KR20160128431A - 항원-특이적인 t 세포 반응을 유도하는 면역 강화제로서 사용을 위한 융합 단백질 - Google Patents
항원-특이적인 t 세포 반응을 유도하는 면역 강화제로서 사용을 위한 융합 단백질 Download PDFInfo
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- KR20160128431A KR20160128431A KR1020167029734A KR20167029734A KR20160128431A KR 20160128431 A KR20160128431 A KR 20160128431A KR 1020167029734 A KR1020167029734 A KR 1020167029734A KR 20167029734 A KR20167029734 A KR 20167029734A KR 20160128431 A KR20160128431 A KR 20160128431A
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- leu
- ala
- antigen
- virus
- glu
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Abstract
본 발명은 강화된 병원균(pathogen) 항원(antigen)-특이적인 T 세포 반응을 유도하기 위한 융합 단백질(fusion protein)을 포함하는 백신 조성물(vaccine composition)을 개시하였다. 상기 융합 단백질은 하기를 포함한다: (a) 융합 단백질의 N-말단에 위치한, 항원-제시 세포(antigen-presenting cell; APC)-결합 도메인(binding domain) 또는 CD91 수용체(receptor)-결합 도메인; (b) APC-결합 도메인 또는 CD91 수용체-결합 도메인의 C-말단에 위치한 서열번호 4, 2, 3 또는 6과 최소 90% 일치하는 아미노산 서열을 포함하는 34 내지 112 아미노산 잔기 길이의 전좌 펩타이드(translocation peptide); 및 (c) 전좌 펩타이드의 C-말단에 위치한, 병원균의 항원; (d) 서열번호 13의 아미노산 잔기를 포함하는 핵 배출 신호(nuclear export signal); 및 (e) 융합 단백질의 C-말단에 위치한, 소포체(endoplasmic reticulum) 유지(retention) 서열.
Description
본 발명은 일반적으로 융합 단백질(fusion protein) 및 면역학(immunology)에 관한 것이다.
분자 생물학(molecular biology)은 면역원(immunogen)이 모단백질(parent protein) 또는 복합체(complex)의 절편 또는 소단위(subunit)인, 소단위 백신(vaccine)의 생산을 가능하게 하였다. T 세포 민감성 반응(T cell sensitizing responses)을 유도할 수 있고 감염성 시약(infectious agent)의 많은 종(strains)으로부터의 서열을 포함하기에 충분히 유연한 안정한 백신의 개발이 필요하다.
한 측면에서, 본 발명은 하기를 포함하는 융합 단백질과 연관된다:
(a) 융합 단백질의 N-말단에 위치한 항원-제시 세포(antigen-presenting cell; APC)-결합 도메인 또는 CD91 수용체-결합 도메인;
(b) APC-결합 도메인 또는 CD91 수용체-결합 도메인의 C-말단에 위치한, 서열번호 4, 2, 3, 또는 6과 최소 90% 동일한 아미노산 서열을 포함하는, 34 내지 112 아미노산 잔기 길이의 전좌 펩타이드(translocation peptide); 및
(c) 전좌 펩타이드의 C-말단에 위치한 핵 배출 신호(nuclear export signa);
(d) 서열번호 13의 아미노산 서열을 포함하는 핵 배출 신호; 및
(e) 융합 단백질의 C-말단에 위치한 소포체(endoplasmic reticulum) 유지 서열.
본 발명의 한 실시예에서, 상기 APC-결합 도메인 또는 CD91 수용체-결합 도메인은 서열번호 1 및 8 내지 11로 이루어진 군으로부터 선별된 서열과 최소 90% 동일한 아미노산 서열을 포함하는 폴리펩타이드이다.
본 발명의 또 다른 실시예에서, 상기 핵 배출 신호는 서열번호 14의 아미노산 서열을 포함한다.
본 발명의 또 다른 실시예에서, 상기 소포체 유지 서열은 서열번호 15의 아미노산 서열을 포함한다.
본 발명의 또 다른 실시예에서, 상기 핵 배출 신호는 전좌 펩타이드 및 항원 사이에 위치한다.
본 발명의 또 다른 실시예에서, 상기 핵 배출 신호는 항원 및 소포체 유지 서열 사이에 위치한다.
본 발명의 또 다른 실시예에서, 상기 핵 배출 신호 및 ER 유지 신호는 서열번호 12와 최소 90% 동일한 아미노산 서열을 포함하는 융합 단백질을 형성한다.
본 발명의 또 다른 실시예에서, 상기 전좌 펩타이드는 34 내지 61 아미노산 잔기 길이이다.
본 발명의 또 다른 실시예에서, 상기 전좌 펩타이드는 34 내지 46 아미노산 잔기 길이이다.
본 발명의 또 다른 실시예에서, 상기 APC-결합 도메인 또는 CD91 수용체-결합 도메인은 수도모나스 덱소톡신 A(Pseudomonas exotoxin A; PE) 결합 도메인 I의 아미노산 서열이 없다.
본 발명의 또 다른 실시예에서, 상기 APC-결합 도메인 또는 CD91 수용체-결합 도메인은 서열번호 8의 아미노산 서열을 포함한다.
본 발명의 또 다른 실시예에서, 상기 APC-결합 도메인 또는 CD91 수용체-결합 도메인의 아미노산 서열은 서열번호 1이다.
본 발명의 또 다른 실시예에서, 상기 항원은 병원균(pathogen)으로부터 유래한 두 개 또는 그 이상의 항원성 펩타이드의 융합이다.
본 발명의 또 다른 실시예에서, 상기 ER 유지 서열은 4개 이상의 아미노산 잔기 길이를 갖는다.
본 발명의 또 다른 실시예에서, 상기 전좌 펩타이드는 서열번호 4, 2, 3, 또는 6과 최소 95% 동일한 아미노산 서열을 포함한다.
본 발명의 또 다른 실시예에서, 상기 APC-결합 도메인 또는 CD91 수용체-결합 도메인은 수지상 세포(dendritic cells), 단핵 백혈구(monocytes), B-세포 및 림프구(lymphocytes)로 이루어진 군으로부터 선별된 항원-제시 세포(APC)에 있는 수용체를 인식 및 결합하는 특징을 나타낸다.
본 발명의 또 다른 실시예에서, 상기 병원균은 PRRSV, PCV, FMDV, CSFV, NDV, 전염성 위장염 바이러스(Transmissible gastroenteritis virus; TGEV), 돼지 재생산 및 호흡 증후군 바이러스(Porcine epidemic diarrhea virus; PEDV), 인플루엔자 바이러스(Influenza virus), 수도라비스 바이러스(Pseudorabies virus), 파보바이러스(Prvovirus), 수도라비스 바이러스(Pseudorabies virus), 돼지 수포병 바이러스(Swine vesicular disease virus; SVDV), 폭스바이러스(Poxvirus), 로타바이러스(Rotavirus), 마이코플라스마 폐렴(Mycoplasma pneumonia), 헤르페스 바이러스(Herpes virus), 닭전염성 기관지염(Infectious bronchitis), 및 감보로 바이러스(Infectious bursal disease virus)로 이루어진 군으로부터 선별된 것이다.
또 다른 측면에서, 본 발명은 필수적으로, 또는 하기의 구성으로 구성한다:
(a) 융합 단백질의 N-말단에 위치한 항원-제시 세포(antigen-presenting cell; APC)-결합 도메인 또는 CD91 수용체-결합 도메인;
(b) APC-결합 도메인 또는 CD91 수용체-결합 도메인의 C-말단에 위치한, 서열번호 4, 2, 3, 또는 6과 최소 90% 동일한 아미노산 서열을 포함하는, 34 내지 112 아미노산 잔기 길이의 전좌 펩타이드(translocation peptide); 및
(c) 전좌 펩타이드의 C-말단에 위치한 핵 배출 신호(nuclear export signa);
(d) 서열번호 13의 아미노산 서열을 포함하는 핵 배출 신호; 및
(e) 융합 단백질의 C-말단에 위치한 소포체(endoplasmic reticulum) 유지 서열.
추가적인 또 다른 측면에서, 본 발명은 앞서 말한 것으로서 융합 단백질 및 아주번트(adjuvant)를 포함하는 백신 조성물과 연관된다.
또 다른 측면에서, 본 발명은 앞서 말한 융합 단백질을 그것을 필요로 하는 개체에 치료적으로 효과적인 양, 및 이를 통해 강화된 병원체 항원-특이적인 T 세포 반응을 유도하는 것을 포함하는 백신 조성물의 투여를 포함하는, 강화된 병원균 항원-특이적인 T 세포 반응을 유도하기 위한 방법과 연관된다.
본 발명은 또한 강화된 병원균 항원-특이적인 T 세포 반응을 유도하거나 강화된 병원균 항원-특이적인 T 세포 반응을 유도하기 위한 약물의 제조에서 앞서 말한 융합 단백질의 사용에 있어서 앞서 말한 융합 단백질 또는 백신 조성물과 연관된다.
도 1A는 전장(full-length) 수도모나스 에루지노사 엑소톡신 A(Pseudomonas aeruginosa exotoxin A; PE), 및 PE의 절편의 개략적인 그림을 나타내는 도이다.
도 1B 및 1C는 벡터 지도(vector map)를 나타내는 도이다.
도 2 내지 5의 a 및 b 그래프는 각각 강화된 CD8+/IFN-γ+ T 세포 및 CD4+/IFN-γ+ T 세포 매개의 면역원성(immunogenicity)을 유도하는 본 발명을 따르는 융합 단백질을 나타내는 도이다:
도 2a 및 2b에서
1: 플라시보,
2: PE407-ORF2-K3,
3: PE313-ORF2-NESK,
도 3a 및 3b에서
1: 플라시보,
2: PE407-E2-K3,
3: PE313-E2-NESK,
도 4a 및 4b에서
1: 플라시보,
2: PE407-VP1-3A-K3,
3: PE313-VP1-3A-NESK,
도 5a 및 5b에서
1: 플라시보,
2: PE407-FHN-K3,
3: PE313-FHN-NESK.
도 6은 동물 그룹, 백신 및 동물의 면역화에 사용되는 투여량(dosage) 및 면역화(immunization) 스케줄을 나타낸 도이다.
도 7 및 8은 다양한 융합 단백질 또는 플라시보로 백신화된 동물 그룹에서 각각 종양 크기 곡선 및 종양-없는 마우스의 백분율을 나타낸 도이다.
도 1B 및 1C는 벡터 지도(vector map)를 나타내는 도이다.
도 2 내지 5의 a 및 b 그래프는 각각 강화된 CD8+/IFN-γ+ T 세포 및 CD4+/IFN-γ+ T 세포 매개의 면역원성(immunogenicity)을 유도하는 본 발명을 따르는 융합 단백질을 나타내는 도이다:
도 2a 및 2b에서
1: 플라시보,
2: PE407-ORF2-K3,
3: PE313-ORF2-NESK,
도 3a 및 3b에서
1: 플라시보,
2: PE407-E2-K3,
3: PE313-E2-NESK,
도 4a 및 4b에서
1: 플라시보,
2: PE407-VP1-3A-K3,
3: PE313-VP1-3A-NESK,
도 5a 및 5b에서
1: 플라시보,
2: PE407-FHN-K3,
3: PE313-FHN-NESK.
도 6은 동물 그룹, 백신 및 동물의 면역화에 사용되는 투여량(dosage) 및 면역화(immunization) 스케줄을 나타낸 도이다.
도 7 및 8은 다양한 융합 단백질 또는 플라시보로 백신화된 동물 그룹에서 각각 종양 크기 곡선 및 종양-없는 마우스의 백분율을 나타낸 도이다.
본 발명은 오직 당업계에 종사하는 기술자에게는 자명한 수많은 변형 및 변이 기술로서 설명되는 것으로 의도되는 하기의 실험예에서 더 명확하게 기술된다. 본 발명의 다양한 실시예를 이제 자세하게 기술한다. 도면을 참조하는 것은, 전체에 걸쳐서 숫자가 같은 것이 구성요소 같은 것을 가르키는 것이다. 본 명세서의 기술 및 청구항 전체에 사용된 하기의, "단수어(a)", "단수어(an)", 및 "한정어(the)"는 문맥상 명백하게 다른 것을 나타내지 않는다면 복수 참조를 포함하는 의미이다. 또한, 본 명세서의 기술 및 청구항 전체에서 사용된 하기의, "안에(in)"는 문맥상 명백하게 다른 것을 나타내지 않는다면 "안(in)" 및 "위(on)"을 포함하는 의미이다. 더 나아가, 본 명세서의 제목 및 부제목은 본 발명의 범위에 영향을 주지 않고, 독자의 편의를 위해서 사용하였다. 추가적으로, 본 명세서에 사용된 몇몇의 용어는 하기에 더 자세하게 정의하였다.
정의
본 명세서에서 사용된 용어는 일반적으로 본 발명의 문맥 안에서, 당업계에서 및 각 용어가 사용된 특정 문맥에서의 그들의 보통의 의미를 갖는다. 본 발명을 설명하는데 사용된 특정 용어는 본 발명의 기술을 고려하는 전문가에게 추가적인 지도를 제공하기 위해 하기 또는 본 명세서의 어딘가에서 논의하였다. 편의를 위해서, 특정 용어는, 예를 들면 이탤릭체(italics) 및/또는 따옴표(quotation marks)의 형태로 강조하였다. 같은 것이 하나 이상의 방법으로 얘기할 수 있다는 것이 이해될 것이다. 결론적으로, 대체적인 언어 및 동의어는 본 명세서에서 논의되는 한 또는 그 이상의 용어로 사용되며, 용어가 본 명세서에서 확대되거나 논의되던지 간에 어떠한 특별한 중요성을 갖지 않는다. 특정 용어에 대한 동의어는 제공하였다. 하나 또는 이상의 동의어의 설명이 다른 동의어의 사용을 배재 하는 것은 아니다. 본 명세서에서 논의된 임의의 용어의 예시를 포함하는 본 명세서의 어딘가에 있는 실험예의 사용은 오직 설명적이며, 어떠한 방식으로든 본 발명 및 임의의 예시된 용어의 범위 및 의미를 제한한다. 이처럼, 본 발명은 본 명세서에 제시된 다양한 실시예에 한정되지 않는다.
정의되지 않는 한, 본 명세서에 사용된 모든 기술적 및 과학적인 용어들은 본 발명이 적용되는 당업계의 평범한 기술을 가진 자에 의해 일반적으로 이해되는 것과 같은 의미를 가진다. 논란의 경우에, 용어를 포함하는 본 문서는 조절될 것이다.
용어 "항원-제시 세포(APC) 또는 부수적인 세포(accessory cell)"은 세포 표면에 주요 조직적합성 복합체(major histocompatibility complexes; MHCs)와 복합체를 이루는 외부 항원을 나타내는 세포를 말한다. T-세포는 T-세포 수용체(T-cell receptors; TCRs)를 이용하여 이러한 복합체들을 인식할 것이다. 이러한 세포는 항원을 처리하며 이들을 T-세포로 제시한다. 다양한 종류의 전문적인 항원-제시 세포는 수지상 세포(dendritic cells; DCs), 대식세포(macrophages), 또한 CD4+인 것들 및 그러므로 또한 HIV에 의한 감염에 민감한 것들; 단핵 백혈구(monocytes), 및 특정 B-세포이다.
용어 "항원-제시 세포(APC)-결합 도메인"은 항원-제시 세포(APC)에 결합할 수 있는 도메인(폴리펩타이드 인 것)을 말한다. 상기 APC-결합 도메인은 서열번호 1 및 8 내지 11로 구성된 군으로부터 선별된 서열과 최소 90% 동일한 아미노산 서열을 포함하는 폴리펩타이드 일 수 있다. APC-결합 도메인은 APC에 있는 수용체를 인식하고 결합하는 리간드(ligand)이다.
분화의 집단 91(cluster of differentiation 91; CD91)은 세포의 막에 있는 수용체를 형성하고 수용체-매개의 세포내섭취(endocytosis)에 관여하는 단백질이다.
용어 "PEt"는 34 내지 112 아미노산 잔기(amino acid residues) 길이를 갖는 전좌 펩타이드(또는 전좌 도메인)을 말한다. PEt는 서열번호 2 내지 4 및 6과 최소 90% 동일한 아미노산 서열을 포함할 수 있다. 예를 들면, PEt의 아미노산 서열은 PE의 a.a. 280 - a.a 313(서열번호 4), a.a. 268 - a.a 313(서열번호 3), a.a. 253 - a.a. 313(서열번호 2), 또는 a.a. 253 -a.a 364(서열번호 6)의 절편일 수 있다. 즉, PEt의 아미노산 서열은 PE 도메인 II(a.a. 253 에서 a.a. 364; 서열번호 6)의 임의의 영역을 포함할 수 있는데, 이는 a.a 280 - a.a. 313(서열번호 4) 필수 서열(즉, 필수 절편)을 포함할 만큼 길다.
PE407(서열번호 7)은 이전 특허(US 7,335,361 B2)에서 PE(△III)로서 기술되어 있다.
용어 "최저(minimum) 전좌 펩타이드"는 표적 세포의 세포질로 항원을 이동시킬 수 있는 PE253-313(서열번호 2)를 말한다.
용어 "소포체(endoplasmic reticulum; ER) 유지 서열"은 세포질에서 ER로 항원의 전좌를 돕고 ER의 루멘(lumen) 안에 항원을 유지하는 기능을 하는 펩타이드를 말한다. ER 유지 서열은 Lys Asp Glu Leu(KDEL; 서열번호 15) 또는 RDEL을 포함한다. ER 유지 서열은 KDEL, RDEL, KDELKDELKDEL(K3; 서열번호 16), KKDLRDELKDEL(K3; 서열번호 17), KKDELRDELKDEL(K3; 서열번호 18), 또는 KKDELRVELKDEL(K3; 서열번호 19)를 포함할 수 있다.
용어 "NESK"는 NES 및 ER 유지 신호의 융합 펩타이드(즉, ER 유지 신호에 결합된 NES)를 말한다. 이는 핵 방출 신호(nuclear export signal; NES) 및 ER 유지 서열의 기능을 진행하는 인공적인 펩타이드이다. 그러므로, 이는 핵 구멍 복합체(nuclear pore complex)를 통해 항원을 세포 핵으로부터 세포질로 배출할 수 있으며, 세포질로부터 ER로 항원의 전좌를 돕고 및 ER의 루멘에 항원을 유지할 수 있다. 예를 들면, NESK의 아미노산 서열은 LQKKLEELELAKDEL(서열번호 12)일 수 있다.
항원은 병원균에 의한 질병에 책임이 있거나, 또는 병원균의 감염에 의한 숙주내에서의 면역성 반응을 유도할 수 있거나, 또는 종양 세포에 발현되어 있는 특정 폴리펩타이드인 종양-연관 항원(tumor-associated antigen; TAA)와 같은 병원성 단백질, 폴리펩타이드 또는 펩타이드일 수 있다. 상기 항원은 인간 파필로마바이러스(Human Papillomavirus; HPV), 돼지 재생산 및 호흡 증후군 바이러스(Porcine reproductive and respiratory syndrome virus; PRRSV), 인간 면역결핍 바이러스-1(Human immunodeficiency virus-1; HIV-1), 댕기 바이러스(Dangue virus), C형 간염 바이러스(Hepatitis C virus; HCV), B형 간염 바이러스(Hepatitis B virus; HBV), 돼지 서코바이러스(Porcine Circovirus 2; PCV2), 돼지 콜레라 바이러스(Classical Swine Fever Virus; CSFV), 발-및-입 질병 바이러스(Foot-and-Mouth disease virus; FMDV), 뉴캐슬 질병 바이러스(Newcastle disease virus; NDV), 전염성 위장염 바이러스(Transmissible gastroenteritis virus; TGEV), 돼지 유행성 설사 바이러스(Porcine epidemic diarrhea virus; PEDV), 인플루엔자 바이러스(Influenza virus), 수도라비스 바이러스(Pseudorabies virus), 파르보바이러스(Parvovirus), 수도라비스 바이러스(Pseudorabies virus), 돼지 수포병 바이러스(Swine vesicular disease virus; SVDV), 폭스바이러스(Poxvirus), 로타바이러스(Rotavirus), 마이코플라스마 폐렴(Mycoplasma pneumonia), 헤르페스 바이러스(Herpes virus), 닭전염성 기관지염(infectious bronchitis), 또는 감보로 바이러스(infectious bursal disease virus), 비소세포성 폐암(non-small cell lung cancer), 유방암(breast carcinoma), 흑색종(melanoma), 림프종(lymphomas), 대장암(colon carcinoma), 간세포 암종(hepatocellular carcinoma) 및 이러한 것들의 임의의 조합을 포함하는 병원균 또는 암 세포로부터 선별될 수 있으나 이에 한정되지 않는다. 예를 들면, J{V E7 단백질(E7), HCV 중심 단백질(HCV core), HBV X 단백질(HBx)가 백신의 개발을 위한 항원으로 선별된다. 상기 항원은 하나 또는 그 이상의 병원성 단백질로부터 선택된 둘 또는 그 이상의 항원의 융합으로부터의 융합 항원일 수 있다. 예를 들면, PRRSV ORF6 및 ORF5 절편의 융합 항원, 또는 PRRSV 및 PCV2 병원균으로부터 항원성 단백질의 융합이다.
용어 "치료(treating)" 또는 "치료(treatment)"는 암 또는 감염을 갖거나, 이러한 질병에 대해 증상 또는 소질(predisposition)을 갖고 있는 개체에 질병의 예방, 증상 또는 그것에 대한 소질을 예방하거나 치료, 완화(alleviate), 안정, 요법(remedy), 개선의 목적을 갖고, 효과적인 양의 융합 단백질을 투여하는 것을 말한다. 이러한 개체는 어떠한 적합한 진단 방법에 의한 결론에 기초하는 건강 관리 전문가에 의해 확인될 수 있다.
용어 "효과적인 양"은 치료된 개체에서 치료적인 효과를 부여하는데에 필요한 활성화된 화합물(active compound)의 양을 말한다. 효과적인 도스(dose)는 다향할 것이고, 투여의 경로, 첨가제(excipient) 사용, 및 다른 치료적 치료와의 공동-사용의 가능성에 의존하여 당업계의 기술자에 의해 인식될 수 있다.
본 발명은 강화된 항원 전달 및 세포-매개의 면역 반응의 조절에 대한 융합 단백질과 연관된다. 상기 융합 단백질은 하기를 포함한다: (a) 융합 단백질의 N-말단에 위치한 항원-제시 세포(APC)-결합 도메인 또는 CD91 수용체-결합 도메인; (b) 서열번호 2 내지 4와 최소 90% 일치하고 APC-결합 도메인 또는 CD91 수용체-결합 도메인의 C-말단에 위치한 아미노산 서열을 포함하는 34 내지 112 아미노산 잔기 길이의 전좌 펩타이드; 및 (c) 전좌 펩타이드의 C-말단에 위치한 병원균의 항원; (d) 핵 배출 신호(NES); 및 (e) 소포체 유지 서열, 상기 ER 유지 서열은 서열번호 13의 아미노산 서열을 포함하는 NES가 존재하는 융합 단백질의 C-말단에 위치한다.
실험예로서 융합 단백질 PE313-ORF2-NESK의 사용하는 전략은 본 발명의 융합 단백질이 돼지 서코바이러스 타입 2(Porcine Circovirus Type 2; PCV2) 캡시드(capsid) 단백질 ORF2 항원을 인식하는 T 세포의 생산 및 활성화를 자극한다는 것이다. 상기 융합 단백질은 N-말단에서 C-말단으로, PE 도메인 I(APC-결합 도메인), 34 내지 112 아미노산 잔기 길이의 전좌 펩타이드(예를 들어, PE 도메인 II의 a.a. 253-313), 짧아진 PCV2 ORF2 단백질(N-말단 핵 위치 신호가 제거된), NES 신호 및 ER 유지 서열(KDEL)을 포함한다. PE313-ORF2-NESK에 의한 강화된 ORF2-특이적인 T 세포 면역 반응 유도의 근본적인 기전은 하기의 과정을 포함한다: a) 수지상 세포(또는 항원-제시 세포) 표면 수용체(CD91)로의 결합; b) 세포내섭취에 의한 내재화; c) ER로의 운송 및 전좌 펩타이드의 앞에 퓨린(furin)에 의한 단백질 가수분해(proteolytic hydrolysis); d) MHC I 복합체에 의한 제조 및 제시; 및 e) 항원-특이적인 CD4+ 및 CD8+ T 세포의 활성화. CD4+ Th1 세포는 세포독성의 CD8+ T 세포 면역 반응을 효과적으로 자극하고 강화할 수 있다. 종합하여, 이러한 적응 면역 시스템의 두 개의 팔은 PCV2 및 PCV2-감염된 세포를 사멸하기 위한 특이성(specificity) 및 효능을 갖는다.
상기 융합 단백질 PE313-ORF2-NESK는 US 7,335,361의 Lai에 의해 공개된 융합 단백질 백신 PE407-Ag-K3과 여러 면에서 구별된다. 첫째로, PE313(서열번호 5)의 길이는 PE407(서열번호 7)보다 94 아미노산 잔기가 짧아, 추가의 PE 절편의 존재로 인해 유도되는 원치않는 체액성(humoral) 반응이 최소화되거나 제거된다는 장점을 가진다. 둘째로, ER 유지 서열이 짧아져 있다. K3(KDER의 3)을 대신하여, 오직 하나의 KEDR 또는 REDR이 필요하다. 셋째로, 오직 세포기질성(cytosolic) 항원이 MHC 타입 I 경로에 의해 제작되고 제시될 수 있으며, 이로써 융합 단백질로의 NES 신호의 추가는 항원을 세포기질로 전좌시키는 기회를 증가시키기 때문에 병원균 항원-특이적인 T 세포 반응을 강화하는데 도움이 된다. 병원균의 항원은 세포 핵으로 이입될 수 있다. NES 신호의 포함에 의해, 세포 핵으로 이입된 항원은 융합 단백질의 NES 신호에 의해 세포질로 배출될 수 있다.
실험예
본 발명, 예시적 기기, 기구, 방법 및 본 발명의 실시예를 따르는 상기와 연관된 결과들의 범위를 한정하는 의도가 없이, 하기에 제공하였다. 제목 또는 부제목은 독자의 편의를 위해 실험예에서 사용되었는데, 본 발명의 범위를 한정하는 방법이 아닌 것을 알린다. 나아가, 특정 이론은 본 명세서에서 제안되고 기술되었다; 그러나, 상기의 옳고 그름에 관계없이, 본 발명은 임의의 특정 이론이나 작용 방식에 관계없이 본 발명에 따라 실시되는 대로 발명의 범위를 제한한다.
<실험예 1> 발현 벡터의 제조
도 1A는 PE가 3개의 도메인(I, II 및 III)를 포함하는 것을 나타낸다. PE407은 PE의 a.a. 1로부터 a.a. 407까지의 영역이다. PE407은 세포독성 도메인 III를 포함하지 않고 도메인 I 및 II를 포함한다. PE313은 PE의 a.a. 1로부터 a.a. 313까지의 영역이다. 그러므로, PE313은 오직 도메인 Ia 및 PE의 도메인 II의 부분적인 N-말단 영역을 포함한다.
도 1B 및 C는 항원-제시 세포(APC)-결합 도메인, 전좌 펩타이드, 항원, 핵 배출 신호(NES)와 함께(아래쪽 패널) 또는 없이(위쪽 패널); 및 소포체(ER) 유지 서열(위쪽 패널, K3 또는 아래쪽 패널, K), 융합 단백질의 C-말단에 위치해 있는 ER 유지 서열을 포함하는 발현 벡터의 제조를 나타낸다. 플라스미드(plasmids) pTac-2-PE313-NESK, pTac-2-PE407-K3, pTac-2-RAP1-PE268-313-NESK 및 pTac-2-RAP1-PE268-313-K3은 하기로 생성된다: NdeIPE313-(EcoRI, XhoI )-NESKXhoI, NdeIPE407-(EcoRI, XhoI )-K3XhoI, NdeIRAP1-(EcoRI)-PE268-313-(EcoRI, XhoI )-NESKXhoI 및 NdeIRAP1-(EcoRI)-PE268-313-(EcoRI, XhoI )-K3XhoI절편들은 PCR에 의해 합성되었고 각각의 플라스미드를 얻기 위해 가나마이신(kanamycin) 저항성 유전자와 함께 pUC18 백본(backbone)에 결합하였다.
관심 있는 병원균의 항원 또는 융합 항원을 암호화하는 표적 DNA는 융합 단백질의 발현을 위한 발현 벡터를 생성하기 위해 앞서 언급한 플라스미드에 삽입하였다. 예를 들면, 돼지 서코바이러스 타입 2(PCV2) ORF2(서열번호 20), 돼지 콜레라 바이러스(CSFV) E2(서열번호 21), 발-및-입 질병 바이러스(FMDV) VP1-3A(서열번호 24) 및 뉴캐슬 질병 바이러스(NDV) FHN(서열번호 27)은 합성되어 플라스미드 pTac-2-PE313-NESK, pTac-2-PE407-K3로 각각 삽입하여, 하기의 벡터를 생성하였다: (1) PE313-ORF2-NESK; (2) PE407-ORF2-K3; (3) PE313-E2-NESK; (4) PE407-E2-K3; (5) PE313-VP1-3A-NESK; (6) PE407-VP1-3A-K3; (7) PE313-FHN-NESK; 및 (8) PE407-FHN-K3. 인간 파필로마바이러스 타입 16 E7(서열번호 28)의 항원을 암호화하는 DNA 절편은 합성되어 플라스미드 pTac-2-PE407-K3, pTac-2-RAP1-PE268-313-NESK 및 pTac-2-RAP1-PE268-313-K3로 각각 삽입하여 하기의 발현 벡터를 생성하였다: (9) PE407-E7-K3, (10) RAP1-PE268-313-E7-NESK 및 (11) RAP1-PE268-313-E7-K3.
<실험예 2> 단백질 발현
융합 단백질 (1) PE313-ORF2-NESK; (2) PE407-ORF2-K3; (3) PE313-E2-NESK; (4) PE407-E2-K3; (5) PE313-VP1-3A-NESK; (6) PE407-VP1-3A-K3; (7) PE313-FHN-NESK; 및 (8) PE407-FHN-K3; (9) PE407-E7-K3; (10) RAP1-PE268-313-E7-NESK 및 (11) RAP1-PE268-313-E7-K3의 발현을 위한 플라스미드를 갖고 있는 E. coli BL21 세포는 37℃의 25 ppm의 가나마이신을 함유하는 루리아 버타니 브로스(Luria Bertani broth)에서 각각 배양하였다. 상기 배양물이 초기 로그 기(log phase)(A600=0.1 내지 0.4)에 도달했을 때, 이소프로필-1-싸이오-β-D-갈락토피라노시드(isopropyl-1-thio-β-D-galactopyranoside; IPTG)를 유도(induction)를 하기 위해 최종 농도가 0.5 내지 2 mM이 되도록 첨가하였다. 배양 후 4시간 후에 세포를 수확하였고 즉시 -70℃에 보관하였다. 상기 융합 단백질은 이전에 기술된 바와 같이(Liao 등, 1995. Appl. Microbiol. Biotechnol. 43: 498-507) 우레아(urea) 추출에 의해 정제하였고 이후 하루 동안 4℃에서 TNE 완충용액(50 mM Tris, 50 mM NaCl 및 1 mM EDTA)의 50배 부피에 대한 투석 방법에 의해 재접힘(refold)하였다. 상기 재접힘된 단백질은 SDS-PAGE 분석에 주어졌고 브래드포드 단백질 분석 키트(Bradford Protein Assay kit(Pierce))를 사용하여 정량 분석을 수행하였다. 상기의 결과는 대부분의 재접힘된 단백질이 비-환원 조건에서 모노머(monomers)라는 것을 나타내는데 이는 융합 단백질이 쉽게 재접힘되고 응집되지 않는다는 것을 나타낸다.
<실험예 3> PCV 소단위 백신 면역성 분석
마우스는 알루미늄 포스페이트(aluminum phosphate)(융합 단백질의 느린 용리를 위한 단백질 흡수체; 10% v/v) 및 10 ㎍의 사포닌(Auillaja saponaria로부터 추출된 아주번트(adjuvant))를 함유하는 40 ㎍의 PE313-ORF2-NESK or PE407-ORF2-K3를 포함하는 0.1 ml의 PCV2 소단위 백신으로 피하(subcutaneous; s.c.) 주사로 3주간 1주일에 한번 백신화하였다. 대조군(플라시보)은 오직 융합 단백질만 없는 아주번트를 주사하였다. 모든 마우스는 마지막 면역화 이후 14일째에 희생하였고, 비장(spleen)을 수확하였다. 상기 비장 세포(splenocyte)는 분리되어, 6-웰 배양접시(108 세포/2 ml/웰)에서 1 ㎍/ml의 GolgiPlug(BD Pharmingen, San Diego, CA)의 존재하에서 재조합 ORF2 단백질과 함께 또는 없이 37 ℃에서 16시간 동안 배양하였다. 상기 자극된 비장 세포는 그 후 FACScan 완충용액으로 세척하였고 피코에리쓰린(phycoerythrin)-결합된 단클론 생쥐 항-마우스 CD8a 및 AF700-결합된 단클론 생쥐 항-마우스 CD4 항체와 함께 염색되었다. 세포는 제조자(BD Pharmingen)의 지시에 따라 Cytofix/Cytoperm 키트를 사용하여 세포내의 사이토카인(cytokine) 염색되었다. 세포내 IFN-γ는 면역 반응 및 사이토카인 수준의 측정을 위해 AF388-결합된 생쥐 항-마우스 IFN-γ로 염색하였다. 유동 세포 분석(flow cytometry analyses)은 Gallios Flow Cytometry와 Kaluza 분석 소프트웨어(Beckman Coulter)를 사용하여 수행하였다.
도 2a 및 b는 각각 플라시보(융합 단백질 없이 오직 아주번트) 또는 융합 단백질로 백신화된 마우스로부터 얻어진 비장세포 안에 존재하는 CD8 및 CD4 양성 IFN-γ T 세포의 개수를 나타낸다. ORF2로 자극된 비장세포 내의 CD4+ 및 CD8+ T 세포에 의한 IFN-γ 생산은 유동 세포 분석을 통한 세포 내의 염색에 의해 확인하였다. 막대 그래프는 ORF2 펩타이드에 의한 자극과 함께(회색 그래프) 또는 없이(흑색 그래프)의 각 그룹으로부터 ORF2-특이적인 IFN-γ+CD4+ T 세포(도 2a) 및 IFN-γ+CD8+ T 세포(도 2b)의 개수를 나타낸다. 상기 결과는 PE313-ORF2-NESK로 백신화된 마우스가 PE407-ORF2-K3 그룹으로 백신화된 마우스보다 ORF2 펩타이드에 의한 자극된 ORF2-특이적인 CD4+IFN-γ+ 및 CD4+IFN-γ+ T 세포를 더 많이 갖고 있음을 나타낸다.
<실험예 4> CSFV 소단위 백신 면역원성 분석
같은 면역화 스케쥴 및 투여량을 사용하여, 마우스는 PE313-E2-NESK 또는 PE407-E2-K3를 포함하는 CSFV 소단위 백신으로 백신화하였고, 비장세포를 분리하여, 배양한 후 배양액 내의 비장세포에 재조합 E2 단백질을 첨가하여 자극하는 것을 제외하고, 상기에 기술된 유동 세포 분석 방법에 의해 분석하였다.
도 3a 및 b는 각각 플라시보(융합 단백질 없이 오직 아주번트) 또는 융합 단백질로 백신화된 마우스로부터 얻어진 비장세포 안에 존재하는 CD8 및 CD4 양성 IFN-γ T 세포의 개수를 나타낸다. E2로 자극된 비장세포 내의 CD4+ 및 CD8+ T 세포에 의한 IFN-γ 생산은 유동 세포 분석을 통한 세포 내의 염색에 의해 확인하였다. 막대 그래프는 E2 펩타이드에 의한 자극과 함께(회색 그래프) 또는 없이(흑색 그래프)의 각 그룹으로부터 E2-특이적인 IFN-γ+CD4+ T 세포(도 3b) 및 IFN-γ+CD8+ T 세포(도 3a)의 개수를 나타낸다. 상기 결과는 PE313-E2-NESK로 백신화된 마우스가 PE407-E2-K3 그룹으로 백신화된 마우스보다 E2 펩타이드에 의한 자극된 E2-특이적인 CD4+IFN-γ+ 및 CD4+IFN-γ+ T 세포를 더 많이 갖고 있음을 나타낸다.
<실험예 5> FMDV 소단위 백신 면역원성 분석
같은 면역화 스케쥴 및 투여량을 사용하여, 마우스는 PE313-VPI-3A-NESK 또는 PE407-VPI-3A-K3를 포함하는 FMDV 소단위 백신으로 백신화하였고, 비장세포를 분리하여, 배양한 후 배양액 내의 비장세포에 재조합 VPI-3A 단백질을 첨가하여 자극하는 것을 제외하고, 상기에 기술된 유동 세포 분석 방법에 의해 분석하였다.
도 4a 및 b는 각각 플라시보(융합 단백질 없이 오직 아주번트) 또는 융합 단백질로 백신화된 마우스로부터 얻어진 비장세포 안에 존재하는 CD8 및 CD4 양성 IFN-γ T 세포의 개수를 나타낸다. VPI-3A로 자극된 비장세포 내의 CD4+ 및 CD8+ T 세포에 의한 IFN-γ 생산은 유동 세포 분석을 통한 세포 내의 염색에 의해 확인하였다. 막대 그래프는 VPI-3A 펩타이드에 의한 자극과 함께(회색 그래프) 또는 없이(흑색 그래프)의 각 그룹으로부터 VPI-3A-특이적인 IFN-γ+CD4+ T 세포(도 4b) 및 IFN-γ+CD8+ T 세포(도 4a)의 개수를 나타낸다. 상기 결과는 PE313-VPI-3A-NESK로 백신화된 마우스가 PE407-VPI-3A-K3 그룹으로 백신화된 마우스보다 VPI-3A 펩타이드에 의한 자극된 VPI-3A-특이적인 CD4+IFN-γ+ 및 CD4+IFN-γ+ T 세포를 더 많이 갖고 있음을 나타낸다.
<실험예 6> NDV 소단위 백신 면역원성 분석
같은 면역화 스케쥴 및 투여량을 사용하여, 마우스는 PE313-FHN-NESK 또는 PE407-FHN-K3를 포함하는 FMDV 소단위 백신으로 백신화하였고, 비장세포를 분리하여, 배양한 후 배양액 내의 비장세포에 재조합 FHN 단백질을 첨가하여 자극하는 것을 제외하고, 상기에 기술된 유동 세포 분석 방법에 의해 분석하였다.
도 5a 및 b는 각각 플라시보(융합 단백질 없이 오직 아주번트) 또는 융합 단백질로 백신화된 마우스로부터 얻어진 비장세포 안에 존재하는 CD8 및 CD4 양성 IFN-γ T 세포의 개수를 나타낸다. FHN로 자극된 비장세포 내의 CD4+ 및 CD8+ T 세포에 의한 IFN-γ 생산은 유동 세포 분석을 통한 세포 내의 염색에 의해 확인하였다. 막대 그래프는 FHN 펩타이드에 의한 자극과 함께(회색 그래프) 또는 없이(흑색 그래프)의 각 그룹으로부터 FHN-특이적인 IFN-γ+CD4+ T 세포(도 5b) 및 IFN-γ+CD8+ T 세포(도 5a)의 개수를 나타낸다. 상기 결과는 PE313-FHN-NESK로 백신화된 마우스가 PE407-FHN-K3 그룹으로 백신화된 마우스보다 FHN 펩타이드에 의한 자극된 FHN-특이적인 CD4+IFN-γ+ 및 CD4+IFN-γ+ T 세포를 더 많이 갖고 있음을 나타낸다.
< 실험예 7> 인간 파필로마 바이러스 타입 16 E7 단백질에 의해 유도된 종양의 성장에 대한 강화된 억제
융합 단백질 PE407-E7-K3, RAP1-PE268-313-E7-K3 및 RAP1-PE268-313-E7-NESK은 상기에 기술된 방법을 사용하여 발현되고 재접힘되었다. 마우스는 HPV-16 타입 암종(carcinoma)을 유도하기 위해 피하 주사를 통해서 2 × 103 TC-01 세포(HPV 타입 16 E7 유전자를 갖고 있는 마우스 폐 상피 세포)를 주사하였다. TC-01 세포 시도 12일 후에, 플라시보(PBS), PE407-E7-K3(100 mg/도스), RAP1-PE268-313-E7-K3(100 ㎍/도스) 또는 RAP1-PE268-313-E7-NESK(100 ㎍/도스)를 아주번트로서 AS04C(GlaxoSmithKline)와 함께 3주 동안 한 주에 한번 백신화하였다(도 6). AS04C는 MPL(모노포스포릴 지방 A(monophosphoryl lipid A), 면역 강화제) 및 알루미늄 포스페이트(aluminum phosphate, 항체 전달을 위한 단백질 흡수제)를 포함하는 세포독성 T 림프구-강화 아주번트이다. 용어 "K3"는 KDEL을 포함하는 ER 유지 서열을 말한다. 예를 들면, K3는 아미노산 서열 KDELKDELKDEL(서열번호 16) 일 수 있다. 용어 "NESK"는 핵 배출 신호 및 ER 유지 서열을 포함하는 융합 펩타이드를 말한다. 본 발명의 한 실시예에서, 상기 NESK는 아미노산 서열 LQKKLEELELAKDEL(서열번호 12)이다. 각 그룹에서 종양의 크기 및 종양-없는 동물의 숫자는 기록되었다(도 7 및 8). 종양의 성장은 아주번트로서 AS04C와 함께 PE407-E7-K3, RAP1-PE268-313-E7-K3 및 RAP1-PE268-313-E7-NESK 백신에 의해 현저하게 억제되었다. 반면, RAP1-PE268-313-E7-NESK 백신은 종양 성장 억제 및 종양-없는 동물의 백분율의 증가에서 PE407-E7-K3보다 뛰어나고 RAP1-PE268-313-E7-K3보다 나았다.
<실험예 8>
하기의 융합 단백질을 제조하였다: PE313-NES-항원-K, PE1-252-PE268-313-NES-항원-K, PE1-252-PE280-313-NES-항원-K. 또한, 융합 단백질 PE313-항원-NESK의 PE 도메인 Ia(PE1-252)의 절편은 각각 RAP1 domain 3-PE253-313-항원-NESK, A2M-PE253-313-항원-NESK, Tat- PE253-313-항원-NESK 및 HSP- PE253-313-항원-NESK, RAP1 domain 3-PE268-313-항원-NESK, A2M-PE268-313-항원-NESK, Tat- PE268-313-항원-NESK 및 HSP- PE268-313-항원-NESK 백신, RAP1 domain 3-PE280-313-항원-NESK, A2M-PE280-313-항원-NESK, Tat- PE280-313-antigen -NESK 및 HSP- PE280-313-항원-NESK를 생성하기 위하여, RAP1 도메인 3(서열번호 8), A2M 최소한(서열번호 9), HIV-Tat 최소한(서열번호 10) 또는 HSPs 최소한(서열번호 11)으로 대체되었다. RAP1 domain 3-PE253-313-NES-항원-K, A2M-PE253-313-NES-항원-K, Tat- PE253-313-NES-항원-K 및 HSP- PE253-313-NES-항원-K, RAP1 도메인 3-PE268-313-NES-항원-K, A2M-PE268-313-NES-항원-K, Tat- PE268-313-NES-항원-K 및 HSP- PE268-313-NES-항원-K 백신, RAP1 도메인 3-PE280-313-NES-항원-K, A2M-PE280-313-NES-항원-K, Tat- PE280-313-NES-항원-K 및 HSP- PE280-313-NES-항원-K. 이러한 백신에 의해 강화된 세포 매개 면역 반응은 상기에 기술된 것과 비슷한 방법을 사용하여 검사하였다.
표 1은 다양한 융합 단백질의 제조를 위해 사용된 펩타이드의 서열번호를 나타낸다.
요소 | 서열번호 | 아미노산 잔기 |
최소의 수도모나스 덱소톡신 A(Pseudomonas exotoxin A; PE) 결합 도메인 Ia(APC-결합 도메인, PE의 a.a.1 내지 a.a.252) |
1 |
252 |
PE253-313 |
2 |
61 |
PE268-313(전좌 도메인) |
3 |
46 |
PEt 중심(PE 전좌 도메인 중심; PE의 a.a.280 내지 a.a.313) |
4 | 34 |
PE313(PE의 a.a.1 내지 a.a.313) |
5 |
313 |
PE253-364 |
6 |
112 |
PE407(PE의 a.a.1 내지 a.a.407) |
7 |
407 |
RAP1 최소한(RAP1의 도메인 III) |
8 |
104 |
A2M 최소한 |
9 |
153 |
HIV-Tat 최소한 |
10 |
24 |
HSPs 최소한 |
11 |
641 |
NESK는 LQKKLEELELA KDEL * |
12 |
15 |
NES 일치 서열은 LxxKLxxLxLx, 여기서 "L"은 루신(leucine), "K"는 라이신(lysine) 및 "X"는 임의의 자연적으로 일어나는 아미노산. |
13 |
11 |
NES는 LQKKLEELELA |
14 |
11 |
KDEL |
15 |
4 |
KDELKDELKDEL(K3) |
16 |
12 |
KKDLRDELKDEL(K3) |
17 |
12 |
KKDELRDELKDEL(K3) |
18 |
13 |
KKDELRVELKDEL(K3) |
19 |
13 |
PCV2 ORF2(돼지 서코바이러스 타입 2 개방 해독 틀 2(Open Reading Frame 2)) |
20 |
192 |
CSFV E2(돼지 콜레라 바이러스 껍질 글리코단백질 E2(Classical Swine Fever Virus Envelope glycoprotein E2)) |
21 |
328 |
FMDV VP1 펩타이드(VP1의 바이러스 캡시드 단백질 a.a.127 내지 a.a.176) |
22 |
50 |
FMDV 3A 펩타이드(3A의 a.a.21내지 35) |
23 |
15 |
FMDV(발-및-입 질병 바이러스)VP1-3A 펩타이드** |
24 |
65 |
NDV F 펩타이드(융합 단백질의 a.a.65 내지 a.a.111) |
25 |
18 |
NDV HN 펩타이드(헤마글루티닌-뉴라미니다제(Hemagglutinin-Neuraminidase) a.a.101 내지 a.a.111) |
26 |
11 |
NDV FHN 펩타이드*** |
27 |
29 |
HPV(인간 파필로마바이러스) 타입 16 E7 |
28 |
98 |
전장 PE(엑소톡신 A, 수도모나스 에루지노사(Exotoxin A, Pseudomonas aeruginosa)) |
29 |
613 |
*: 굵은 글자는 인공의 핵 배출 신호의 아미노산 서열을 나타낸다; 밑줄친 글자는 소포체 유지 신호의 아미노산 서열을 나타낸다.
**: VP1-3A 펩타이드는 VP1의 a.a.127 내지 a.a.176 및 3A의 a.a.21 내지 a.a.35로 구성된 융합 항원이다; 즉, FMDV VP1 펩타이드(서열번호 22) 및 FMDV 3A 펩타이드(서열번호 23)의 융합이다.
***: FHN 펩타이드는 융합 단백질의 a.a.65 내지 a.a.82 및 헤마글루티닌-뉴라미니다제의 a.a.101 내지 a.a.111로 구성된 융합 항원이다; 즉, NDV F 펩타이드(서열번호 25) 및 NDV HN 펩타이드(서열번호 26)의 융합이다.
요약하면, 상기 결과는 병원균의 항원에 이어서 N-말단에 APC-결합 도메인, 전좌 도메인 및 카르복실 말단에 NESK의 융합 펩타이드를 포함하는 융합 단백질은 강화된 세포-매개의 면역 반응, 종양 성장의 억제, 및/또는 종양-없는 동물의 백분율의 증가의 면에서 카르복실 말단에 NESK의 융합 펩타이드가 없는 PE-융합 단백질을 넘어서는 개선된 설계임을 증명하였다.
본 발명의 실시예가 묘사되고 기술되었지만, 당업계에서 숙련된 사람에 의해 다양한 변형 및 개선이 가능할 것이다. 이는 본 발명이 묘사된 것의 특정 형태에 한정되지 않는다는 것이며, 또한 본 발명의 정신 및 범위로부터 벗어나지 않는 모든 변형은 첨부된 청구항에서 정의된 범위 안에 존재한다.
상기 실시예 및 실험예는 고려되는 특정한 사용에 적합한 바와 같이 당업계의 숙련된 다른 사람들이 본 발명 및 다양한 변형과 함께 다양한 실시예를 활용하도록 본 발명의 원리 및 그 실제 적용을 설명하기 위하여 선택되고 기술되었다. 대안적인 실시예는 본 발명의 정신 및 범위로부터 벗어나는 것 없이, 발명이 속하는 기술분야에서 통상의 지식을 가진 자에게 명백해 질 것이다. 따라서, 본 발명의 범위는 앞서 말한 기술 및 본 명세서에 기술된 예시적인 실시예 보다는 첨부된 청구항에 의해 정의된다.
몇몇의 참고문헌, 특허를 포함하여, 특허 출원 및 다양한 출판물은 본 발명의 기술에서 언급되고 논의되었다. 이러한 참고문헌의 언급 및/또는 논의는 본 발명의 기술을 단지 명확하게 하기 위해 제공되었고, 어떠한 참고문헌이 본 명세서에 기술된 본 발명의 "선행 기술"이라는 것을 승인하는 것이 아니다. 본 명세서에 언급되고 논의된 모든 참고문헌은 그 전체가 참조에 의해 각각 개별적으로 참고문헌이 참고로 인용된 것과 동일한 정도로 본 명세서에 포함된다.
<110> TheVax Genetics Vaccine Co., Ltd.
<120> FUSION PROTEINS FOR ENHANCING CELL-MEDIATED IMMUNE RESPONSES
<130> 2016FPI-10-002
<150> 61733879
<151> 2012-12-05
<160> 29
<170> PatentIn version 3.5
<210> 1
<211> 252
<212> PRT
<213> Pseudomonas aeruginosa
<400> 1
Ala Glu Glu Ala Phe Asp Leu Trp Asn Glu Cys Ala Lys Ala Cys Val
1 5 10 15
Leu Asp Leu Lys Asp Gly Val Arg Ser Ser Arg Met Ser Val Asp Pro
20 25 30
Ala Ile Ala Asp Thr Asn Gly Gln Gly Val Leu His Tyr Ser Met Val
35 40 45
Leu Glu Gly Gly Asn Asp Ala Leu Lys Leu Ala Ile Asp Asn Ala Leu
50 55 60
Ser Ile Thr Ser Asp Gly Leu Thr Ile Arg Leu Glu Gly Gly Val Glu
65 70 75 80
Pro Asn Lys Pro Val Arg Tyr Ser Tyr Thr Arg Gln Ala Arg Gly Ser
85 90 95
Trp Ser Leu Asn Trp Leu Val Pro Ile Gly His Glu Lys Pro Ser Asn
100 105 110
Ile Lys Val Phe Ile His Glu Leu Asn Ala Gly Asn Gln Leu Ser His
115 120 125
Met Ser Pro Ile Tyr Thr Ile Glu Met Gly Asp Glu Leu Leu Ala Lys
130 135 140
Leu Ala Arg Asp Ala Thr Phe Phe Val Arg Ala His Glu Ser Asn Glu
145 150 155 160
Met Gln Pro Thr Leu Ala Ile Ser His Ala Gly Val Ser Val Val Met
165 170 175
Ala Gln Thr Gln Pro Arg Arg Glu Lys Arg Trp Ser Glu Trp Ala Ser
180 185 190
Gly Lys Val Leu Cys Leu Leu Asp Pro Leu Asp Gly Val Tyr Asn Tyr
195 200 205
Leu Ala Gln Gln Arg Cys Asn Leu Asp Asp Thr Trp Glu Gly Lys Ile
210 215 220
Tyr Arg Val Leu Ala Gly Asn Pro Ala Lys His Asp Leu Asp Ile Lys
225 230 235 240
Pro Thr Val Ile Ser His Arg Leu His Phe Pro Glu
245 250
<210> 2
<211> 61
<212> PRT
<213> Pseudomonas aeruginosa
<400> 2
Gly Gly Ser Leu Ala Ala Leu Thr Ala His Gln Ala Cys His Leu Pro
1 5 10 15
Leu Glu Thr Phe Thr Arg His Arg Gln Pro Arg Gly Trp Glu Gln Leu
20 25 30
Glu Gln Cys Gly Tyr Pro Val Gln Arg Leu Val Ala Leu Tyr Leu Ala
35 40 45
Ala Arg Leu Ser Trp Asn Gln Val Asp Gln Val Ile Arg
50 55 60
<210> 3
<211> 46
<212> PRT
<213> Pseudomonas aeruginosa
<400> 3
Pro Leu Glu Thr Phe Thr Arg His Arg Gln Pro Arg Gly Trp Glu Gln
1 5 10 15
Leu Glu Gln Cys Gly Tyr Pro Val Gln Arg Leu Val Ala Leu Tyr Leu
20 25 30
Ala Ala Arg Leu Ser Trp Asn Gln Val Asp Gln Val Ile Arg
35 40 45
<210> 4
<211> 34
<212> PRT
<213> Pseudomonas aeruginosa
<400> 4
Gly Trp Glu Gln Leu Glu Gln Cys Gly Tyr Pro Val Gln Arg Leu Val
1 5 10 15
Ala Leu Tyr Leu Ala Ala Arg Leu Ser Trp Asn Gln Val Asp Gln Val
20 25 30
Ile Arg
<210> 5
<211> 313
<212> PRT
<213> Pseudomonas aeruginosa
<400> 5
Ala Glu Glu Ala Phe Asp Leu Trp Asn Glu Cys Ala Lys Ala Cys Val
1 5 10 15
Leu Asp Leu Lys Asp Gly Val Arg Ser Ser Arg Met Ser Val Asp Pro
20 25 30
Ala Ile Ala Asp Thr Asn Gly Gln Gly Val Leu His Tyr Ser Met Val
35 40 45
Leu Glu Gly Gly Asn Asp Ala Leu Lys Leu Ala Ile Asp Asn Ala Leu
50 55 60
Ser Ile Thr Ser Asp Gly Leu Thr Ile Arg Leu Glu Gly Gly Val Glu
65 70 75 80
Pro Asn Lys Pro Val Arg Tyr Ser Tyr Thr Arg Gln Ala Arg Gly Ser
85 90 95
Trp Ser Leu Asn Trp Leu Val Pro Ile Gly His Glu Lys Pro Ser Asn
100 105 110
Ile Lys Val Phe Ile His Glu Leu Asn Ala Gly Asn Gln Leu Ser His
115 120 125
Met Ser Pro Ile Tyr Thr Ile Glu Met Gly Asp Glu Leu Leu Ala Lys
130 135 140
Leu Ala Arg Asp Ala Thr Phe Phe Val Arg Ala His Glu Ser Asn Glu
145 150 155 160
Met Gln Pro Thr Leu Ala Ile Ser His Ala Gly Val Ser Val Val Met
165 170 175
Ala Gln Thr Gln Pro Arg Arg Glu Lys Arg Trp Ser Glu Trp Ala Ser
180 185 190
Gly Lys Val Leu Cys Leu Leu Asp Pro Leu Asp Gly Val Tyr Asn Tyr
195 200 205
Leu Ala Gln Gln Arg Cys Asn Leu Asp Asp Thr Trp Glu Gly Lys Ile
210 215 220
Tyr Arg Val Leu Ala Gly Asn Pro Ala Lys His Asp Leu Asp Ile Lys
225 230 235 240
Pro Thr Val Ile Ser His Arg Leu His Phe Pro Glu Gly Gly Ser Leu
245 250 255
Ala Ala Leu Thr Ala His Gln Ala Cys His Leu Pro Leu Glu Thr Phe
260 265 270
Thr Arg His Arg Gln Pro Arg Gly Trp Glu Gln Leu Glu Gln Cys Gly
275 280 285
Tyr Pro Val Gln Arg Leu Val Ala Leu Tyr Leu Ala Ala Arg Leu Ser
290 295 300
Trp Asn Gln Val Asp Gln Val Ile Arg
305 310
<210> 6
<211> 112
<212> PRT
<213> Pseudomonas aeruginosa
<400> 6
Gly Gly Ser Leu Ala Ala Leu Thr Ala His Gln Ala Cys His Leu Pro
1 5 10 15
Leu Glu Thr Phe Thr Arg His Arg Gln Pro Arg Gly Trp Glu Gln Leu
20 25 30
Glu Gln Cys Gly Tyr Pro Val Gln Arg Leu Val Ala Leu Tyr Leu Ala
35 40 45
Ala Arg Leu Ser Trp Asn Gln Val Asp Gln Val Ile Arg Asn Ala Leu
50 55 60
Ala Ser Pro Gly Ser Gly Gly Asp Leu Gly Glu Ala Ile Arg Glu Gln
65 70 75 80
Pro Glu Gln Ala Arg Leu Ala Leu Thr Leu Ala Ala Ala Glu Ser Glu
85 90 95
Arg Phe Val Arg Gln Gly Thr Gly Asn Asp Glu Ala Gly Ala Ala Asn
100 105 110
<210> 7
<211> 407
<212> PRT
<213> Pseudomonas aeruginosa
<400> 7
Ala Glu Glu Ala Phe Asp Leu Trp Asn Glu Cys Ala Lys Ala Cys Val
1 5 10 15
Leu Asp Leu Lys Asp Gly Val Arg Ser Ser Arg Met Ser Val Asp Pro
20 25 30
Ala Ile Ala Asp Thr Asn Gly Gln Gly Val Leu His Tyr Ser Met Val
35 40 45
Leu Glu Gly Gly Asn Asp Ala Leu Lys Leu Ala Ile Asp Asn Ala Leu
50 55 60
Ser Ile Thr Ser Asp Gly Leu Thr Ile Arg Leu Glu Gly Gly Val Glu
65 70 75 80
Pro Asn Lys Pro Val Arg Tyr Ser Tyr Thr Arg Gln Ala Arg Gly Ser
85 90 95
Trp Ser Leu Asn Trp Leu Val Pro Ile Gly His Glu Lys Pro Ser Asn
100 105 110
Ile Lys Val Phe Ile His Glu Leu Asn Ala Gly Asn Gln Leu Ser His
115 120 125
Met Ser Pro Ile Tyr Thr Ile Glu Met Gly Asp Glu Leu Leu Ala Lys
130 135 140
Leu Ala Arg Asp Ala Thr Phe Phe Val Arg Ala His Glu Ser Asn Glu
145 150 155 160
Met Gln Pro Thr Leu Ala Ile Ser His Ala Gly Val Ser Val Val Met
165 170 175
Ala Gln Thr Gln Pro Arg Arg Glu Lys Arg Trp Ser Glu Trp Ala Ser
180 185 190
Gly Lys Val Leu Cys Leu Leu Asp Pro Leu Asp Gly Val Tyr Asn Tyr
195 200 205
Leu Ala Gln Gln Arg Cys Asn Leu Asp Asp Thr Trp Glu Gly Lys Ile
210 215 220
Tyr Arg Val Leu Ala Gly Asn Pro Ala Lys His Asp Leu Asp Ile Lys
225 230 235 240
Pro Thr Val Ile Ser His Arg Leu His Phe Pro Glu Gly Gly Ser Leu
245 250 255
Ala Ala Leu Thr Ala His Gln Ala Cys His Leu Pro Leu Glu Thr Phe
260 265 270
Thr Arg His Arg Gln Pro Arg Gly Trp Glu Gln Leu Glu Gln Cys Gly
275 280 285
Tyr Pro Val Gln Arg Leu Val Ala Leu Tyr Leu Ala Ala Arg Leu Ser
290 295 300
Trp Asn Gln Val Asp Gln Val Ile Arg Asn Ala Leu Ala Ser Pro Gly
305 310 315 320
Ser Gly Gly Asp Leu Gly Glu Ala Ile Arg Glu Gln Pro Glu Gln Ala
325 330 335
Arg Leu Ala Leu Thr Leu Ala Ala Ala Glu Ser Glu Arg Phe Val Arg
340 345 350
Gln Gly Thr Gly Asn Asp Glu Ala Gly Ala Ala Asn Ala Asp Val Val
355 360 365
Ser Leu Thr Cys Pro Val Ala Ala Gly Glu Cys Ala Gly Pro Ala Asp
370 375 380
Ser Gly Asp Ala Leu Leu Glu Arg Asn Tyr Pro Thr Gly Ala Glu Phe
385 390 395 400
Leu Gly Asp Gly Gly Asp Val
405
<210> 8
<211> 104
<212> PRT
<213> Homo sapiens
<400> 8
Ala Glu Phe Glu Glu Pro Arg Val Ile Asp Leu Trp Asp Leu Ala Gln
1 5 10 15
Ser Ala Asn Leu Thr Asp Lys Glu Leu Glu Ala Phe Arg Glu Glu Leu
20 25 30
Lys His Phe Glu Ala Lys Ile Glu Lys His Asn His Tyr Gln Lys Gln
35 40 45
Leu Glu Ile Ala His Glu Lys Leu Arg His Ala Glu Ser Val Gly Asp
50 55 60
Gly Glu Arg Val Ser Arg Ser Arg Glu Lys His Ala Leu Leu Glu Gly
65 70 75 80
Arg Thr Lys Glu Leu Gly Tyr Thr Val Lys Lys His Leu Gln Asp Leu
85 90 95
Ser Gly Arg Ile Ser Arg Ala Arg
100
<210> 9
<211> 153
<212> PRT
<213> Artificial Sequence
<220>
<223> A2M Minimum
<400> 9
Val Tyr Leu Gln Thr Ser Leu Lys Tyr Asn Ile Leu Pro Glu Lys Glu
1 5 10 15
Glu Phe Pro Phe Ala Leu Gly Val Gln Thr Leu Pro Gln Thr Cys Asp
20 25 30
Glu Pro Lys Ala His Thr Ser Phe Gln Ile Ser Leu Ser Val Ser Tyr
35 40 45
Thr Gly Ser Arg Ser Ala Ser Asn Met Ala Ile Val Asp Val Lys Met
50 55 60
Val Ser Gly Phe Ile Pro Leu Lys Pro Thr Val Lys Met Leu Glu Arg
65 70 75 80
Ser Asn His Val Ser Arg Thr Glu Val Ser Ser Asn His Val Leu Ile
85 90 95
Tyr Leu Asp Lys Val Ser Asn Gln Thr Leu Ser Leu Phe Phe Thr Val
100 105 110
Leu Gln Asp Val Pro Val Arg Asp Leu Lys Pro Ala Ile Val Lys Val
115 120 125
Tyr Asp Tyr Tyr Glu Thr Asp Glu Phe Ala Ile Ala Glu Tyr Asn Ala
130 135 140
Pro Cys Ser Lys Asp Leu Gly Asn Ala
145 150
<210> 10
<211> 24
<212> PRT
<213> Artificial Sequence
<220>
<223> HIV-Tat Minimum
<400> 10
Arg Gly Asp Pro Thr Gly Gln Glu Glu Ser Lys Glu Lys Val Glu Lys
1 5 10 15
Glu Thr Val Val Asp Pro Val Thr
20
<210> 11
<211> 641
<212> PRT
<213> Artificial Sequence
<220>
<223> HSPs Minimum
<400> 11
Met Ala Lys Ala Ala Ala Ile Gly Ile Asp Leu Gly Thr Thr Tyr Ser
1 5 10 15
Cys Val Gly Val Phe Gln His Gly Lys Val Glu Ile Ile Ala Asn Asp
20 25 30
Gln Gly Asn Arg Thr Thr Pro Ser Tyr Val Ala Phe Thr Asp Thr Glu
35 40 45
Arg Leu Ile Gly Asp Ala Ala Lys Asn Gln Val Ala Leu Asn Pro Gln
50 55 60
Asn Thr Val Phe Asp Ala Lys Arg Leu Ile Gly Arg Lys Phe Gly Asp
65 70 75 80
Pro Val Val Gln Ser Asp Met Lys His Trp Pro Phe Gln Val Ile Asn
85 90 95
Asp Gly Asp Lys Pro Lys Val Gln Val Ser Tyr Lys Gly Glu Thr Lys
100 105 110
Ala Phe Tyr Pro Glu Glu Ile Ser Ser Met Val Leu Thr Lys Met Lys
115 120 125
Glu Ile Ala Glu Ala Tyr Leu Gly Tyr Pro Val Thr Asn Ala Val Ile
130 135 140
Thr Val Pro Ala Tyr Phe Asn Asp Ser Gln Arg Gln Ala Thr Lys Asp
145 150 155 160
Ala Gly Val Ile Ala Gly Leu Asn Val Leu Arg Ile Ile Asn Glu Pro
165 170 175
Thr Ala Ala Ala Ile Ala Tyr Gly Leu Asp Arg Thr Gly Lys Gly Glu
180 185 190
Arg Asn Val Leu Ile Phe Asp Leu Gly Gly Gly Thr Phe Asp Val Ser
195 200 205
Ile Leu Thr Ile Asp Asp Gly Ile Phe Glu Val Lys Ala Thr Ala Gly
210 215 220
Asp Thr His Leu Gly Gly Glu Asp Phe Asp Asn Arg Leu Val Asn His
225 230 235 240
Phe Val Glu Glu Phe Lys Arg Lys His Lys Lys Asp Ile Ser Gln Asn
245 250 255
Lys Arg Ala Val Arg Arg Leu Arg Thr Ala Cys Glu Arg Ala Lys Arg
260 265 270
Thr Leu Ser Ser Ser Thr Gln Ala Ser Leu Glu Ile Asp Ser Leu Phe
275 280 285
Glu Gly Ile Asp Phe Tyr Thr Ser Ile Thr Arg Ala Arg Phe Glu Glu
290 295 300
Leu Cys Ser Asp Leu Phe Arg Ser Thr Leu Glu Pro Val Glu Lys Ala
305 310 315 320
Leu Arg Asp Ala Lys Leu Asp Lys Ala Gln Ile His Asp Leu Val Leu
325 330 335
Val Gly Gly Ser Thr Arg Ile Pro Lys Val Gln Lys Leu Leu Gln Asp
340 345 350
Phe Phe Asn Gly Arg Asp Leu Asn Lys Ser Ile Asn Pro Asp Glu Ala
355 360 365
Val Ala Tyr Gly Ala Ala Val Gln Ala Ala Ile Leu Met Gly Asp Lys
370 375 380
Ser Glu Asn Val Gln Asp Leu Leu Leu Leu Asp Val Ala Pro Leu Ser
385 390 395 400
Leu Gly Leu Glu Thr Ala Gly Gly Val Met Thr Ala Leu Ile Lys Arg
405 410 415
Asn Ser Thr Ile Pro Thr Lys Gln Thr Gln Ile Phe Thr Thr Tyr Ser
420 425 430
Asp Asn Gln Pro Gly Val Leu Ile Gln Val Tyr Glu Gly Glu Arg Ala
435 440 445
Met Thr Lys Asp Asn Asn Leu Leu Gly Arg Phe Glu Leu Ser Gly Ile
450 455 460
Pro Pro Ala Pro Arg Gly Val Pro Gln Ile Glu Val Thr Phe Asp Ile
465 470 475 480
Asp Ala Asn Gly Ile Leu Asn Val Thr Ala Thr Asp Lys Ser Thr Gly
485 490 495
Lys Ala Asn Lys Ile Thr Ile Thr Asn Asp Lys Gly Arg Leu Ser Lys
500 505 510
Glu Glu Ile Glu Arg Met Val Gln Glu Ala Glu Lys Tyr Lys Ala Glu
515 520 525
Asp Glu Val Gln Arg Glu Arg Val Ser Ala Lys Asn Ala Leu Glu Ser
530 535 540
Tyr Ala Phe Asn Met Lys Ser Ala Val Glu Asp Glu Gly Leu Lys Gly
545 550 555 560
Lys Ile Ser Glu Ala Asp Lys Lys Lys Val Leu Asp Lys Cys Gln Glu
565 570 575
Val Ile Ser Trp Leu Asp Ala Asn Thr Leu Ala Glu Lys Asp Glu Phe
580 585 590
Glu His Lys Arg Lys Glu Leu Glu Gln Val Cys Asn Pro Ile Ile Ser
595 600 605
Gly Leu Tyr Gln Gly Ala Gly Gly Pro Gly Pro Gly Gly Phe Gly Ala
610 615 620
Gln Gly Pro Lys Gly Gly Ser Gly Ser Gly Pro Thr Ile Glu Glu Val
625 630 635 640
Asp
<210> 12
<211> 15
<212> PRT
<213> Artificial Sequence
<220>
<223> NESK
<400> 12
Leu Gln Lys Lys Leu Glu Glu Leu Glu Leu Ala Lys Asp Glu Leu
1 5 10 15
<210> 13
<211> 11
<212> PRT
<213> Artificial Sequence
<220>
<223> NES consensus sequence
<220>
<221> MISC_FEATURE
<222> (2)..(3)
<223> Xaa can be any naturally occurring amino acid
<220>
<221> MISC_FEATURE
<222> (6)..(7)
<223> Xaa can be any naturally occurring amino acid
<220>
<221> MISC_FEATURE
<222> (9)
<223> Xaa can be any naturally occurring amino acid
<220>
<221> MISC_FEATURE
<222> (11)
<223> Xaa can be any naturally occurring amino acid
<400> 13
Leu Xaa Xaa Lys Leu Xaa Xaa Leu Xaa Leu Xaa
1 5 10
<210> 14
<211> 11
<212> PRT
<213> Artificial Sequence
<220>
<223> NES
<400> 14
Leu Gln Lys Lys Leu Glu Glu Leu Glu Leu Ala
1 5 10
<210> 15
<211> 4
<212> PRT
<213> Artificial Sequence
<220>
<223> ER retention sequence
<400> 15
Lys Asp Glu Leu
1
<210> 16
<211> 12
<212> PRT
<213> Artificial Sequence
<220>
<223> K3
<400> 16
Lys Asp Glu Leu Lys Asp Glu Leu Lys Asp Glu Leu
1 5 10
<210> 17
<211> 12
<212> PRT
<213> Artificial Sequence
<220>
<223> K3
<400> 17
Lys Lys Asp Leu Arg Asp Glu Leu Lys Asp Glu Leu
1 5 10
<210> 18
<211> 13
<212> PRT
<213> Artificial Sequence
<220>
<223> K3
<400> 18
Lys Lys Asp Glu Leu Arg Asp Glu Leu Lys Asp Glu Leu
1 5 10
<210> 19
<211> 13
<212> PRT
<213> Artificial Sequence
<220>
<223> K3
<400> 19
Lys Lys Asp Glu Leu Arg Val Glu Leu Lys Asp Glu Leu
1 5 10
<210> 20
<211> 192
<212> PRT
<213> Artificial Sequence
<220>
<223> truncated PCV2 ORF2
<400> 20
Asn Gly Ile Phe Asn Thr Arg Leu Ser Arg Thr Phe Gly Tyr Thr Ile
1 5 10 15
Lys Arg Thr Thr Val Lys Thr Pro Ser Trp Ala Val Asp Met Met Arg
20 25 30
Phe Asn Ile Asn Asp Phe Leu Pro Pro Gly Gly Gly Ser Asn Pro Arg
35 40 45
Ser Val Pro Phe Glu Tyr Tyr Ser Ile Ser Lys Val Lys Val Glu Phe
50 55 60
Trp Pro Cys Ser Pro Ile Thr Gln Gly Asp Ser Gly Val Gly Ser Ser
65 70 75 80
Ala Val Ile Leu Asp Asp Asn Phe Val Thr Lys Ala Thr Ala Leu Thr
85 90 95
Tyr Asp Pro Tyr Val Asn Tyr Ser Ser Arg His Thr Ile Thr Gln Pro
100 105 110
Phe Ser Tyr His Ser Arg Tyr Phe Thr Pro Lys Pro Val Leu Asp Ser
115 120 125
Thr Ile Asp Tyr Phe Gln Pro Asn Asn Lys Arg Asn Gln Leu Trp Leu
130 135 140
Arg Leu Gln Thr Ala Gly Asn Val Asp His Val Gly Leu Gly Thr Ala
145 150 155 160
Phe Glu Asn Ser Ile Tyr Asp Gln Glu Tyr Asn Ile Arg Val Thr Met
165 170 175
Tyr Val Gln Phe Arg Glu Phe Asn Leu Lys Asp Pro Pro Leu Asn Pro
180 185 190
<210> 21
<211> 328
<212> PRT
<213> Artificial Sequence
<220>
<223> truncated CSFV E2
<400> 21
Arg Leu Ser Cys Lys Glu Asp His Arg Tyr Ala Ile Ser Ser Thr Asn
1 5 10 15
Glu Ile Gly Pro Leu Gly Ala Glu Gly Leu Thr Thr Thr Trp Lys Glu
20 25 30
Tyr Ser His Gly Leu Gln Leu Asp Asp Gly Thr Val Arg Ala Ile Cys
35 40 45
Ile Ala Gly Ser Phe Lys Val Thr Ala Leu Asn Val Val Ser Arg Arg
50 55 60
Tyr Leu Ala Ser Leu His Lys Arg Ala Leu Pro Thr Ser Val Thr Phe
65 70 75 80
Glu Leu Leu Phe Asp Gly Thr Ser Pro Ala Ile Glu Glu Met Gly Glu
85 90 95
Asp Phe Gly Phe Gly Leu Cys Pro Phe Asp Thr Thr Pro Val Val Lys
100 105 110
Gly Lys Tyr Asn Thr Thr Leu Leu Asn Gly Ser Ala Phe Tyr Leu Val
115 120 125
Cys Pro Ile Gly Trp Thr Gly Val Ile Glu Cys Thr Ala Val Ser Pro
130 135 140
Thr Thr Leu Arg Thr Glu Val Val Lys Thr Phe Lys Arg Glu Lys Pro
145 150 155 160
Phe Pro His Arg Ala Asp Cys Val Thr Thr Ile Val Glu Lys Glu Asp
165 170 175
Leu Phe His Cys Lys Leu Gly Gly Asn Trp Thr Cys Val Lys Gly Asn
180 185 190
Pro Val Thr Tyr Thr Gly Gly Gln Val Lys Gln Cys Arg Trp Cys Gly
195 200 205
Phe Asp Phe Lys Glu Pro Asp Gly Leu Pro His Tyr Pro Ile Gly Lys
210 215 220
Cys Ile Leu Ala Asn Glu Thr Gly Tyr Arg Val Val Asp Ser Thr Asp
225 230 235 240
Cys Asn Arg Asp Gly Val Val Ile Ser Thr Glu Gly Glu His Glu Cys
245 250 255
Leu Ile Gly Asn Thr Thr Val Lys Val His Ala Leu Asp Gly Arg Leu
260 265 270
Ala Pro Met Pro Cys Arg Pro Lys Glu Ile Val Ser Ser Ala Gly Pro
275 280 285
Val Arg Lys Thr Ser Cys Thr Phe Asn Tyr Thr Lys Thr Leu Arg Asn
290 295 300
Lys Tyr Tyr Glu Pro Arg Asp Ser Tyr Phe Gln Gln Tyr Met Leu Lys
305 310 315 320
Gly Glu Tyr Gln Tyr Trp Phe Asp
325
<210> 22
<211> 50
<212> PRT
<213> Artificial Sequence
<220>
<223> FMDV VP1 peptide
<400> 22
Ala Thr Val Tyr Asn Gly Ser Ser Lys Tyr Gly Asp Thr Ser Thr Ser
1 5 10 15
Asn Val Arg Gly Asp Leu Gln Val Leu Ala Gln Lys Ala Glu Arg Thr
20 25 30
Leu Pro Thr Ser Phe Asn Phe Gly Ala Ile Lys Ala Thr Arg Val Thr
35 40 45
Glu Leu
50
<210> 23
<211> 15
<212> PRT
<213> Artificial Sequence
<220>
<223> FMDV 3A peptide
<400> 23
Ala Ala Ile Glu Phe Phe Glu Gly Met Val His Asp Ser Ile Lys
1 5 10 15
<210> 24
<211> 65
<212> PRT
<213> Artificial Sequence
<220>
<223> FMDV VP1-3A peptide
<400> 24
Ala Thr Val Tyr Asn Gly Ser Ser Lys Tyr Gly Asp Thr Ser Thr Ser
1 5 10 15
Asn Val Arg Gly Asp Leu Gln Val Leu Ala Gln Lys Ala Glu Arg Thr
20 25 30
Leu Pro Thr Ser Phe Asn Phe Gly Ala Ile Lys Ala Thr Arg Val Thr
35 40 45
Glu Leu Ala Ala Ile Glu Phe Phe Glu Gly Met Val His Asp Ser Ile
50 55 60
Lys
65
<210> 25
<211> 18
<212> PRT
<213> Artificial Sequence
<220>
<223> NDV F peptide
<400> 25
Leu Leu Pro Asn Met Pro Lys Asp Lys Glu Gly Cys Ala Lys Ala Pro
1 5 10 15
Leu Glu
<210> 26
<211> 11
<212> PRT
<213> Artificial Sequence
<220>
<223> NDV HN peptide
<400> 26
Pro Asp Glu Gln Asp Tyr Gln Ile Arg Met Ala
1 5 10
<210> 27
<211> 29
<212> PRT
<213> Artificial Sequence
<220>
<223> NDV FHN peptide
<400> 27
Leu Leu Pro Asn Met Pro Lys Asp Lys Glu Gly Cys Ala Lys Ala Pro
1 5 10 15
Leu Glu Pro Asp Glu Gln Asp Tyr Gln Ile Arg Met Ala
20 25
<210> 28
<211> 98
<212> PRT
<213> Human papillomavirus type 16
<400> 28
Met His Gly Asp Thr Pro Thr Leu His Glu Tyr Met Leu Asp Leu Gln
1 5 10 15
Pro Glu Thr Thr Asp Leu Tyr Cys Tyr Glu Gln Leu Asn Asp Ser Ser
20 25 30
Glu Glu Glu Asp Glu Ile Asp Gly Pro Ala Gly Gln Ala Glu Pro Asp
35 40 45
Arg Ala His Tyr Asn Ile Val Thr Phe Cys Cys Lys Cys Asp Ser Thr
50 55 60
Leu Arg Leu Cys Val Gln Ser Thr His Val Asp Ile Arg Thr Leu Glu
65 70 75 80
Asp Leu Leu Met Gly Thr Leu Gly Ile Val Cys Pro Ile Cys Ser Gln
85 90 95
Lys Pro
<210> 29
<211> 613
<212> PRT
<213> Pseudomonas aeruginosa
<400> 29
Ala Glu Glu Ala Phe Asp Leu Trp Asn Glu Cys Ala Lys Ala Cys Val
1 5 10 15
Leu Asp Leu Lys Asp Gly Val Arg Ser Ser Arg Met Ser Val Asp Pro
20 25 30
Ala Ile Ala Asp Thr Asn Gly Gln Gly Val Leu His Tyr Ser Met Val
35 40 45
Leu Glu Gly Gly Asn Asp Ala Leu Lys Leu Ala Ile Asp Asn Ala Leu
50 55 60
Ser Ile Thr Ser Asp Gly Leu Thr Ile Arg Leu Glu Gly Gly Val Glu
65 70 75 80
Pro Asn Lys Pro Val Arg Tyr Ser Tyr Thr Arg Gln Ala Arg Gly Ser
85 90 95
Trp Ser Leu Asn Trp Leu Val Pro Ile Gly His Glu Lys Pro Ser Asn
100 105 110
Ile Lys Val Phe Ile His Glu Leu Asn Ala Gly Asn Gln Leu Ser His
115 120 125
Met Ser Pro Ile Tyr Thr Ile Glu Met Gly Asp Glu Leu Leu Ala Lys
130 135 140
Leu Ala Arg Asp Ala Thr Phe Phe Val Arg Ala His Glu Ser Asn Glu
145 150 155 160
Met Gln Pro Thr Leu Ala Ile Ser His Ala Gly Val Ser Val Val Met
165 170 175
Ala Gln Thr Gln Pro Arg Arg Glu Lys Arg Trp Ser Glu Trp Ala Ser
180 185 190
Gly Lys Val Leu Cys Leu Leu Asp Pro Leu Asp Gly Val Tyr Asn Tyr
195 200 205
Leu Ala Gln Gln Arg Cys Asn Leu Asp Asp Thr Trp Glu Gly Lys Ile
210 215 220
Tyr Arg Val Leu Ala Gly Asn Pro Ala Lys His Asp Leu Asp Ile Lys
225 230 235 240
Pro Thr Val Ile Ser His Arg Leu His Phe Pro Glu Gly Gly Ser Leu
245 250 255
Ala Ala Leu Thr Ala His Gln Ala Cys His Leu Pro Leu Glu Thr Phe
260 265 270
Thr Arg His Arg Gln Pro Arg Gly Trp Glu Gln Leu Glu Gln Cys Gly
275 280 285
Tyr Pro Val Gln Arg Leu Val Ala Leu Tyr Leu Ala Ala Arg Leu Ser
290 295 300
Trp Asn Gln Val Asp Gln Val Ile Arg Asn Ala Leu Ala Ser Pro Gly
305 310 315 320
Ser Gly Gly Asp Leu Gly Glu Ala Ile Arg Glu Gln Pro Glu Gln Ala
325 330 335
Arg Leu Ala Leu Thr Leu Ala Ala Ala Glu Ser Glu Arg Phe Val Arg
340 345 350
Gln Gly Thr Gly Asn Asp Glu Ala Gly Ala Ala Asn Ala Asp Val Val
355 360 365
Ser Leu Thr Cys Pro Val Ala Ala Gly Glu Cys Ala Gly Pro Ala Asp
370 375 380
Ser Gly Asp Ala Leu Leu Glu Arg Asn Tyr Pro Thr Gly Ala Glu Phe
385 390 395 400
Leu Gly Asp Gly Gly Asp Val Ser Phe Ser Thr Arg Gly Thr Gln Asn
405 410 415
Trp Thr Val Glu Arg Leu Leu Gln Ala His Arg Gln Leu Glu Glu Arg
420 425 430
Gly Tyr Val Phe Val Gly Tyr His Gly Thr Phe Leu Glu Ala Ala Gln
435 440 445
Ser Ile Val Phe Gly Gly Val Arg Ala Arg Ser Gln Asp Leu Asp Ala
450 455 460
Ile Trp Arg Gly Phe Tyr Ile Ala Gly Asp Pro Ala Leu Ala Tyr Gly
465 470 475 480
Tyr Ala Gln Asp Gln Glu Pro Asp Ala Arg Gly Arg Ile Arg Asn Gly
485 490 495
Ala Leu Leu Arg Val Tyr Val Pro Arg Ser Ser Leu Pro Gly Phe Tyr
500 505 510
Arg Thr Ser Leu Thr Leu Ala Ala Pro Glu Ala Ala Gly Glu Val Glu
515 520 525
Arg Leu Ile Gly His Pro Leu Pro Leu Arg Leu Asp Ala Ile Thr Gly
530 535 540
Pro Glu Glu Glu Gly Gly Arg Leu Glu Thr Ile Leu Gly Trp Pro Leu
545 550 555 560
Ala Glu Arg Thr Val Val Ile Pro Ser Ala Ile Pro Thr Asp Pro Arg
565 570 575
Asn Val Gly Gly Asp Leu Asp Pro Ser Ser Ile Pro Asp Lys Glu Gln
580 585 590
Ala Ile Ser Ala Leu Pro Asp Tyr Ala Ser Gln Pro Gly Lys Pro Pro
595 600 605
Arg Glu Asp Leu Lys
610
Claims (19)
- 하기로 구성되는 융합 단백질:
(a) 융합 단백질의 N-말단(terminus)에 위치한 항원-제시 세포(antigen-presenting cell; APC)-결합 도메인(domain) 또는 CD91 수용체-결합 도메인;
(b) APC-결합 도메인 또는 CD91 수용체-결합 도메인의 C-말단에 위치한 서열번호 4, 2, 3, 또는 6의 아미노산 서열을 포함하는, 34 내지 112 아미노산 잔기 길이의 전좌(translocation) 펩타이드(peptide); 및
(c) 병원균(pathogen) 또는 암 세포의 항원;
(d) 융합 단백질의 C-말단에 위치한 골지체(endoplasmic reticulum) 유지 서열; 및
(e) 항원 및 골지체 유지 서열 사이에 위치하거나, 또는 전좌 펩타이드 및 항원사이에 위치하는 핵 배출 신호(nuclear export signal)로서, 핵 배출 신호는 서열번호 13의 아미노산 서열을 포함하고, 상기 서열번호 13의 C-말단 아미노산은 알라닌인;
여기서:
상기 병원균은 인간 파필로마바이러스(Human Papillomavirus; HPV), 돼지 재생산 및 호흡 증후군 바이러스(Porcine reproductive and respiratory syndrome virus; PRRSV), 인간 면역결핍 바이러스-1(Human immunodeficiency virus-1; HIV-1), 댕기 바이러스(Dangue virus), C형 간염 바이러스(Hepatitis C virus; HCV), B형 간염 바이러스(Hepatitis B virus; HBV), 돼지 서코바이러스(Porcine Circovirus 2; PCV2), 돼지 콜레라 바이러스(Classical Swine Fever Virus; CSFV), 발-및-입 질병 바이러스(Foot-and-Mouth disease virus; FMDV), 뉴캐슬 질병 바이러스(Newcastle disease virus; NDV), 전염성 위장염 바이러스(Transmissible gastroenteritis virus; TGEV), 돼지 유행성 설사 바이러스(Porcine epidemic diarrhea virus; PEDV), 인플루엔자 바이러스(Influenza virus), 수도라비스 바이러스(Pseudorabies virus), 파르보바이러스(Parvovirus), 돼지 수포병 바이러스(Swine vesicular disease virus; SVDV), 폭스바이러스(Poxvirus), 로타바이러스(Rotavirus), 마이코플라스마 폐렴(Mycoplasma pneumonia), 헤르페스 바이러스(Herpes virus), 닭전염성 기관지염(infectious bronchitis), 및 감보로 바이러스(infectious bursal disease virus)로 구성된 군으로부터 선택되는 적어도 하나인;
및 추가적으로 여기서:
상기 암은 비소세포성 폐암(non-small cell lung cancer), 유방암(breast carcinoma), 흑색종(melanoma), 림프종(lymphomas), 대장암(colon carcinoma) 및 간세포 암종(hepatocellular carcinoma)으로 구성된 군으로부터 선택되는 적어도 하나이다.
- 제 1항에 있어서, 상기 병원균의 항원이 PCV2 ORF2, CSFV E2 및 인간 파필로마바이러스(HPV) E7 단백질로 구성된 군으로부터 선택되는 적어도 하나인 융합 단백질.
- 제 2항에 있어서, 상기 PCV2 ORF2 단백질이 서열번호 20의 아미노산 서열을 포함하는 융합 단백질.
- 제 2항에 있어서, 상기 병원균의 항원이 서열번호 20의 아미노산 서열과 최소 90% 동일한 아미노산 서열을 포함하는 융합 단백질.
- 제 2항에 있어서, 상기 CSFV E2 단백질이 서열번호 21의 아미노산 서열을 포함하는 융합 단백질.
- 제 2항에 있어서, 상기 병원균의 항원이 서열번호 21의 아미노산 서열과 최소 90% 동일한 아미노산 서열을 포함하는 융합 단백질.
- 제 1항에 있어서, 상기 항원이 발-및-입 질병 바이러스 단백질 VP1(FMDV VP1) 및 발-및-입 질병 바이러스 단백질 3A(FMDV 3A)의 융합 항원인 융합 단백질.
- 제 7항에 있어서, 상기 융합 항원이 서열번호 24의 아미노산 서열을 포함하는 융합 단백질.
- 제 7항에 있어서, 상기 융합 항원이 서열번호 24의 아미노산 서열과 최소 90% 동일한 아미노산 서열을 포함하는 융합 단백질.
- 제 1항에 있어서, 상기 항원은 뉴캐슬 질병 바이러스(NDV) F 펩타이드 및 뉴캐슬 질병 바이러스 헤마글루티닌-뉴라미니다제(Hemagglutinin-Neuraminidase)(NDV HN) 단백질의 융합 항원인 융합 단백질.
- 제 10항에 있어서, 상기 융합 항원이 서열번호 27의 아미노산 서열을 포함하는 융합 단백질.
- 제 10항에 있어서, 상기 융합 항원이 서열번호 27의 아미노산 서열과 최소 90% 동일한 아미노산 서열을 포함하는 융합 단백질.
- 제 2항에 있어서, 상기 HPV E7 단백질이 서열번호 28의 아미노산 서열을 포함하는 융합 단백질.
- 제 13항에 있어서, 상기 병원성 항원이 서열번호 28의 아미노산 서열과 최소 90% 동일한 아미노산 서열을 포함하는 융합 단백질.
- 제 1항에 있어서, 상기 항원이 병원균으로부터의 두 개 또는 그 이상의 항원성 펩타이드의 융합 항원인 융합 단백질.
- 하기로 구성되는 융합 단백질:
(a) 융합 단백질의 N-말단에 위치한 항원-제시 세포-결합 도메인 또는 CD91 수용체-결합 도메인;
(b) APC-결합 도메인 또는 CD91 수용체-결합 도메인의 C-말단에 위치한 서열번호 4, 2, 또는 3의 아미노산 서열을 포함하는, 34 내지 61 아미노산 잔기 길이의 전좌 펩타이드; 및
(c) 병원균 또는 암 세포의 항원;
(d) 융합 단백질의 C-말단에 위치한 골지체 유지 서열; 및
(e) 항원 및 골지체 유지 서열 사이에 위치하거나, 또는 전좌 펩타이드 및 항원사이에 위치하는 핵 배출 신호로서, 핵 배출 신호는 서열번호 13의 아미노산 서열을 포함하인;
여기서:
상기 병원균은 인간 파필로마바이러스(HPV), 돼지 재생산 및 호흡 증후군 바이러스(PRRSV), 인간 면역결핍 바이러스-1(HIV-1), 댕기 바이러스, C형 간염 바이러스(HCV), B형 간염 바이러스(HBV), 돼지 서코바이러스(PCV2), 돼지 콜레라 바이러스(CSFV), 발-및-입 질병 바이러스(FMDV), 뉴캐슬 질병 바이러스(NDV), 전염성 위장염 바이러스(TGEV), 돼지 유행성 설사 바이러스(PEDV), 인플루엔자 바이러스, 수도라비스 바이러스, 파르보바이러스, 돼지 수포병 바이러스(SVDV), 폭스바이러스, 로타바이러스, 마이코플라스마 폐렴, 헤르페스 바이러스, 닭전염성 기관지염, 및 감보로 바이러스로 구성된 군으로부터 선택되는 적어도 하나인;
및 추가적으로 여기서:
상기 암은 비소세포성 폐암, 유방암, 흑색종, 림프종, 대장암 및 간세포 암종으로 구성된 군으로부터 선택되는 적어도 하나이다.
- 제 16항에 있어서, 상기 병원균의 항원이 PCV2 ORF2, CSFV E2 및 인간 파필로마바이러스(HPV) E7 단백질로 구성된 군으로부터 선택되는 적어도 하나인 융합 단백질.
- 제 16항에 있어서, 상기 항원이 발-및-입 질병 바이러스 단백질 VP1(FMDV VP1) 및 발-및-입 질병 바이러스 단백질 3A(FMDV 3A)의 융합 항원, 또는 뉴캐슬 질병 바이러스(NDV) F 펩타이드 및 뉴캐슬 질병 바이러스 헤마글루티닌-뉴라미니다제(NDV HN) 단백질의 융합 항원인 융합 단백질.
- 제 1항 내지 제 18항 중 어느 한 항의 융합 단백질 및 아주번트(adjuvant)를 포함하는 백신 조성물.
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