KR102611853B1 - 안정화된 키메라 fabs - Google Patents
안정화된 키메라 fabs Download PDFInfo
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- KR102611853B1 KR102611853B1 KR1020207000438A KR20207000438A KR102611853B1 KR 102611853 B1 KR102611853 B1 KR 102611853B1 KR 1020207000438 A KR1020207000438 A KR 1020207000438A KR 20207000438 A KR20207000438 A KR 20207000438A KR 102611853 B1 KR102611853 B1 KR 102611853B1
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Abstract
람다 경쇄를 갖는 부모 키메라 Fab로부터 유래된 안정화된 키메라 Fabs가 본원에서 제공된다. 상기 안정화된 키메라 Fabs는 상기 부모 키메라 Fab의 면역글로블린 중쇄 폴리펩티드 구조체를 포함하고, CH1 서열 및 VH 서열, 뿐만 아니라 V람다-C카파 키메라 경쇄 구조체를 보유한다. 키메라 경쇄 구조체의 V람다 서열은 상기 부모 키메라 Fab의 것에 대응하며, 그리고 상기 부모 키메라 Fab와 비교하여 상기 안정화된 키메라 Fab의 열 안정성을 증가시키는 하나 또는 그 이상의 안정화 아미노산 변형을 포함한다. 상기 안정화된 Fabs는 치료 폴리펩티드로 유용하며, 또는 다른 포멧의 항체 구조체를 만들 때 이용될 수 있다. 상기 안정화된 키메라 Fabs는 람다 경쇄를 갖는 항체의 안정성을 증가시키는데 일반적으로 또한 유용할 수 있다.
Description
도 2는 항체 CAT-2200의 예시적인 V람다-C카파 키메라 경쇄 구조체의 서열을 나타낸다. CAT-2200에 대응하는 WT 람다 경쇄 서열 (PDB 엔트리 2VXS, 쇄 L)은 상기 CAT-2200 항체에 기초한 V람다-C카파 키메라 경쇄 구조체와 나란히 배열되어, 이들 두 구조체 간의 차이를 강조한다. V람다-C카파 키메라 경쇄 구조체는 잔기 L106A에서 끝나는 CAT-2200의 람다 가변 도메인 서열과 위치 R108에서 출발하는 IGKC*01에 대응하는 카파 불변 도메인 서열을 포함한다. EMBL-EBI 웹사이트를 참고하였을 때, 별표 (*)는 단일 보존된 잔기를 갖는 위치를 나타내고; 콜론(:)은 상당히 유사한 성질들의 집단 간에 보존을 나타내고; 마침표 (.)는 유사성이 매우 약한 집단 간에 보존을 나타내고; 그리고 합의(consensus) 기호가 없다는 것은 매우 상이한 잔기를 나타낸다.
도 3a-3d는 경쇄에서 가변 도메인-불변 도메인 계면의 리본 다이아그램을 도시한다. 도 3a는 Fab의 도식적 표시를 나타낸다. 상자 영역에 대응하는 영역은 대응하는 도 3b 내지 3d에 확대되어 있다. 도 3b 는 V카파-C카파 계면에서 핫 스팟 잔기 83, 85 및 105를 강조한다 (D3H44 항체, PDB:1jpt). 도 3c는 V람다-C람다 계면 (CAT-2200 항체, PDB:2vxs)을 나타내며, 또한 잔기 83, 85 및 105를 강조한다. 도 3d 는 최적화되지 않은(unoptimized) V람다-C카파 계면 (항체 S4, PDB: 3nps)을 나타내며, 다시 잔기 83, 85 및 105를 강조한다.
도 4는 Mab 형식에 적용된 도 1과 유사한 도해로 나타내는데, WT 람다 Mab, V람다-C카파 키메라 Mab 및 기획된 V람다-C카파 키메라 Mab (안정화된 Mab로도 또한 지칭됨)을 도시하고, 여기에서 별표는 안정성 최적화 디자인의 존재를 보여준다.
도 5는 CAT-2200 시스템에서 선별된 기획된 키메라 Fabs (CAT-2200 항체 중쇄의 가변 영역은 VH3 생식계열 하위집단에 속하고, 단백질-A에 결합하는 능력을 갖는다), Mabs 그리고 각각의 야생형 포멧에 대한 단백질-A 역가(titers)를 비교한 것을 제공한다. 3개의 독립적인 50 ml 형질감염으로부터의 평균 단백질-A 역가 (mg/L)가 플롯된다.
도 6a-6b는 83X 디자인 테마 안에 그리고 이를 가로질러 안정화 아미노산 변형의 효과를 나타내며, 여기에서 상이한 부모 키메라 Fabs에 근거하였을 때, X= F, V, I, A이다. 도 6a는 CAT-2200 람다 항체에 기초하여 안정화된 키메라 Fabs의 열 안정성을 나타내고; 그리고 도 6b는 H3 람다 항체에 기초하여 안정화된 키메라 Fabs의 열 안정성을 나타낸다. 각각의 부모 키메라 Fab의 것과 비교하였을 때, 안정화된 키메라 Fab의 Tm에서의 변화(DSF에 의해 측정됨)가 테마 디자인 수에 대하여 플롯된다.
도 7은 상이한 Fab 시스템에 걸쳐 열 안정성의 증가 정도를 도시한다. 3가지 테스트 시스템 H3, CAT-2200 및 EP6b_B01에서 7개의 선별된 디자인(모든 테마를 커버함)에 대하여 각각의 부모 키메라 Fab의 것과 비교하였을 때, 기획된 키메라 Fab의 Tm에서의 변화(DSC에 의해 측정됨)가 플롯된다.
도 8은 Fab에서 Mab 포멧으로의 안정성 증가의 이동성을 드러낸다. 2개의 테스트 시스템 H3 및 CAT-2200에 대하여 각각의 키메라 Fab 또는 Mab의 것과 비교하였을 때, 7가지 선별된 기획된 키메라 Fabs 및 Mabs의 Tm에서의 변화(DSC에 의해 측정됨)가 플롯된다.
도 9a-9b는 H3 항체 시스템에서 2개의 디자인 (디자인 18 및 39)의 하위집단 상에 기획된 키메라 Fabs (도 9a) 및 Mabs (도 9b)의 전형적인 DSC 프로파일을 도시한다. 각각의 야생형 그리고 키메라 Fabs 및 Mabs에 대한 DSC 프로파일은 참조용으로 포함된다.
도 10a-10f는 벤치탑 안정성 연구의 상이한 시점에서 H3 시스템에 기초한 기획된 키메라 Mabs의 전형적인 단분산 UPLC-SEC 프로파일을 도시한다. 이 연구는 37℃에서 PBS 완충액 pH 7.4에서 5 mg/ml 농도에서 실행되었다. 도 10a, 10c, 그리고 10e는 차례로 0일, 20일, 그리고 30일에 야생형 람다 Mab의 UPLC-SEC 프로파일을 나타낸다. 도 10b, 10d, 그리고 10f는 차례로 0일, 20일 30일에 디자인 37에 대응하는 안정화 아미노산 변형을 갖는 안정화된 Mab의 UPLC-SEC 프로파일을 나타낸다.
도 11은 세포에서 2개의 상이한 경쇄가 2개의 상이한 중쇄와 함께 공동-발현될 때, 예상될 수 있는 잠재적 중쇄-연합된 산물을 도시한다. 선호적 페어링(pairing)은 SMCA (단일클론성 항체 경쟁 분석)을 이용하여 평가된다.
도 12는 부모의 Fab 1 (카파 Fab) 및 부모의 Fab 2 (기획된 V람다-C카파 키메라 Fab)로 구성된 예시적인 기획된 이중특이적 키메라 항체의 도식적 표시를 나타내고, 여기에서 별표는 안정성 최적화 디자인을 나타내고, 직사각형 기호는 경쇄 페어링 디자인 또는 중쇄 페어링 디자인을 나타낸다.
Claims (61)
- 다음을 포함하는 키메라 이형이량체:
a) 중쇄 불변 도메인 1 (CH1) 서열 및 중쇄 가변 도메인 (VH) 서열을 포함하는 제1 면역글로불린 중쇄 폴리펩티드 구조체 (H1), 및
b) 카파 경쇄 불변 도메인 (C카파) 서열 및 람다 경쇄 가변 도메인 (V람다) 서열을 포함하는 제1 키메라 면역글로불린 경쇄 폴리펩티드 구조체 (L1), 이때 상기 V람다 서열은 시차주사열량분석 (DSC) 또는 차등적 스캐닝 형광측정법 (DSF)에 의해 측정 시 안정화 아미노산 변형이 없는 대응하는 야생형 키메라 이형이량체와 비교하였을 때 키메라 이형이량체의 용융 온도를 증가시키는 하나 이상의 안정화 아미노산 변형을 포함하며,
이때 H1 및 L1은 제1 에피토프에 결합하는 제1 Fab 영역을 형성하고,
이때 하나 이상의 안정화 아미노산 변형은 잔기 83, 잔기 85, 또는 두 잔기 모두의 치환을 포함하고, 이때 잔기 83은 F, V, I, 또는 A로 치환되고, 잔기 85는 T 또는 V로 치환되고;
이때 아미노산 잔기의 번호매김은 Kabat에 따른다. - 청구항 1에 있어서, V람다 서열은 C카파 서열과 V람다 서열 사이의 계면에서 하나 이상의 아미노산 잔기의 안정화 아미노산 변형을 추가로 포함하고, 이때 하나 이상의 아미노산 잔기는 잔기 80, 105 및 106으로 이루어진 군으로부터 선택되고, 이때 잔기 80은 A 또는 P로 치환되고, 잔기 105는 E로 치환되고, 잔기 106은 I로 치환되는, 키메라 이형이량체.
- 청구항 1에 있어서, V람다 서열은 잔기 83, 85, 105 및 106으로 이루어진 군으로부터 선택된 2개 이상의 잔기의 안정화 아미노산 변형을 포함하고, 이때 잔기 83은 F, V, I, 또는 A로 치환되고, 잔기 85는 T 또는 V로 치환되고, 잔기 105는 E로 치환되고, 잔기 106은 I로 치환되는, 키메라 이형이량체.
- 청구항 1에 있어서, 키메라 이형이량체의 V람다 서열이 다음의 안정화 아미노산 변형 중 하나를 포함하는 것인 키메라 이형이량체:
(a) 83F, 105E 및 106AK;
(b) 83F, 105E, V106I 및 106AK;
(c) 80A, 83F, 105E 및 106AK;
(d) 80A, 83F, 105E, 106I 및 106AK;
(e) 80A, 83F, 85T, 105E 및 106AK;
(f) 80A, 83F, 85T, 105E, 106I 및 106AK;
(g) 80P, 83F, 85T, 105E, 106I 및 106AK;
(h) 85T;
(i) 85V;
(j) 83F;
(k) 83F 및 105E;
(l) 83F 및 106I;
(m) 83F 및 85T;
(n) 83F, 85T 및 105E;
(o) 83F, 85V 및 105E;
(p) 83F, 85T, 105E 및 106I;
(q) 83F, 85V, 105E 및 106I;
(r) 83F, 85T, 105E, 106I 및 106AK;
(s) 83V;
(t) 83V 및 105E;
(u) 83V 및 106I;
(v) 83V 및 85T;
(w) 83V, 85T 및 105E;
(x) 83V, 85V 및 105E;
(y) 83V, 85T, 105E 및 106I;
(z) 83I;
(aa) 83I 및 105E;
(bb) 83I 및 85T;
(cc) 83I, 85T 및 105E;
(dd) 83I, 85T, 105E 및 106I;
(ee) 83A;
(ff) 83A 및 105E;
(gg) 83A 및 85T;
(hh) 83A, 85T 및 105E; 또는
(ii) 83A, 85T, 105E 및 106I. - 청구항 1에 있어서, 키메라 이형이량체의 용융 온도가 안정화 아미노산 변형이 없는 대응하는 야생형 키메라 이형이량체와 비교하였을 때 1, 2, 3, 4, 5, 6, 7, 8, 또는 9℃만큼 증가되는, 키메라 이형이량체.
- 다음을 포함하는 항체 구조체:
a) 제1 이형이량체, 이때 상기 제1 이형이량체는 청구항 1에 따른 키메라 이형이량체임, 및
b) 스캐폴드
이때 전술한 제1 이형이량체의 H1 및 L1 중 최소한 하나는 링커와 함께, 또는 링커 없이 상기 스캐폴드에 연계된다. - 청구항 6에 있어서, 제2 이형이량체를 더 포함하며, 전술한 제2 이형이량체는 다음을 포함하는 항체 구조체:
i) 중쇄 불변 도메인 1 (CH1) 서열, 및 중쇄 가변 도메인 (VH) 서열을 포함하는 제2 면역글로불린 중쇄 폴리펩티드 구조체 (H2), 및
ii) 경쇄 불변 도메인 (CL) 서열 및 경쇄 가변 도메인 (VL) 서열을 포함하는 제2 이뮤노글로불린 경쇄 폴리펩티드 구조체 (L2),
이때 H2와 L2는 제2 에피토프에 결합하는 제2 Fab 영역을 형성하고, 그리고 H2 및 L2 중 최소한 하나는 링커와 함께, 또는 링커 없이, 상기 스캐폴드에 연결된다. - 청구항 7에 있어서, 상기 제1 에피토프와 제2 에피토프는 동일한, 항체 구조체.
- 청구항 7에 있어서, 제1 에피토프와 제2 에피토프는 서로 상이한, 항체 구조체.
- 청구항 7에 있어서, 제1 이형이량체, 제2 이형이량체, 또는 두 이형이량체 모두는 경쇄 페어링을 촉진시키는 하나 이상의 아미노산 치환을 더 포함하는, 항체 구조체.
- 청구항 7에 있어서, 상기 스캐폴드는 제1 중쇄 불변 도메인 3 (CH3) 서열 및 제2 CH3 서열을 포함하는 Fc 영역인, 항체 구조체.
- 청구항 11에 있어서, 상기 제1 CH3 서열 및 제2 CH3 서열은 각각 동종이량체 CH3 도메인과 비교하였을 때, 이형이량체 CH3 도메인 형성을 촉진시키는 하나 이상의 아미노산 변형을 포함하는, 항체 구조체.
- 청구항 11에 있어서, 상기 Fc 영역은 제1 불변 도메인 2 (CH2) 서열과 제2 CH2 서열을 더로 포함하는, 항체 구조체.
- 청구항 11에 있어서, Fc 영역은 인간 Fc, 인간 IgG1 Fc, 인간 IgA Fc, 인간 IgG Fc, 인간 IgD Fc, 인간 IgE Fc, 인간 IgM Fc, 인간 IgG2 Fc, 인간 IgG3 Fc, 또는 인간 IgG4 Fc인, 항체 구조체.
- 청구항 6에 있어서, 상기 링커는 하나 이상의 폴리펩티드 링커인, 항체 구조체.
- 청구항 6에 있어서, 상기 링커는 하나 이상의 항체 힌지 영역을 포함하는, 항체 구조체.
- 청구항 16에 있어서, 상기 링커는 하나 이상의 IgG1 힌지 영역을 포함하는, 항체 구조체.
- 청구항 6에 있어서, 약물에 접합된 항체 구조체.
- 청구항 1에 따른 키메라 이형이량체, 또는 청구항 6에 따른 항체 구조체, 및 약학적으로 수용가능한 운반체를 포함하는 암 치료용 약학 조성물.
- 청구항 1에 따른 키메라 이형이량체, 또는 청구항 6에 따른 항체 구조체를 인코딩하는 폴리뉴클레오티드 또는 폴리뉴클레오티드의 세트.
- 청구항 20에 따른 폴리뉴클레오티드 또는 폴리뉴클레오티드 세트 중 하나 이상을 포함하는 벡터 또는 벡터 세트.
- 청구항 20에 따른 폴리뉴클레오티드 또는 폴리뉴클레오티드의 세트를 포함하는, 단리된 세포.
- 청구항 1에 따른 키메라 이형이량체 또는 청구항 6에 따른 항체 구조체를 준비하는 방법이며,
(a) 청구항 1에 따른 키메라 이형이량체 또는 청구항 6에 따른 항체 구조체를 인코딩하는 폴리뉴클레오티드 또는 폴리뉴클레오티드 세트를 포함하는 숙주 세포를 획득하는 단계;
(b) 상기 키메라 이형이량체 또는 항체 구조체의 발현을 허용하는 조건 하에 숙주 세포 배양물에서 상기 숙주 세포를 배양하는 단계, 및
(c) 상기 숙주 세포 배양물로부터 상기 키메라 이형이량체 또는 항체 구조체를 수거하는 단계
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| US201762527561P | 2017-06-30 | 2017-06-30 | |
| US62/527,561 | 2017-06-30 | ||
| PCT/CA2018/050809 WO2019000105A1 (en) | 2017-06-30 | 2018-06-29 | STABILIZED CHIMERIC FABES |
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| EP (1) | EP3645575A4 (ko) |
| JP (1) | JP7245793B2 (ko) |
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2018
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- 2018-06-29 AU AU2018292438A patent/AU2018292438B2/en active Active
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Non-Patent Citations (2)
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| J. L. Jordan et al, Proteins, 77(4), 832-841(2009.06.19.) 1부.* |
| R. Toughri et al, mAbs, 8(7), 1276-1285(2016.09.16.) 1부.* |
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| RU2019142330A (ru) | 2021-07-30 |
| JP2020530265A (ja) | 2020-10-22 |
| BR112019025105A2 (pt) | 2020-10-20 |
| KR20200024828A (ko) | 2020-03-09 |
| AU2018292438A1 (en) | 2019-12-12 |
| US20200308270A1 (en) | 2020-10-01 |
| WO2019000105A1 (en) | 2019-01-03 |
| EP3645575A1 (en) | 2020-05-06 |
| US11965019B2 (en) | 2024-04-23 |
| CA3064966A1 (en) | 2019-01-03 |
| RU2019142330A3 (ko) | 2021-12-13 |
| CN110831978A (zh) | 2020-02-21 |
| JP7245793B2 (ja) | 2023-03-24 |
| EP3645575A4 (en) | 2021-03-24 |
| AU2018292438B2 (en) | 2024-11-14 |
| MX2019015293A (es) | 2020-02-17 |
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