어진 군으로부터 선택되는 것인 펩티드. - 제1항에 있어서,
인간 주요 조직 적합 유전자 복합체(MHC) 클래스 I 또는 클래스 II의 분자와 결합하는 능력을 유지하며 CD4 또는 CD8 T 세포를 자극할 수 있는 펩티드. - 제1항에 있어서,
아미노산 서열이 서열번호 1 내지 11에 따른 연속 아미노산 스트레치를 포함하는 펩티드. - 제1항에 있어서,
전체 길이가 8 내지 100개의 아미노산인 펩티드. - 제1항에 있어서,
-CH2-NH, -CH2S-, -CH2CH2-, -CH=CH-, -COCH2-, -CH(OH)CH2- 및 -CH2SO-로 이루어진 군으로부터 선택되는 비펩티드 결합을 포함하는 펩티드. - 제1항에 있어서,
HLA(인간 백혈구 항원)-DR 항원-관련 불변 쇄(Ii)의 N-말단 아미노산 80개를 포함하는 융합 단백질인 펩티드. - 제1항에 따른 펩티드를 코딩하는 핵산.
- 제7항에 따른 핵산을 발현할 수 있는 발현 벡터.
- 제7항에 따른 핵산 또는 제8항에 따른 발현 벡터를 포함하는 숙주 세포로서, 상기 숙주 세포가 항원 제시 세포인 숙주 세포.
- 펩티드를 제조하는 방법으로서,
제9항에 따른 숙주 세포를 배양하는 단계, 및
상기 숙주 세포 또는 이의 배양 배지로부터 상기 펩티드를 단리하는 단계
를 포함하는 방법. - 시험관 내에서 세포독성 T 림프구(CTL)와, 항원 제시 세포 또는 인공 항원 제시 세포의 표면 상에 발현된 항원-적재된 인간 MHC 클래스 I 또는 클래스 II 분자를 접촉시키는 단계를 포함하는 활성화된 CTL을 시험관내에서 제조하는 방법으로서, 상기 항원이 제1항 내지 제6항 중 어느 한 항에 따른 펩티드인, 방법.
- 제11항에 따른 방법에 의해 제조된 활성화된 CTL.
- 유효한 수의 제12항에 정의된 CTL 및 약제학적으로 허용가능한 부형제를 포함하는 암세포를 사멸시키기 위한 약제학적 조성물.
- 제1항 내지 제6항 중 어느 한 항에 따른 펩티드, 제7항에 따른 핵산 또는 제8항에 따른 발현 벡터를 포함하는 암의 치료 또는 예방용 약제학적 조성물.
- 제14항에 있어서,
백신으로서 사용되는 약제학적 조성물. - 제14항에 있어서,
상기 암이 성상세포종, 털모양 성상세포종, 배아형성장애 신경상피 종양, 희소돌기아교세포종, 뇌실막세포종, 다형성아교모세포종, 혼합된 신경아교종, 희소돌기성상세포종, 속질모세포종, 망막모세포종, 신경모세포종, 배아종, 기형종, 신경절교종, 신경절세포종, 중추 신경절세포종, 원시 신경 외배엽 종양, 송과체실질 종양, 뇌실막세포 종양, 맥락막망 종양, 기원이 불확실한 신경상피 종양, 신경아교모세포종, 폐암 및 선편평상피 암종으로 구성된 군에서 선택되는 약제학적 조성물.
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