KR20130084332A - 아밀로이드 베타 단백질에 대한 모노클로날 항체 및 이의 용도 - Google Patents
아밀로이드 베타 단백질에 대한 모노클로날 항체 및 이의 용도 Download PDFInfo
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Abstract
Description
도 2는 원섬유-결합된 중쇄 및 경쇄 항체 (4, 6, 8번 레인(lane)) 및 상청액 중의 상응하는 비-결합된 유리 분획 (3, 5, 7번 레인)의 SDS-PAGE 분석을 보여준다.
도 3은 경증 인지 장애 (MCI, 상단) 또는 알츠하이머병 (AD, 하단) 환자로부터의 CSF 샘플 중의 Aβ42 및 Aβ40의 함량을 보여준다. 두 그룹에서, 표준 항체 6E10과 비교하거나, 또는 동일한 ELISA를 사용한 직접적인 샘플 분석과 비교하면, 8F5를 사용한 경우에는, Aβ(l-42)는 더 많은 양이 검출되고, Aβ(l-40)은 동일하거나 더 적은 양이 검출된다는 것을 관찰할 수 있다.
도 4는 세 그룹의 APP 유전자전이된(transgenic) 마우스 (즉, 6G1, 8F5, PBS) 및 한 그룹의 유전자 비-전이된 동복자(littermate) (야생형)에서, 미지의 물체 대 익숙한 물체의 경우 걸리는 시간에 따른 신규 물체 인지 지수(novel object recognition index)를 보여준다. 상기 동물을 (그룹당 마릿수는 그래프 아래에 제시됨) 3주 동안 매주 1회 복강내로 주사하여 모노클로날 항체 6G1 또는 8F5로 면역화시키거나 비히클 (즉, 인산염 완충 식염수; PBS, 및 야생형)로 처리하였다. 마지막으로 주사하는 날에, 신규 물체 인지 과제를 수행하였다. 본 패러다임에서 PBS 그룹과 야생형 그룹 간의 차이는 APP 유전자전이된 마우스의 인지 결핍을 나타내었다. PBS를 주사한 마우스의 수행능력은 우연 수준(chance level)이었지만 (즉, 50과 유의적인 차이가 없음), 모든 다른 마우스는 물체 인지를 보였다 (t-검정; *). 항체를 처리한 APP 유전자전이된 마우스의 수행능력을 대조군 그룹과 비교하면, PBS를 처리한 마우스에 대해서는 유의적인 차이가 나타났지만, 야생형 마우스에 대해서는 유의적인 차이가 나타나지 않아 (ANOVA 및 사후 t-검정(post-hoc t-test); ○), 항체 처리는 상기 APP 유전자전이된 마우스에서 인지 결핍을 회복시킨 것으로 나타났다.
도 5(A)는 본원에서 "8F5"라고 하는 모노클로날 항체를 암호화하는 가변 중쇄의 DNA 서열 (서열번호 1)을 나타내고, 도 5(B)는 모노클로날 항체 8F5를 암호화하는 가변 경쇄의 DNA 서열 (서열번호 2)을 나타낸다 (각각의 서열에서 상보성 결정 영역(CDR)이 밑줄로 표시되어 있다; 도 6을 참조한다).
도 6(A)는 모노클로날 항체 8F5의 가변 중쇄의 아미노산 서열 (서열번호 3)을 나타내고, 도 6(B)는 모노클로날 항체 8F5의 가변 경쇄의 아미노산 서열 (서열번호 4)을 나타낸다. 가변 중쇄의 하나의 CDR은 아미노산 서열 SYGMS (서열번호 5)로 표시된다. 가변 중쇄의 다른 CDR은 아미노산 서열 ASINSNGGSTYYPDSVKG (서열번호 6)으로 표시되고, 가변 중쇄의 또다른 CDR은 아미노산 서열 SGDY (서열번호 7)로 표시된다. 가변 경쇄의 하나의 CDR은 아미노산 서열 RSSQSLVYSNGDTYLH (서열번호 8)로 표시된다. 가변 경쇄의 다른 CDR은 아미노산 서열 KVSNRFS (서열번호 9)로 표시되고, 가변 경쇄의 또다른 CDR은 아미노산 서열 SQSTHVPWT (서열번호 10)으로 표시된다. 모든 상기 CDR은 도 6(A) 및 6(B)에서 밑줄로 표시되어 있다.
도 7은 상이한 농도에서 알츠하이머병(AD) 환자 또는 고령의 APP 유전자전이된 마우스의 신피질의 횡절편에 대한 항체의 결합을 보여준다. 특히, 도 7(A)는 APP 유전자전이된 마우스 계통 Tg2576 및 AD 환자(RZ55)에서, 아밀로이드 침착물이 콩고레드(Congo Red) 염색에 의해 뇌 조직 내의 플라크 및 뇌 혈관 내의 뇌 아밀로이드 혈관병증(CAA)으로서 확인됨을 보여준다. 도 7(B)는 AD 환자(RZ16)에서 6G1 및 시판되는 항체인 6E10으로만 Aβ(아밀로이드 플라크)의 실질조직 침착물이 염색되고, 8F5 및 8C5로는 상당히 약하게 염색된다는 것을 보여준다. 도 7(C)는 TG2576 마우스에서 6G1 및 시판되는 항체인 6E10으로만 Aβ(아밀로이드 플라크)의 실질조직 침착물이 강하게 염색되고, 8F5 및 8C5로는 상당히 약하게 염색된다는 것을 보여준다. 도 7(D) 내지 (G)는 조직학적 이미지에서 이미지 분석을 사용한 Aβ 플라크 염색의 정량 분석을 보여준다. 광학밀도 값(0% = 염색되지 않음)은 {플라크의 그레이 스케일(gray scale) 값} - {배경 조직의 그레이 스케일 값}으로 계산하였다 (도 7(D) = Tg2576 마우스에서 0.7㎍/ml 항체의 결합; 도 7(E) = APP/L 마우스에서 0.07 내지 0.7㎍/ml 항체의 결합; 도 7(F)는 AD 환자(RZ55)에서 0.7㎍/ml 항체의 결합; 및 도 7(G) = AD 환자(RZ16)에서 0.07 내지 0.7㎍/ml 항체의 결합). 시판되는 항체인 6E10 (*) 및 4G8 (○)과 항체 6G1, 8C5 및 8F5의 염색 간의 차이를 통계적으로 평가하였다 (*/○: 대조군에 대해 p < 0.05, **/○○: p < 0.01, 및 ***/○○○: p<0.001; p<0.001로 ANOVA 분석 후에 사후 본페로니 t-검정(post-hoc Bonferroni's t-test)을 함) (도 7(D) 및 7(E)). 도 7(E) 및 7(G)에서, 항체 8C5 및 8F5는 시판되는 항체인 6E10 및 4G8보다 항상 유의적으로 낮은 염색을 보였다 (ANOVA에서 p<0.001이었고 사후 t-검정에서 p<0.05였다). 도 7(H)는 6G1 및 시판되는 항체인 6E10으로만 Aβ의 혈관 침착물(화살표)이 강하게 염색되고, 8F5 또는 8C5로는 매우 약하게 염색된 것을 보여준다. Tg2576 마우스에서 정성적으로 유사한 상태가 관찰되었다 (본원에 제시되지 않음).
도 8은 글로불로머 대 Aβ(1-42) 단량체, Aβ(1-40) 및 sAPP에 대한 8C5의 선택성을 보여준다. 8C5에 대한 선택성 인자는 EC50 값 간의 비로서 계산할 수 있다 (對 HFIP 중의 Aβ(l-42) 단랑체): 2346/568.2 = 4.1; 對 NH4OH 중의 Aβ(l-42) 단량체): >100; 對 Aβ(l-40) 단량체: >100; 對 sAPP: >100).
도 9(A)는 8C5의 중쇄를 암호화하는 뉴클레오티드 서열 (서열번호 11)을 나타내고, 도 9(B)는 8C5의 경쇄를 암호화하는 뉴클레오티드 서열 (서열번호 12)를 나타낸다. 도 10(A) 및 10(B)에 언급된 상응하는 CDR을 암호화하는 뉴클레오티드 서열은 밑줄로 표시되어 있다.
도 10(A)는 모노클로날 항체 8C5의 가변 중쇄의 아미노산 서열 (서열번호 19)를 나타내고, 도 10(B)는 모노클로날 항체 8F5의 가변 경쇄의 아미노산 서열 (서열번호 20)을 나타낸다. 가변 중쇄의 하나의 CDR은 아미노산 서열 SYGMS (서열번호 13)으로 표시된다. 가변 중쇄의 다른 CDR은 아미노산 서열 SIKNNGGSTYYPDSLKG (서열번호 14)로 표시되고, 가변 중쇄의 또다른 CDR은 아미노산 서열 SGDY (서열번호 15)로 표시된다. 가변 경쇄의 하나의 CDR은 아미노산 서열 RSSQSLVHSNGDTFLH (서열번호 16)으로 표시된다. 가변 경쇄의 다른 CDR은 아미노산 서열 KVSNRFS (서열번호 17)로 표시되고, 가변 경쇄의 또다른 CDR은 아미노산 서열 SQSIHVPWT (서열번호 18)로 표시된다. 모든 상기 CDR은 도 10(A) 및 10(B)에서 밑줄로 표시되어 있다.
Claims (16)
- 가변 중쇄 및 경쇄를 포함하는 모노클로날 항체로서,
a) 가변 중쇄의 3개의 상보성 결정 영역 (CDR)이 서열번호 5, 서열번호 6 및 서열번호 7이고, 가변 중쇄의 3개의 CDR이 서열번호 8, 서열번호 9 및 서열번호 10이거나;
b) 가변 중쇄가 서열번호 1에 의해 암호화되는 가변 중쇄 또는 이와 96% 이상의 동일성을 갖는 가변 중쇄이고, 가변 경쇄가 서열번호 2에 의해 암호화되는 가변 경쇄 또는 이와 96% 이상의 동일성을 갖는 가변 경쇄이거나;
c) 가변 중쇄가 서열번호 3 또는 이와 96% 이상의 동일성을 갖는 서열을 포함하고, 가변 경쇄가 서열번호 4 또는 이와 96% 이상의 동일성을 갖는 서열을 포함하는, 모노클로날 항체. - 가변 중쇄 및 경쇄를 포함하는 사람화된 항체로서,
a) 가변 중쇄의 3개의 상보성 결정 영역 (CDR)이 서열번호 5, 서열번호 6 및 서열번호 7이고, 가변 중쇄의 3개의 CDR이 서열번호 8, 서열번호 9 및 서열번호 10이거나;
b) 가변 중쇄의 3개의 CDR이 서열번호 1에 의해 암호화되거나 이와 96% 이상의 동일성을 갖는 가변 중쇄의 CDR이고, 가변 경쇄의 3개의 CDR이 서열번호 2에 의해 암호화되거나 이와 96% 이상의 동일성을 갖는 가변 경쇄의 CDR이거나;
c) 가변 중쇄의 3개의 CDR이 서열번호 3을 포함하는 중쇄 또는 이와 96% 이상의 동일성을 갖는 서열의 CDR이고, 가변 경쇄의 3개의 CDR이 서열번호 4를 포함하는 경쇄 또는 이와 96% 이상의 동일성을 갖는 서열의 CDR인, 사람화된 항체. - 제1항에 있어서, 가변 중쇄가 서열번호 3을 포함하고, 가변 경쇄가 서열번호 4를 포함하는 모노클로날 항체.
- 제2항에 있어서, 가변 중쇄의 3개의 CDR이 서열번호 3을 포함하는 가변 중쇄의 CDR이고, 가변 경쇄의 3개의 CDR이 서열번호 4를 포함하는 가변 경쇄의 CDR인 사람화된 항체.
- 제4항에 있어서, 가변 중쇄의 3개의 CDR이 서열번호 5, 서열번호 6 및 서열번호 7이고, 가변 경쇄의 3개의 CDR이 서열번호 8, 서열번호 9 및 서열번호 10인 사람화된 항체.
- 제2항, 제4항 및 제5항 중 어느 한 항에 있어서, 골격 영역 전부 또는 실질적으로 전부가 사람 면역글로불린 컨센서스 서열의 골격 영역에 상응하는 사람화된 항체.
- 아메리칸 타입 컬쳐 컬렉션 (ATCC; American Type Culture Collection) 수탁번호 PTA-7238의 하이브리도마.
- 제7항의 하이브리도마에 의해 생성되는 모노클로날 항체 (8F5).
- a) 알츠하이머병에 걸린 것으로 의심되는 환자로부터 분리된 생물학적 샘플을, 항원/항체 복합체가 형성되는데 충분한 시간 및 조건 하에서, 제1항 내지 제5항 및 제8항 중 어느 한 항에 따른 항체와 접촉시키는 단계; 및
b) 상기 샘플 중의 상기 항원/항체 복합체의 존재를 검출 (상기 복합체의 존재는 상기 환자에서 알츠하이머병의 진단을 나타낸다)하는 단계를 포함하여,
알츠하이머병에 걸린 것으로 의심되는 환자로부터 분리된 생물학적 샘플에서 항원/항체 복합체의 존재를 검출하는 방법. - (a) 제1항 내지 제5항 및 제8항 중 어느 한 항에 따른 항체; 및
(b) 검출가능한 시그널을 발생시킬 수 있는 시그날 발생 화합물에 부착된 제2의 Aβ 단백질 글로불로머-특이적 항체를 포함하는 접합체를 포함하는,
알츠하이머병에 걸린 것으로 의심되는 환자에서 Aβ 단백질 글로불로머의 존재를 측정하기 위한 키트. - (a) 제1항 내지 제5항 및 제8항 중 어느 한 항에 따른 항체에 대한 항-항체; 및
(b) 검출가능한 시그널을 발생시킬 수 있는 시그날 발생 화합물에 부착된 Aβ 단백질 글로불로머를 포함하는 접합체를 포함하는,
알츠하이머병에 걸린 것으로 의심되는 환자에서 Aβ 단백질 글로불로머의 존재를 측정하기 위한 키트. - a) 알츠하이머병에 걸린 것으로 의심되는 환자로부터 분리된 생물학적 샘플을, 항원/항체 복합체가 형성되는데 충분한 시간 및 조건 하에서, 제6항에 따른 항체와 접촉시키는 단계; 및
b) 상기 샘플 중의 상기 항원/항체 복합체의 존재를 검출 (상기 복합체의 존재는 상기 환자에서 알츠하이머병의 진단을 나타낸다)하는 단계를 포함하여,
알츠하이머병에 걸린 것으로 의심되는 환자로부터 분리된 생물학적 샘플에서 항원/항체 복합체의 존재를 검출하는 방법. - (a) 제6항에 따른 항체; 및
(b) 검출가능한 시그널을 발생시킬 수 있는 시그날 발생 화합물에 부착된 제2의 Aβ 단백질 글로불로머-특이적 항체를 포함하는 접합체를 포함하는,
알츠하이머병에 걸린 것으로 의심되는 환자에서 Aβ 단백질 글로불로머의 존재를 결정하기 위한 키트. - (a) 제6항에 따른 항체에 대한 항-항체; 및
(b) 검출가능한 시그널을 발생시킬 수 있는 시그날 발생 화합물에 부착된 Aβ 단백질 글로불로머를 포함하는 접합체를 포함하는,
알츠하이머병에 걸린 것으로 의심되는 환자에서 Aβ 단백질 글로불로머의 존재를 결정하기 위한 키트. - 제1항 내지 제5항 및 제8항 중 어느 항의 분리된 항체를 포함하는 알츠하이머병을 치료 또는 예방하기 위한 약제학적 조성물.
- 제6항의 분리된 항체를 포함하는 알츠하이머병을 치료 또는 예방하기 위한 약제학적 조성물.
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