KR101808020B1 - p75NTR 뉴로트로핀 결합 단백질의 치료학적 용도 - Google Patents
p75NTR 뉴로트로핀 결합 단백질의 치료학적 용도 Download PDFInfo
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- KR101808020B1 KR101808020B1 KR1020147024077A KR20147024077A KR101808020B1 KR 101808020 B1 KR101808020 B1 KR 101808020B1 KR 1020147024077 A KR1020147024077 A KR 1020147024077A KR 20147024077 A KR20147024077 A KR 20147024077A KR 101808020 B1 KR101808020 B1 KR 101808020B1
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Abstract
본 발명은 통증 및/또는 통증 증후의 치료에서의 용도를 위한 p75NTR 뉴로트로핀 결합 단백질, p75NTR(NBP)에 관한 것이다.
Description
본 발명은 통증 및/또는 통증 증후의 치료에서의 용도를 위한 p75NTR 뉴로트로핀 결합 단백질, p75NTR(NBP)에 관한 것이다.
뉴로트로핀, 신경영양성장인자(neurotrophic growth factor(NGF)), 뇌유래 신경영양인자(brain-derived neurotrophic factor (BDNF)), 뉴로트로핀 3(NT-3) 및 뉴로트로핀 4/5(NT-4/5)는 4개의 수용체를 통해 작용한다: 저 친화성 p75 신경영양인자(p75NTR), 및 고 친화성 티로신 키나아제 수용체; TrkA, TrkB 및 TrkC. 저 친화성 수용체 p75NTR은 4개의 뉴로트로핀 전부에 의해 결합하고 활성화되며 다른 수용체로부터 독립적으로 기능하는 것이 보고되어 있다. 그렇지만, Trk 수용체는 더 선택적으로 활성화된다. 즉 NGF는 TrkA에 대한 선택적 리간드이고, BDNF는 TrkB에 대한 리간드이고, NT-3, 4/5는 TrkC에 대한 리간드이다. 또한 p75NTR과 Trk 단백질이 공동발현되었을 때, 그들은 복합체를 형성하고, 이는 양 수용체의 시그널링(signaling)을 변경하는 것이 보고되어 있다(Huang and Reichardt, 2003). 사실, p75NTR은 그들 각각의 Trk 수용체에 대해 각각의 뉴로트로핀의 선택성을 촉진하는 것이 제시되어 있다.
p75NTR은 종양괴사인자 수퍼패밀리(tumor necrosis factor receptor superfamily(TNFR-SF))의 구성원이고, 완전하게 특징지어진 이 수퍼패밀리의 첫 번째 구성원이다. 수퍼패밀리(인간의 일부 30개 유전자에 의해 엔코드된)는 p75NTR에서 첫 번째로 동정된 40 아미노산 시스테인-풍부 도메인(CRD)의 반복체가 하나 이상(전형적으로 4개)으로 구성된 리간드-결합 도메인으로 규정된다(Johnson et al., 1986; Radeke et al., 1987). 대조적으로, 시퀀스 모티프(sequence motif)는 모든 TNFR-SF 패밀리 멤버의 세포내 도메인에 의해 공유되지 않는다. 결론적으로, TNFR-SF 단백질의 시그널링 메카니즘은 상당히 다양하다.
트랜스멤브레인 도메인 내에서 시스테인 잔기(cysteinyl residues)를 통해 형성된 p75NTR 구조의 특이한 특징은 디설파이드-연결 p75NTR 다이머의 존재이다. 이 디설파이드 결합은 p75NTR에 의해 효과적인 뉴로트로핀-의존 시그널링을 위해 요구되며 세포내 및 세포외 도메인의 형성에서 중요한 역할을 한다(Vilar et al., 2009b). 뉴로트로핀은 대략 5분의 분포 반감기(distribution half-life)로 다이머와 비공유결합으로 연결된 채 생리학적으로 존재한다(Tria et al., 1994). 뉴로트로핀-의존 p75NTR 활성은 p75NTR 다이머의 두 개의 세포외 도메인의 CRDs 2-4를 가지는 뉴로트로핀 다이머의 연계(association)를 수반한다(He and Garcia, 2004). 디설파이드 결합 중심에서 세포내 도메인을 달패이용 집게 같은 동작으로 서로 벌어지게 강제하고 시그널링 어댑터 단백질, NRIF 및 TRAF6로 세포내 도메인의 연계를 허용하는 최근 연구는 뉴로트로핀 결합이 p75NTR 다이머의 두 개의 세포외 도메인이 서로 더 가깝게 이동하도록 한다는 모델을 지지한다(Vilar et al., 2009a, 2009b). 예를 들어 p75NTR에 존재하는 것과 같은 인트라-트랜스맴브레인 도메인 디설파이드 결합은 다른 TNFR-SF 패밀리 구성원에서 또는 어떠한 다른 멤브레인 단백질에서 이전에 언급된 적이 없다.
p75NTR은 α-세크레타아제와 γ-세크레타아제 활성과 그것의 세포내 도메인(intracellular domain(ICD))을 세포질 내로 방출하는 기질 단백질분해효소(matrix metalloproteinases(MMPs))에 의해, 노치와 β-아밀로이드 전구체 단백질의 절단-의존성 시그널링 경로와 유사한 방식으로 연속적 단백질분해 절단(sequential proteolytic cleavage)을 수행한다(Jung et al., 2003; Kanning et al., 2003). 이 경로에 의한 p75NTR ICD의 세포질 방출은 연결된 NRIF에 의해 시그널링을 촉진한다(Kenchappa et al., 2006). α-세크레타아제와 γ-세크레타아제 활성과 MMPs에 의한 단백질 분해 절단 후, p75NTR의 세포외 도메인의 역할은 완전하게 이해되어 있지 않다.
NGF와 다른 뉴로트로핀(BDNF, NT-3 및 NT-4/5)은 골관절염, 췌장염, 류마티스 관절염, 건선, 소양증 및 다발성 경화증에 기인하는 통증 병리학에서 매우 중요한 역할을 한다(Watanabe et al., 2010; Raychaudhuri et al., 2011; Barthel et al., 2009; Truzzi et al., 2011; McDonald et al., 2011; Yamaoka et al., 2007). 뉴로트로핀 중 어느 것이나 선택적 항체가 입증되었다; NGF 또는 BDNF, NT-3 및 NT-4/5는 통증을 현저하게 감소시킨다. 게다가, 뉴로트로핀 수용체 p75NTR, TrkA, TrkB 또는 TrkC에 직결된 항체는 또한 통증 모델에 효과적인 것으로 입증되었다(Orita S et al., 2010; Svensson P et al., 2010; Iwakura et al., 2010; Cirilio et al., 2010; Pezet et al., 2010; Hayashi et al., 2011; Chu et al., 2011; Ueda et al., 2010; Ghilardi et al., 2010; Fukui et al., 2010). 통증 모델(좌골 신경 크러쉬 후에 나타나는 기계적 이질통)에서 후쿠이 등(Fukui et al.,)(2010)은 항-p75NTR 항체로 치료 후 통증 관련 종점에서 상당한 효능을 입증하였다. 이 연구로부터 p75NTR 저해 항체로 하는 치료가 통증의 상당한 감소를 가져오게 하여 CGRP와 p75NTR 발현을 감소시켰다고 결론지었다.
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본 발명은 세포막으로부터 절단 후 외인성 또는 내인성의 p75NTR의 세포외 도메인이 각각의 뉴로트로핀 NGF, BDNF, NT-3 및 NT-4/5에게 뉴로트로핀 결합 단백질 또는 가용성 수용체로서 작용하고, 기능, 뉴로트로핀 기능의 생리학 및 항상성에서 중요한 역할을 한다는 것을 입증한다. 또한, 예를 들면 정적 이질통 및 열적 통각과민 모델에서, NGF, BDNF, NT-3 및 NT-4/5를 포함하는 신경영양 인자의 생리학적 작용을 조정 또는 중화하기 위한 p75NTR의 세포외 도메인의 용도를 설명한다. 따라서 p75NTR 뉴로트로핀 결합 단백질은 통증 및 건선, 습진, 류마티스 관절염, 방광염, 자궁내막증 및 골관절염과 같은 병리학에 관련된 다른 신경영양 인자의 치료에서의 용도가 발견된다.
본 발명의 제1 측면에 따르면, 통증 치료 용도를 위한, 또는 통증 및/또는 통증 증후(symptoms)의 예방 및/또는 치료를 위한, 또는 통증 및/또는 통증 증후의 완화, 제어, 발생을 감소시키기 위한, 또는 통증 및/또는 통증 증후의 발전(development) 또는 진전(progression)을 지연시키기 위한 p75NTR 뉴로트로핀 결합 단백질(NBP)이 제공된다.
본 발명의 제2 측면에 따르면, 제1 측면에 따른 용도를 위한 p75NTR 뉴로트로핀 결합 단백질이 제공되며, p75NTR(NBP)는 하나 이상의 보조 분자에 연결된 p75NTR(NBP)를 포함한다. 바람직하게, p75NTR(NBP)는 하나 이상의 링커를 통해 하나 이상의 보조 분자에 연결된다.
본 발명의 제3 측면에 따르면, 제1 또는 제2 측면에 따른 p75NTR(NBP) 또는 p75NTR(NBP)의 하나 이상의 보조 분자에 연결된 p75NTR(NBP)를 엔코딩하는 핵산 분자가 제공된다. 핵산 분자는 엔코딩 신호 서열을 더 포함할 수도 있다. 또한 통증의 치료를 위한 핵산 분자의 용도도 제공된다.
본 발명의 제4 측면에 따르면, 세포를 트랜스팩션하기 위한 복제 가능한 발현 벡터가 제공되며, 벡터는 제3 측면의 핵산 분자를 포함하며, 바람직하게 벡터는 바이러스 벡터이다. 또한 통증 치료를 위한 벡터의 용도를 제공한다.
본 발명의 제5 측면에 따르면, 제3 또는 제4 측면의 핵산 분자를 함유하는 숙주 세포가 제공된다.
본 발명의 제6 측면에 따르면, 제1 또는 제2 측면에 따른 또는 그들의 바람직한 구현예에 따른 용도를 위한 p75NTR(NBP)가 제공된다. 또는 제3 및 제4 측면에 따른 용도를 위한 핵산 또는 벡터가 제공된다. 여기서 p75NTR(NBP) 또는 핵산 분자 또는 벡터는 제2의 약리학적 활성 화합물과 결합된 조합에서 별개의, 순차적 또는 동시적 사용을 위한 것이다.
본 발명에 따르면, 통증 치료 용도를 위한, 또는 통증 및/또는 통증 증후(symptoms)의 예방 및/또는 치료를 위한, 또는 통증 및/또는 통증 증후의 완화, 제어, 발생을 감소시키기 위한, 또는 통증 및/또는 통증 증후의 발전(development) 또는 진전(progression)을 지연시키기 위한 p75NTR 뉴로트로핀 결합 단백질(NBP)이 제공된다.
본 발명에 따르면, 본 발명에 따른 p75NTR(NBP) 또는 p75NTR(NBP)의 하나 이상의 보조 분자에 연결된 p75NTR(NBP)를 엔코딩하는 핵산 분자가 제공된다. 또한 통증의 치료를 위한 핵산 분자의 용도도 제공된다.
본 발명에 따르면, 세포를 트랜스팩션하기 위한 복제 가능한 발현 벡터가 제공되며, 벡터는 본 발명에 따른 핵산 분자를 포함하며, 통증 치료를 위한 벡터의 용도를 제공한다.
본 발명에 따르면, 본 발명에 따른 핵산 분자를 함유하는 숙주 세포가 제공된다.
본 발명에 따르면, 통증 및/또는 통증의 징후의 예방, 완화, 제어, 발생 감소, 또는 전개 또는 진전의 지연 중 하나 이상을 위한 본 발명에 따른 p75NTR(NBP) 또는 핵산 분자 또는 벡터 및 약학적으로 수용가능한 담체 및/또는 첨가제를 포함하는 약학적 조성물이 제공된다.
본 발명에 따르면, 본 발명에 따른 p75NTR(NBP) 또는 핵산 분자 또는 벡터, 또는 약학적 조성물; 및 개인에게 통증 및/또는 통증 증후의 예방 또는 치료 중 어느 하나 이상을 위한 또는 통증 및/또는 통증 증후의 완화, 제어, 발생 감소, 또는 발전 또는 진전의 지연을 위한 상기 p75NTR(NBP), 핵산 분자, 벡터 또는 약학적 조성물의 유효량 투여에 관한 지시서를 포함하는 키트가 제공된다.
본 발명에 따르면, 본 발명에 따른 p75NTR(NBP) 또는 핵산 분자 또는 벡터의 치료학적으로 유효한 양을 개인에게 투여하는 것을 포함하고, 선택적으로 약학적으로 수용가능한 담체를 더 포함하는 개인의 통증 및/또는 통증 증후의 치료 및/또는 예방 방법이 제공된다.
도 1은 p75NTR 세포외 도메인 서열, 뉴로트로핀 결합 도메인이 굵게 강조된 것이다.
도 2는 인간 혈장 내 p75NBPP 펩타이드 표준 절편(standard fragments)과 p75NTR(NBP)-NGF 복합체를 입증하는 p75NTR(NBP)와 NGF의 공동면역침강을 나타낸 것이다. 도 2(a)에서 펩티드는 p75NTR-Fc 키메라, 표준 소화(standard digest)의 LCMS/MS에 의해 동정된 것이다. 도 2(b)에서 펩티드는 p75NTR-Fc 키메라, 표준 소화(standard digest)의 LCMS/MS에 의해 동정된 것이다.
도 3은 도 2에서 나타낸 WADAECEEIPGR(SEQ ID NO.7) 피크의 MS/MS 서열 확인을 나타낸 것이다.
도 4는 p75NTR(NBP)가 TrkA를 발현하는 U20S 세포선과 TrkA와 p75NTR을 공동 발현하는 U20S 세포선에서 NGF 기능을 저해하는 것을 나타낸 것이다.
도 5는 가용성 p75NTR(NBP)가 TrkA를 발현하는 U20S 세포선과 TrkA와 p75NTR을 공동 발현하는 U20S 세포선에서 BDNF 기능을 저해하는 것을 나타낸 것이다.
도 6은 BDNF에 결합하는 p75NTR(NBP)를 입증하는 바이오코어 데이터(biocore data)와 항-BDNF와 p75NTR(NBP) 사이의 경쟁을 나타낸 것이다.
도 7은 PC12 세포에서 NGF 활성의 p75NTR(NBP) 저해를 나타낸 것이다.
도 8은 뉴로트로핀 결합 단백질 p75NTR(NBP)가 신경 흥분 모델에서 BDNF 통증 효과를 저해하는 것을 나타낸 것이다.
도 9는 뉴로트로핀 결합 단백질 p75NTR(NBP)가 UVIH 모델에서 통각과민증을 저해하는 것을 나타낸 것이다.
도 10은 SEQ ID NO.1로 인간 p75NTR 전체 아미노산 서열(full amino acid sequence)이다.
도 11은 SEQ ID NO.2로 인간 p75NTR 신호 서열을 포함하는 세포외 도메인이다.
도 12는 SEQ ID NO.3으로 신호 서열이 없는 인간 p75NTR 세포외 도메인이다.
도 13은 SEQ ID NO.4로 인간 p75NTR(NBP) 뉴로트로핀 결합 도메인 1이다.
도 14는 SEQ ID NO.5로 인간 p75NTR(NBP) 뉴로트로핀 결합 도메인 2다.
도 15는 SEQ ID NO.6으로 인간 p75NTR(NBP) 뉴로트로핀 결합 도메인 3이다.
도 16은 SEQ ID NO.7로 인간 p75NTR(NBP) 뉴로트로핀 결합 도메인 4이다.
도 17은 SEQ ID NO.8로 인간 p75NTR(NBP) 뉴로트로핀 결합 도메인 5이다.
도 18은 SEQ ID NO.9로 인간 트랜스페린(Human Transferrin)이다.
도 19는 SEQ ID NO.10으로 인간 알부민이다.
도 20은 SEQ ID NO.11로 인간 Fc IgG1이다.
도 21은 SEQ ID NO.12로 인간 Fc IgG2이다.
도 22는 SEQ ID NO.13으로 인간 Fc IgG3이다.
도 23은 SEQ ID NO.14로 인간 Fc IgG4이다.
도 24는 SEQ ID NO.15로 연장된 혈청 반감기를 위해 조작된 인간 Fc 절편이다.
도 25는 SEQ ID NO.16으로 작동자 기능(Effector Functions)의 결여를 위해 조작된 인간 Fc 절편이다.
도 26은 SEQ ID NO.17로 p75NTR(NBP)-Fc 링커이다.
도 27은 SEQ ID NO.18로 p75NTR(NBP)-Fc 링커이다.
도 28은 SEQ ID NO.19로 p75NTR(NBP)-Fc 링커이다.
도 2는 인간 혈장 내 p75NBPP 펩타이드 표준 절편(standard fragments)과 p75NTR(NBP)-NGF 복합체를 입증하는 p75NTR(NBP)와 NGF의 공동면역침강을 나타낸 것이다. 도 2(a)에서 펩티드는 p75NTR-Fc 키메라, 표준 소화(standard digest)의 LCMS/MS에 의해 동정된 것이다. 도 2(b)에서 펩티드는 p75NTR-Fc 키메라, 표준 소화(standard digest)의 LCMS/MS에 의해 동정된 것이다.
도 3은 도 2에서 나타낸 WADAECEEIPGR(SEQ ID NO.7) 피크의 MS/MS 서열 확인을 나타낸 것이다.
도 4는 p75NTR(NBP)가 TrkA를 발현하는 U20S 세포선과 TrkA와 p75NTR을 공동 발현하는 U20S 세포선에서 NGF 기능을 저해하는 것을 나타낸 것이다.
도 5는 가용성 p75NTR(NBP)가 TrkA를 발현하는 U20S 세포선과 TrkA와 p75NTR을 공동 발현하는 U20S 세포선에서 BDNF 기능을 저해하는 것을 나타낸 것이다.
도 6은 BDNF에 결합하는 p75NTR(NBP)를 입증하는 바이오코어 데이터(biocore data)와 항-BDNF와 p75NTR(NBP) 사이의 경쟁을 나타낸 것이다.
도 7은 PC12 세포에서 NGF 활성의 p75NTR(NBP) 저해를 나타낸 것이다.
도 8은 뉴로트로핀 결합 단백질 p75NTR(NBP)가 신경 흥분 모델에서 BDNF 통증 효과를 저해하는 것을 나타낸 것이다.
도 9는 뉴로트로핀 결합 단백질 p75NTR(NBP)가 UVIH 모델에서 통각과민증을 저해하는 것을 나타낸 것이다.
도 10은 SEQ ID NO.1로 인간 p75NTR 전체 아미노산 서열(full amino acid sequence)이다.
도 11은 SEQ ID NO.2로 인간 p75NTR 신호 서열을 포함하는 세포외 도메인이다.
도 12는 SEQ ID NO.3으로 신호 서열이 없는 인간 p75NTR 세포외 도메인이다.
도 13은 SEQ ID NO.4로 인간 p75NTR(NBP) 뉴로트로핀 결합 도메인 1이다.
도 14는 SEQ ID NO.5로 인간 p75NTR(NBP) 뉴로트로핀 결합 도메인 2다.
도 15는 SEQ ID NO.6으로 인간 p75NTR(NBP) 뉴로트로핀 결합 도메인 3이다.
도 16은 SEQ ID NO.7로 인간 p75NTR(NBP) 뉴로트로핀 결합 도메인 4이다.
도 17은 SEQ ID NO.8로 인간 p75NTR(NBP) 뉴로트로핀 결합 도메인 5이다.
도 18은 SEQ ID NO.9로 인간 트랜스페린(Human Transferrin)이다.
도 19는 SEQ ID NO.10으로 인간 알부민이다.
도 20은 SEQ ID NO.11로 인간 Fc IgG1이다.
도 21은 SEQ ID NO.12로 인간 Fc IgG2이다.
도 22는 SEQ ID NO.13으로 인간 Fc IgG3이다.
도 23은 SEQ ID NO.14로 인간 Fc IgG4이다.
도 24는 SEQ ID NO.15로 연장된 혈청 반감기를 위해 조작된 인간 Fc 절편이다.
도 25는 SEQ ID NO.16으로 작동자 기능(Effector Functions)의 결여를 위해 조작된 인간 Fc 절편이다.
도 26은 SEQ ID NO.17로 p75NTR(NBP)-Fc 링커이다.
도 27은 SEQ ID NO.18로 p75NTR(NBP)-Fc 링커이다.
도 28은 SEQ ID NO.19로 p75NTR(NBP)-Fc 링커이다.
본 발명의 제1 측면에 따르면, p75NTR 뉴로트로핀 결합 단백질 (p75NTR(NBP))이 통증의 치료를 위한 용도를 위해, 또는 통증 및/또는 통증 증후의 예방 및/또는 치료를 위해, 또는 완화, 제어, 발생을 감소시키기 위해, 또는 통증 및/또는 통증 증후의 발전 또는 진전을 지연시키기 위해 제공된다. 바람직하게 p75NTR 뉴로트로핀 결합 단백질, p75NTR(NBP)는 페길화(pegylated)되어 있으며, 더 바람직하게는 글리코실화(glycosylated)되어 있다.
p75NTR 뉴로트로핀 결합 단백질, p75NTR(NBP)는 바람직하게 (a) 하나 이상의 뉴로트로핀 결합 도메인 1[SEQ ID NO. 4], 2[SEQ ID NO. 5], 3[SEQ ID NO. 6], 4[SEQ ID NO. 7] 또는 5[SEQ ID NO. 8]를 포함한다. 더 바람직하게 p75NTR(NBP)는 (b) 각각의 뉴로트로핀 결합 도메인 1[SEQ ID NO. 4], 2[SEQ ID NO. 5], 3[SEQ ID NO. 6], 4[SEQ ID NO. 7] 및 5[SEQ ID NO. 8]를 포함하거나 또는 (c) 각각의 뉴로트로핀 도메인 1[SEQ ID NO. 4], 3[SEQ ID NO. 6], 4[SEQ ID NO. 7] 및 5[SEQ ID NO. 8]를 포함한다. 더 바람직하게 p75NTR(NBP)는 세포외 도메인 2[SEQ ID NO.3] 또는 상기 (a), (b) 또는 (c)를 포함하는 그들의 부분을 포함한다. 더 바람직하게는 p75NTR(NBP)는 세포외 도메인 1[SEQ ID NO.2] 또는 상기 (a), (b) 또는 (c)를 포함하는 그들의 부분을 포함한다.
바람직하게 p75NTR(NBP)는 각각의 뉴로트로핀 NGF, NT3, BDNF 및 NT4/5, 바람직하게 인간 NGF, NT3, BDNF 및 NT4/5에 결합된다. 더 바람직하게 p75NTR(NBP)는 각각의 뉴로트로핀 NGF, NT3, BDNF 및 NT4/5에, 바람직하게 인간 NGF, NT3, BDNF 및 NT4/5에, 바람직하게 순수한 완전 서열 p75NTR[SEQ ID NO.1]과 동등하거나 똑같은 결합 정수로 결합된다. 결합 정수(binding constant)는 20℃에서 표면 플라즈몬 공명을 사용하는 것에 의한 것과 같은 여기에 설명된 분석법을 사용하여 결정될 수 있으며, 천연 단백질 결합 정수에 대한 분석법은 알려져 있으며 이 기술분야에서 알려진 세포 기반 분석법을 포함한다. 바람직하게 p75NTR(NBP)는 하나 이상의 앞서 언급한 뉴로트로핀을 인비보 또는 인비트로, 혈장 또는 다른 인체 유체 내에서의 저하로부터 보호하고, 그리고/또는 하나 이상의 상기 언급한 뉴로트로핀의 항상성 밸런스를 그들의 생물학적 유리 형태와 비교하여 유지시킨다.
본 발명의 p75NTR(NBP)는 바람직하게 하나 이상의 NGF, BDNF, NT3 또는 NT4/5에 약 0.1nM에서 약 0.5nM 사이의 결합 친화도(Kd)로 결합된다. 일부 바람직한 구현예에서, 결합 친화도(Kd)는 여기서 설명된 바람직하게 20℃에서 표면 플라즈몬 공명에 의해 측정되는 바와 같이 NGF, BDNF, NT3 또는 NT4/5에 대한 인비트로 결합 분석법으로 측정되는 약 0.1nM과 약 0.2nM, 0.5nM, 1nM, 1.5nM, 2nM, 2.5nM, 3nM, 3.5nM, 4nM, 4.5nM, 5nM, 5.5nM, 6nM, 6.5nM, 7nM, 7.5nM, 8nM, 8.5nM, 9nM, 9.5nM, 10nM, 15nM, 20nM, 25nM, 30nM, 35nM, 40nM, 45nM 또는 50nM 중 어느 것 사이이다. 일부 더 바람직한 구현예에서, 결합 친화도(Kd)는 여기서 설명된 바와 같이 바람직하게 20℃에서 표면 플라즈몬 공명에 의해 측정되는 바와 같이, 뉴로트로핀을 가지는 p75NTR(NBP)에 대한 인비트로 결합 분석에서 측정되는 약 250pM, 300pM, 350pM, 400pM, 450pM, 500pM, 550pM, 600pM, 650pM, 700pM, 750pM, 800pM, 850pM, 950pM 또는 1nM 중 어느 것 이하이다. 한층 더 바람직한 구현예에서, 결합 친화도(Kd)는 여기서 설명된 바와 같이 바람직하게 20℃에서 표면 플라즈몬 공명에 의해 측정되는 바와 같이, 뉴로트로핀을 가지는 p75NTR(NBP)에 대한 인비트로(in-vitro) 결합 분석에서 측정되는 약 0.3nM 또는 약 1nM이다.
더 바람직하게 p75NTR(NBP)는 상기한 뉴로트로핀, NGF, BDNF, NT3 또는 NT4/5의 기능적 활성(뉴로트로핀의 기능적 활성을 조정 또는 상승 또는 저하 조절로서 언급된), 예를 들면, 그들 각각의 수용체와 그들의 상호작용으로부터 얻어지는 상기한 뉴로트로핀의 기능적 활성에 영향을 준다.
바람직하게 p75NTR(NBP)는 뉴런 및 시냅스의 성장 및 분화, 뉴런 세포의 생존 및 분화, Trk 시그널링, 인비트로 또는 인비보(in-vivo)에서 축색돌기로부터 자라난 것의 자극의 기능적 분석에 의해 평가되는 BDNF의 기능적인 활성에 영향을 준다.
바람직하게 p75NTR(NBP)는 고전적인 뉴런 생존 분석에서 입증되는 바와 같이(Cowan, W.M., Hamburger, V., Levi-Montalcini, R. Annu . Rev . Neurosci . 2001;24:551-600에서 제공되는 바와 같이), TrkA에 결합하는 NGF 및 TrkA의 활성을 측정하여 평가되는 NGF의 기능적 활성에 영향을 준다.
바람직하게 p75NTR(NBP)는 Trk 수용체 인산화, 미토젠-활성화된 단백질 키나아제 인산화 리포터 분석법 또는 세포 생존 및 신경돌기 신장(neurite extension) 분석법으로 입증되는 바와 같이, 결합되는 NT3와 내생의(endogenous) Trk 수용체 활성의 활성화를 측정하여 평가되는 NT3의 기능적 활성에 영향을 준다.
바람직하게 p75NTR(NBP)는 예를 들어 미엘린 기초 단백질(MBP) 인산화 분석에서 또는 대안적으로 인비보 혈관신생인자(vascular endothelial growth factor, VEGF)/염기성 섬유모세포성장인자(basic fibroblast growth factor)-유도 앤지오제네시스의 마트리겔 앤지오제네시스(Matrigel angiogenesis) 분석에서 NT4/5 인비트로 또는 인비보 인산화 및 활성화 분석을 측정하여 평가되는 NT4/5의 기능적 활성에 영향을 준다.
바람직하게 p75NTR(NBP)는 히 앤드 가르시아(He and Garcia (2001) Science, 301, 870 - 805페이지)에 나타난 바와 같이 하나 이상의 뉴로트로핀 NGF, NT3, BDNF 및 NT4/5의 접촉 잔류물(contact residues)에 결합된다.
바람직하게 p75NTR(NBP)는 용해성이 있으며, 바람직하게 수용성 용액에 용해성이 있고, 바람직하게 혈청, 혈장, 혈액과 같은 생물학적 유체에 용해성이 있다.
본 발명의 두 번째 측면에 따르면, 첫 번째 측면에 따른 용도를 위한 p75NTR(NBP)가 제공되며, p75NTR(NBP)는 하나 이상의 보조 분자에 연결된p75NTR(NBP)를, 바람직하게 첫 번째 측면의 p75NTR(NBP)를 포함한다. 바람직하게, p75NTR(NBP)는 하나 이상의 링커를 통해 하나 이상의 보조 분자에 연결되어 있다.
바람직하게 하나 이상의 보조 분자는 (a) 트랜스페린 또는 그것의 일부분, 바람직하게 트랜스페린은 인간 트랜스페린이고, 바람직하게 SEQ ID NO.9이며, (b) 알부민 또는 그것의 일부분, 바람직하게 알부민은 인간 알부민이고, 바람직하게 SEQ ID NO. 10이며, (c) 면역글로불린 Fc 또는 그것의 일부분, 바람직하게 면역글로불린 Fc는 인간 면역글로불린 Fc이고, (d) 폴리에틸렌 글리콜 폴리머 체인, (e) 카보하이드레이트 체인으로부터 선택된다.
여기서 사용되는 용어, "면역글로불린 Fc" 또는 "Ig Fc"는 면역글로불린 체인 불변 영역, 바람직하게 면역글로불린 중사슬(heavy chain) 불변 영역의, 또는 그것의 일부분의 카르복실 말단부를 의미하는 것으로 이해한다. 바람직하게 면역글로불린 Fc는 선택적으로 면역글로불린 경첩 영역(hinge region)을 가지는 1) CH1 도메인, CH2 도메인, 및 CH3 도메인, 2) 선택적으로 면역글로불린 경첩 영역(hinge region)을 가지는 CH1 도메인 및 CH2 도메인, 3) 선택적으로 면역글로불린 경첩 영역(hinge region)을 가지는 CH1 도메인 및 CH3 도메인, 4) 선택적으로 면역글로불린 경첩 영역(hinge region)을 가지는 CH2 도메인 및 CH3 도메인, 또는 5) 선택적으로 면역글로불린 경첩 영역과 연결되는 CH1, CH2 및 CH3로부터 선택되는 하나 이상의 도메인의 조합을 포함한다. 바람직하게 면역글로불린 Fc는 Fc 또는 IgG, IgM, IgA, IgD, IgE, 더 바람직하게 IgG1, IgG2, IgG3, IgG4, IgA1, IgA2, sIgA, 한층 더 바람직하게 IgG2 또는 IgG4, 가장 바람직하게 IgG2로부터 선택되는 면역글로불린 아이소타입의 Fc의 일부분을 포함하거나 구성된다. 선택적으로 면역글로불린 Fc는 또한 아미노산 돌연변이, 결실, 치환, 또는 보체 고정(complement fixation) 또는 항체-의존성 세포 독성작용에 기여하거나 또는 Fc 수용체 결합 친화도를 개선하는 화학 수식(chemical modification)을 포함한다.
더 바람직하게 면역글로불린 Fc는 (1) CH2 도메인 또는 그것의 일부분 및 CH3 도메인 또는 그것의 일부분, (b) CH2 도메인 또는 그것의 일부분, 또는 (c) CH3 도메인 또는 그것의 일부분 중의 어느 것을 포함하거나 구성되며, 면역글로불린 Fc 또는 그것의 일부분은 IgG, IgM, IgA, IgD, IgE, 더 바람직하게 IgG1, IgG2, IgG3, IgG4, IgA1, IgA2, sIgA, 한층 더 바람직하게 IgG2 또는 IgG4, 가장 바람직하게 IgG2로부터 선택되는 아이소타입이다.
바람직하게 면역글로불린 Fc는 면역글로불린 중사슬의 카르복실 말단부를 포함하거나 구성되며 IgG, IgA 또는 IgD 항체 아이소타입으로부터 CH2 및/또는 CH3 도메인 또는 그들의 일부, 또는 IgM 또는 IgE로부터 CH2 및/또는 CH3 및/또는 CH4 도메인 또는 그들의 일부를 포함할 수도 있다. 바람직하게 면역글로불린 Fc는 면역글로불린의 펩신 소화에 의해 유도 가능하다시피, 주로 CH3 및 CH2의 작은 부분(small portion)을 포함하는 Fc의 절편을 포함하거나 구성된다. 바람직하게 면역글로불린 Fc는 면역글로불린의 파파인 소화에 의해 생성될 수 있는 대로, CH2 및 CH3를 포함하고, 부가적으로 온전한 면역글로불린에서 CH1 및 CH2 영역을 연결하는 중사슬의 짧은 부분인 경첩 영역에 연결된 전체 Fc 영역을 포함하거나 구성된다. 바람직하게 면역글로불린 경첩 영역은 IgG 바람직하게 인간 IgG, 더 바람직하게 IgG1, IgG2, IgG3 또는 IgG4에서 선택되는 IgG, 가장 바람직하게 IgG1으로부터 유도되는 경첩 영역 또는 경첩 영역의 부분을 포함하거나 구성되며 또는 대안적으로 앞선 경첩 영역 구현예의 종(species) 또는 대립유전자 변종(allelic variant)이다. 경첩 영역 또는 면역글로불린 경첩 영역의 부분은 Fc 영역의 C 또는 N-말단에, 바람직하게 N-말단에 위치될 수 있다.
본 발명의 바람직한 구현예에 따르면, 면역글로불린 Fc는 바람직하게 Fc 작동 기능(effector function)을 저감시키는 CH2 영역 내 야생형 서열의 아미노산 돌연변이를 하나 이상 포함하는 면역글로불린 Fc 또는 면역글로불린 Fc의 일부를 포함하거나 구성된다. 바람직하게 이들 돌연변이는 A330, P331에서 S330, S331이다(야생형 IgG2 서열을 참고로 하여 아미노산 넘버링, CH2 영역은 인간 중사슬 IgG2 불변 영역이다:[Eur. J. Immunol. (1999) 29:2613-2624]). 바람직하게 면역글로불린 Fc는 글리코실화되어 있고 생리학적 pH에서 높게 충전되어 있어서 p75NTR(NBP)를 가용화하는 것을 돕는다. Fc 영역은 또한 진단 목적으로 예를 들면 항-Fc ELISA에 의해 p75NTR(NBP)의 검출을 가능하게 한다. 본 발명의 p75NTR(NBP)는 바람직하게 정상 글리코실화 사이트에서 Ig Fc를 글리코실화하는 세포에서 바람직하게 합성된다.
바람직하게 면역글로불린 Fc는 SEQ ID No. 11, 12, 13, 14, 15 또는 16 또는 그들의 종 또는 대립유전자 변종, 또는 CH2 및/또는 CH3 도메인, 또는 SEQ ID No. 11, 12, 13, 14, 15 또는 16으로부터 유도되는 그들의 부분으로부터 선택되는 아미노산의 인간 면역글로불린 Fc 영역을 포함하거나 구성된다.
본 발명에 따르면, 하나 이상의 보조 분자에 연결된 p75NTR(NBP)는 바람직하게 p75NTR(NBP)의 개선된 용해도 및/또는 p75NTR(NBP)의 안정성 및/또는 p75NTR(NBP)의 개선된 혈청 반감기의 유용한 생물학적 특성을 입증한다. 개선된 용해도는 p75NTR(NBP)의 생물학적 이용가능성이 투여시 최대화되고 p75NTR(NBP)의 정확한 복용량(dosage)이 결정되고 수행되기 위해서 바람직하다. 개선된 용해도는 인비보 전달에서 통증을 유발하고 잠재적 염증을 유발하여 바람직하지 않은 응집 문제를 극복하기에 유리하다. 개선된 혈청 반감기는 전달된 p75NTR(NBP)의 치료 효과를 동등하게 달성하거나 유지하기 위해, 치료를 위한 사용 동안 요구 복용량의 감소된 레벨 또는 감소된 주기를 촉진하는 이점을 가진다. 혈액 또는 혈청 내에서 연장된 반감기와 더 높은 안정성은 덜 잦은 복용의 복용법을 허용하고/하거나 복용량 수준을 낮출 수 있게 하는 장점을 가져서 인비보 잠재적 독성 또는 부작용을 감소시킨다. 이 경우에 p75NTR(NBP)는 그의 치료 효과에서 더 강력하고/하거나 순환에서 더 안정적이다. 얻어지는 더 낮거나 덜 잦은 복용량은 p75NTR(NBP) 투여와 관련하여 어떠한 잠재적 독성 효과 또는 부작용을 잠재적으로 최소화하기에 유용하다. 또한 하나 이상의 보조 분자에 연결된 p75NTR(NBP)의 분자량은 단독의 p75NTR(NBP)를 초과하여 증가되며, 이는 분자가 원하지 않는 부위, 예를 들면 중추신경계에 침투하는 위험을 줄이고 표적 조직에 보유 또는 농축을 위해 적합한 분자를 만들도록 정맥주사로 투여되었을 때 혈액 순환에서 잘 보유될 것이라는 이점을 가진다.
바람직하게 하나 이상의 보조 분자에 연결된 p75NTR(NBP)는 그렇게 연결되지 않은 p75NTR(NBP)와 비교하여 p75NTR(NBP)의 개선된 용해도 및/또는 p75NTR(NBP)의 개선된 안정성 및/또는 개선된 혈청 반감기를 입증한다. 바람직하게 개선된 용해도는 바람직하게 생리학적 pH, 바람직하게 pH 5 내지 8, 바람직하게 약 pH 7에서의 바람직하게 버퍼 및/또는 염과 같은 첨가제를 가지는 물과 같은 수용액에서의 용해도이며 또는 혈청 또는 혈액과 같은 생물학적 유체에서의 용해도이다. 바람직하게 개선된 안정성은 저장 기간 또는 연이은 냉동 및 해동 동안의 기간 동안 변성, 산화, 분절화 또는 응집 효과에 기인하는 p75NTR(NBP) 단백질의 활성의 안정성 또는 구조적 강직성이다. 구조적 안정성은 변성, 산화, 응집 또는 응집의 표준 측정에 의해 판단될 수 있으며, 활성의 안정성은 여기서 개시된, 알려진 단백질 혈청 반감기의 측정법인 결합 또는 기능적 분석법에 의해 측정될 수 있다.
바람직하게 하나 이상의 보조 분자에 연결된 p75NTR(NBP)는 단일 종을 제공하기 위해 포유류 숙주 세포의 다양성으로부터 높은 수준에서 발현될 수 있으며 친화도 크로마토그래피에 의해 효율적으로 정제될 수 있으며 예를 들어 포도상구균 단백질 A(Staphylococcus aureus protein A)에 결합되어 정제될 수 있다. 바람직하게 하나 이상의 보조 분자에 연결된 p75NTR(NBP)는 이량화될 수 있으며 바람직하게 이량체는 그렇게 연결되지 않은 p75NTR(NBP)와 비교하여 뉴로트로핀 NGF, BDNF, NT3 또는 NT4/5에 증가된 친화도를 가진다. 더 단단한 결합은 더 높은 효능과 예를 들어 여기에 개시된 뉴로트로핀 기능적 분석법에 의해 결정되는 것과 같은 75NTR(NBP) 효과에 의해 판단되는 대로 더 높은 치료학적 효능의 이점을 가진다. 더 높은 효능은 p75NTR(NBP)가 동일한 치료학적 효능을 달성하기 위해 더 낮은 복용량에서 사용될 수 있어서 인비보에서 잠재적 독성 또는 부작용을 감소시킨다는 이점을 가진다.
바람직하게 본 발명의 p75NTR(NBP)는 약 2, 4, 6, 8, 10, 12, 14, 16, 18, 20, 22, 24, 26, 28, 30, 32, 34, 36, 38, 40, 42, 44, 46, 48, 50, 52, 54, 56, 58, 60, 62, 64, 66, 68, 70, 72, 74, 76, 78, 80, 82, 84, 86, 88, 90, 92, 94, 96, 98, 100, 102, 104, 106, 108, 110, 112, 114, 116, 118, 120, 122, 124, 126, 128, 130, 132, 134, 136, 138, 140, 142, 144, 146, 148, 150, 152,154, 156, 158, 160, 62, 164, 166, 168, 170, 172, 174, 176, 178, 180, 182, 184, 186, 188, 190, 192, 194, 196, 198, 200, 202, 204, 206, 208 또는 210시간 +/- 1시간 또는 이들 중 어느 하나의 이상인 인비보 반감기를 가지며, 더 바람직하게 본 발명의 75NTR(NBP)는 약 24시간 이상의 인비보 반감기를 가진다.
더 바람직하게 본 발명의 p75NTR(NBP)는 약 2, 4, 6, 8, 10, 12, 14, 16, 18, 20, 22, 24, 26, 28, 30, 32, 34, 36, 38, 40, 42, 44, 46, 48, 50, 52, 54, 56, 58, 60, 62, 64, 66, 68, 70, 72, 74, 76, 78, 80, 82, 84, 86, 88, 90, 92, 94, 96, 98, 100, 102, 104, 106, 108, 110, 112, 114, 116, 118, 120, 122, 124, 126, 128, 130, 132, 134, 136, 138, 140, 142, 144, 146, 148, 150, 152,154, 156, 158, 160, 62, 164, 166, 168, 170, 172, 174, 176, 178, 180, 182, 184, 186, 188, 190, 192, 194, 196, 198, 200, 202, 204, 206, 208 또는 210일 +/- 1일 또는 이들에서 선택된 어느 하나보다 더 큰 인비트로 반감기를 가지며, 더 바람직하게 본 발명의 p75NTR(NBP)는 약 6일 이상의 인비트로 반감기를 가진다. 바람직하게 안정성은 대략 생리학적 pH, 완충된 수용액에서, 바람직하게 20℃ 또는 37℃에서 측정된다.
앞선 바람직한 구현예에 따르면, 바람직하게 인비보 반감기는 래트에서의 반감기 또는 인간에서의 반감기이고, 더 바람직하게 인간에서의 반감기이다. 바람직하게 반감기는 예를 들어 정맥주사로 또는 피하주사에 의한 인비보 투여 후 본 발명의 p75NTR(NBP)의 레벨의 혈청 측정으로부터 결정된다.
본 발명의 제2 측면에 따르면, 링커는 바람직하게 (a) 공유결합, (b) 비공유 결합, (c) 펩티드 결합, (d) 펩티드를 포함하는 하나의 아미노산 또는 복수의 아미노산으로부터 선택된다. 바람직하게 p75NTR(NBP)는 하나 이상의 보조 분자에 연결되며, 선택적으로 각 보조 분자는 동일하거나 또는 다르거나 또는 같거나 상이한 분자의 혼합물이다. 더 바람직하게 하나 이상의 보조 분자는 다합체 또는 링커를 통해 p75NTR(NBP)에 연결된 복수의 보조 분자를 포함하며, 각각의 분자는 동일하거나 또는 다르거나 또는 같거나 상이한 분자의 혼합물일 수 있다.
바람직하게 링커는 아미노산의 폴리펩티드 서열을 포함하거나 구성되며 하나 또는 복수의 아미노산을 포함하거나 구성되며, 바람직하게 약 1에서 약 25 아미노산, 바람직하게 1, 2, 3, 4, 5, 6, 7, 8 또는 9 아미노산 중 어느 하나, 더 바람직하게 약 10, 11, 12, 13, 14, 15, 16, 17, 18, 19, 20, 21, 22, 23 또는 24 아미노산 중 어느 하나, 가장 바람직하게 13 아미노산이다.
바람직하게 링커는 알파 헬릭스, 베타 스트렌드, 310 헬릭스 및 pi 헬릭스, 폴리프롤린 헬릭스, 알파 시트와 같은 어떤 안정한 2차 구조가 결핍된 아미노산의 폴리펩티드 서열을 포함하거나 구성된다. 바람직하게 링커 영역은 예를 들어 가연성 루프, 랜덤 코일 또는 가연성 턴과 같은 유연한 또는 동적인 또는 비구조화된 폴리펩티드를 규정하는 아미노산의 폴리펩티드 서열을 포함하거나 구성되며, 비구조화된 폴리펩티드는 종종 큰 단백질 분자 내에서 2차 구조를 연결하는 영역이 발견된다.
바람직하게 링커는 p75NTR(NBP)에 약 50% 이상의 글리신 및/또는 알라닌 및/또는 세린을, 더 바람직하게는 p75NTR(NBP)에 약 55%, 60%, 70%, 75%, 80%, 85%, 90%, 95% 또는 10% 이상의 글리신 및/또는 알라닌 및/또는 세린을 포함하는 아미노산의 폴리펩티드 서열이다. 바람직하게 링커 영역은 글리신 및 세린을 모두, 바람직하게는 세린보다 글리신의 비율을 더 크게 포함하는 아미노산의 폴리펩티드 서열을 포함하거나 구성되며, 바람직하게 링커 영역은 유연성 링커, SEQ ID NO. 17 (GGGGS)n(n= 1 - 4), 나선형 링커, SEQ ID NO. 18 (EAAAK)n (n = 2 - 5) 또는 글리신, 세린, 알라닌 및 각각의 아미노산의 1 내지 10 반복 범위를 가지는 트레오닌 및 그들의 조합으로부터 선택되는 아미노산 잔류물을 우세하게 포함하는 아미노산폴리펩티드 링커를 포함하거나 구성된다.
바람직하게 링커는 보조 분자에 연결되지 않는 p75NTR(NBP)와 비교할 때 상기한 p75NTR(NBP)의 뉴로트로핀 결합 능력 또는 생물학적 활성을 간섭할 수 있는 보조 분자로부터 입체 장애를 극복하거나 또는 방지한다. 이로 인해 링커 영역은 바람직하게 p75NTR(NBP)와 보조 분자 사이의 유연성을 허용하며, 그렇게 연결되지 않은 유리 또는 천연 p75NTR(NBP)와 비교하여 예를 들어 여기서 설명된 결합 분석법을 사용하여 뉴로트로핀에 결합시키는 것에 의해 결정되는 것과 같은 상기한 p75NTR(NBP)의 생물학적 활성의 보유 또는 개선을 허용한다.
더 바람직하게 링커는 보체의존성 세포용해반응(complement mediated lysis)을 촉발하지 않도록 면역학적으로 불활성이며, 항체의존성 세포 매개성 세포독성(antibody-dependent cell mediated cytotoxicity, ADCC)을 자극하지 않으며, 미세아교세포(microglia) 또는 T-세포를 활성화하지 않는다. 바람직하게 링커 영역은 하나 이상의 이들의 활성에서 감소된다.
더 바람직하게 링커는 유연한 또는 동적인 또는 비구조환된 폴리펩티드이거나 또는 안정한 2차 구조가 결핍된 알려져 있거나 또는 구조 분석 또는 구조 예측으로부터 예견되는 폴리펩티드를 포함하거나 구성된다.
가장 바람직하게 링커는 SEQ ID NO. 19(GGGGS)인 폴리펩티드 서열을 포함하거나 구성된다.
본 발명의 p75NTR(NBP)는 또한 단백질 분해 절단 부위를 포함할 수도 있으며, 선택적으로 p75NTR(NBP)와 보조 분자 사이에 배치될 수 있다. 단백질 분해 절단 부위는 p75NTR(NBP) 또는/및 보조 분자를 가지는 링커 내에 또는 링커의 연결부에 위치할 수 있다. p75NTR(NBP)는 치료학적 목적을 위한 제형화 및/또는 투여에 앞서 선택적으로 보조 분자로부터 제거될 수도 있다.
바람직하게 링커 및/또는 하나 이상의 보조 분자는 p75NTR(NBP)를 손상시키지 않거나 상당히 손상시킨다:
(a) 뉴로트로핀(뉴로트로핀의 기능적 활성을 조정하거나 또는 상향 또는 하향 조절하는 것으로 규정되는) NGF, BDNF, NT3 또는 NT4/5의 기능적 활성에 미치는 영향,
(b) 약 0.1nM에서 약 50nM 사이의 결합 친화도를 가지는 NGF, BDNF, NT3 또는 NT4/5 중 어느 하나에 대한 결합친화도,
(c) 각각의 뉴로트로핀 NGF, NT3, BDNF 및 NT4/5, 바람직하게 인간 NGF, NT3, BDNF 및 NT4/5에 대한 결합 능력.
본 발명의 일 및 이 측면의 바람직한 구현예에 따르면, 본 발명의 p75NTR(NBP)는 통증을 치료하기 위한 용도를 위해 하기로 구성되는 p75NTR(NBP)가 제공된다: (A) 서열 SEQ ID NO. 3의 p75NTR(NBP), 및 선택적으로 (B) 면역글로불린 Fc, 및 더 선택적으로 SEQ ID NO. 11로 구성되는 면역글로불린 Fc 및 선택적으로 (C) 링커, 선택적으로 SEQ ID NO. 9로 구성되는 링커.
본 발명의 제3 측면에 따르면, 본 발명의 제1 또는 제2 측면에 따르는 p75NTR(NBP) 또는 하나 이상의 보조 분자에 연결된 p75NTR(NBP)를 엔코딩하는 핵산 분자가 제공된다. 바람직하게 핵산 분자는 통증의 치료를 위한 용도이다.
본 발명의 바람직한 구현예에 따르면, 핵산 분자는 신호 서열을 엔코딩하는 영역, 바람직하게 p75NTR(NBP) 신호 서열, 예를 들어 DNA 또는 RNA 서열을 더 포함할 수도 있다.
본 발명의 제4 측면에 따르면, 세포를 트랜스펙션하기 위한 복제가능한 발현 벡터가 제공되며, 벡터는 제3 측면의 핵산 분자를 포함하며, 바람직하게 벡터는 바이러스성 벡터이다. 바람직하게 벡터는 통증의 치료를 위한 용도이다.
본 발명의 제3 또는 제4 측면에 따르면, p75NTR(NBP) 또는 하나 이상의 보조 분자에 연결된 p75NTR(NBP)를 생산 또는 분비하기 위해 본 발명의 핵산 분자 또는 벡터를 발현시키기 위한 방법이 제공된다. 바람직하게 본 방법은 세포 내로 핵산 분자 또는 벡터의 도입과 p75NTR(NBP) 또는 하나 이상의 보조 분자에 연결된 p75NTR(NBP)를 생산 또는 분비하기 위해 세포 내에서 핵산의 발현을 포함한다. 바람직하게 핵산 분자 또는 벡터는 인비트로에서 대안적으로 인비보에서 세포 내로 도입된다. 바람직하게 발현된 p75NTR(NBP) 또는 하나 이상의 보조 분자에 연결된 p75NTR(NBP)는 인비트로에서 발현되고, 선택적으로 더 분리되고 정제되며, 대안적으로 바람직하게 발현된 p75NTR(NBP) 또는 하나 이상의 보조 분자에 연결된 p75NTR(NBP)는 인비보에서 발현되고, 바람직하게 인비보 발현은 유전자 치료에 기여한다. 바람직하게 벡터는 복제 가능한 발현 벡터이며, 선택적으로 포유류 세포를 트랜스팩션하기 위한 것이며, 바람직하게 벡터는 바이러스성 벡터이다.
본 발명의 제5 측면에 따르면, 본 발명의 제3 또는 제4 측면에 따른 핵산 분자 또는 벡터를 함유하는 숙주 세포가 제공되며, 바람직하게 세포는 포유류 세포이다.
본 발명의 제6 측면에 따르면, 본 발명의 제1 또는 제2 측면 또는 그들의 바람직한 구현예에 따르는 용도를 위한 p75NTR(NBP) 또는 본 발명의 제3 또는 제4 측면에 따른 핵산 또는 벡터가 제공되며, 여기에서 통증 또는 통증의 증후는 하기로부터 선택된다:
(a) 급성 통증 및/또는 자발통,
(b) 만성 통증 및/또는 진행성 통증,
(c) 관절염 통증, 골관절염 또는 류마티스성 관절염으로부터 오는 통증, 염증성 장 질환으로부터 오는 통증, 건선 및 습진의 어느 것을 포함하는 염증성 통증,
(d) 침해성 통증(nociceptive pain),
(e) 고통스러운 당뇨병성 신경병증 또는 포진 후 신경통과 관련되는 통증을 포함하는 신경병성 통증,
(f) 통각 과민,
(g) 이질통,
(h) 중추성 통증, 뇌졸중 후 중추성 통증, 다발성 경화증으로부터 오는 통증, 척수 손상으로부터 오는 통증, 파킨슨병 또는 뇌전증으로부터 오는 통증,
(i) 암성 통증,
(j) 수술 후 통증,
(k) 소화기 내장성 통증 및 비소화기 내장성 통증을 포함하는 내장통(visceral pain), 위장관병(gastrointestinal (GI) disorders)에 기인하는 통증, 기능성 장질환(functional bowel disorders(FBD))으로부터 오는 통증, 염증성 장질환(inflammatory bowel diseases(IBD))으로부터 오는 통증, 월경통, 골반통, 방광염, 간질성 방광염 또는 췌장염으로부터 오는 통증,
(l) 근골격계 통증, 근육통, 섬유근육통, 척추염, 혈청 음성(비류머티즘성) 관절통증, 비-관절성 류머티즘, 근이영양증(dystrophinopathy), 글리코겐 분해, 다발성 근육염, 화농성 근염,
(m) 심장 또는 혈관 통증, 협심증에 의한 통증, 심근경색, 승모판막 협착증, 심낭염, 레이노 증후군, 공피증(scleredoma), 공피증 또는 골격근 허혈,
(n) 편두통, 조짐편두통, 무조짐편두통, 군발두통, 긴장성 두통을 포함하는 두통,
(o) 치통, 턱관절 근막통증(temporomandibular myofascial pain) 또는 이명을 포함하는 구강안면 통증, 또는
(p) 요통, 윤활낭염, 월경통, 편두통, 연관통, 삼차 신경병증, 하이퍼센티세이션(hypersensitisation), 척수 외상 및/또는 변성(degeneration) 또는 뇌졸중(stroke)으로부터 오는 통증.
본 발명의 제7 측면에 따르면, 본 발명의 제1 또는 제2 측면 또는 그들의 바람직한 구현예에 따른 용도를 위한 p75NTR(NBP), 또는 본 발명의 제3 또는 제4 측면에 따른 용도를 위한 핵산 분자 또는 벡터가 제공되며, p75NTR(NBP) 또는 핵산 분자 또는 벡터는 약물학적 활성 화합물과 결합된 조합에서 별개로, 연속적으로 또는 동시 사용을 위한 것이다. 바람직하게 조합의 제2 약물학적 활성 화합물은 하기로부터 선택된다:
- 모르핀, 헤로인, 하이드로모르폰, 옥시모르폰, 레보파놀, 레발로판, 메타돈, 메페리딘, 펜타닐, 코카인, 코데인, 디하이드로코데인, 옥시코돈, 하이드로코돈, 프로폭시펜, 날메펜, 날로핀, 날록손, 날트렉손, 부프레노르핀, 부토르파놀, 날부핀 또는 펜타조신과 같은 오피오이드 진통제;
- 아스피린, 디클로페낙, 디플루시날, 에토돌락, 펜부펜, 페노프로렌, 플루페니살, 플루비프로펜, 이부프로펜, 인도메타신, 케토프로펜, 케토롤락, 메클로페남산, 메페남산, 멜록시캄, 나부메톤, 나프록센, 니메술리드, 니트로플루비프로펜, 올살라진, 옥사프로진, 페닐부타존, 피록시캄, 설파알라진, 술린닥, 톨메틴 또는 조메피락과 같은 비스테로이드성 항염증성 약물(NSAID);
- 아모바비탈, 아프로바비탈, 부타바비탈, 부타비탈, 메포바비탈, 메타르비탈, 메쏘헥시탈, 펜토바비탈, 페노바비탈, 세코바비탈, 탈부탈, 티아미랄(theamylal) 또는 티오펜탈과 같은 수면 진정제(barbiturate sedative);
- 클로르디아제폭시드, 클로라제페이트, 디아제팜, 플루라제팜, 로라제팜, 옥사제팜, 테마제팜 또는 트리아졸람과 같은 진정 작용이 있는 벤조디아제핀;
- 디펜히드라민, 피릴라민, 프로메타진, 클로르페니라민 또는 클로르사이클리진과 같은 진정 작용이 있는 H1 길항제;
- 글루테티이미드, 메프로바메이트, 메타쿠알론 또는 디클로랄페나존과 같은 진정제;
- 바클로펜, 카리소프로돌, 클로르족사존, 시클로벤자프린, 메토카바몰 또는 오르프레나딘과 같은 골격근이완제;
- 덱스트로메트로판(dextromethorphan)((+)-3-하이드록시-N-메틸모르피난((+)-3-hydroxy-N-methylmorphinan)) 또는 그것의 대사산물 덱스트로판(dextrorphan)((+)3-하이드록시-N-메틸모르피난), 케타민, 메만틴, 피롤로퀴놀린 퀴닌, 시스-4-(포스포노메틸)-2-피페리딘카복시산, 부디핀, EN-3231(MorphiDex®, 모르핀과 덱스트로메트로판의 조합 제제), 토피라메이트, 네라멕산 또는 이펜프로딜, 트락소프로딜 또는 (-)-(R)-6-{2-[4-(3-플루오로페닐)-4-하이드록시-1-피페리디닐]-1-하이드록시에틸-3,4-디하이드로-2(1H)-퀴놀리논과 같은 NR2B 길항제를 포함하는 페르진포텔과 같은 NMDA 수용체 길항제;
- 독사조신, 탐술로신, 클로니딘, 구안파신, 덱스메타토미딘, 모다피닐, 또는 4-아미노-6,7-디메톡시-2-(5-메탄-술폰아미도-1,2,3,4-테트라하이드로이소퀴놀-2-일)-5-(2-피리딜) 퀴나졸린)과 같은 알파-수용체;
- 데시프라민, 이미프라민, 아미트립틸린 또는 노르트립틸린과 같은 삼환계 항우울제;
- 카바마제핀, 라모트리진, 토피라트메이트 또는 발프로에이트와 같은 경련 예방제;
- (αR,9R)-7-[3,5-비스(트리플루오로메틸)벤질]-8,9,10,11-테트라하이드로-9-메틸-5-(4-메틸페닐)-7H-[1,4]디아조시노[2,1-g][1,7]-나프티리딘-6-13-디온(TAK-637), 5-[[(2R,3S)-2-[(1R)-1-[3,5-비스(트리플루오로메틸)페닐]에톡시-3-(4-플루오로페닐)-4-모르폴리닐]-메틸]-1,2-디하이드로-3H-1,2,4-트리아졸-3-온(MK-869), 아프레피탄트, 라네피탄트, 다피탄트 또는 3-[[2-메톡시-5-(트리플루오로메톡시)페닐]-메틸아미노]-2-페닐피페리딘(2S,3S)과 같은 타치키닌 (NK) 길항제(tachykinin (NK) antagonist), 특히 NK-3, NK-2 또는 NK-1 길항제;
- 옥시부티닌, 톨테로딘, 프로피베린, 염화트로스피움, 다리페나신, 솔리페나신, 테미베린 및 이프라트로피움과 같은 무스카린 길항제;
- 셀레콕시브, 로페콕시브, 파레콕시브, 발데콕시브, 데라콕시브, 에토리콕시브 또는 루미라콕시브와 같은 COX-2 선택적 저해제;
- 콜-타르 수용체(coal-tar analgesic), 특히 파라세타몰;
- 드로페리돌, 클로르프로마진, 할로페리돌, 페르페나진, 티오리다진, 메소리다진, 트리플루오페라진, 플루페나진, 클로자핀, 올란자핀, 리스페리돈, 지프라시돈, 퀘티아핀, 세르틴돌, 아리피프라졸, 소네피프라졸, 블로난세린, 일로페리돈, 페로스피론, 라클로프라이드, 조테핀, 비페프루녹스, 아세나핀, 루라시돈, 아미술프라이드, 발라페리돈, 팔린도르(palindore), 에플리반세린, 오사네탄트, 리모나반트, 메클리네르탄트(meclinertant), 미락시온(Miraxion®) 또는 사리조탄과 같은 신경이완제;
- 바닐로이드 수용체 작용제(예. 레신페라톡신) 또는 길항제(예. 캅사제핀);
- 프로파놀롤과 같은 베타-수용체;
- 멕실레틴과 같은 국소마취제;
- 덱사메타손과 같은 코르티코스테로이드;
- 5-HT 수용체 작용제 또는 길항제, 특히 엘레트립탄, 수마트립탄, 나라트립탄, 졸미트립탄 또는 리자트립탄과 같은 5-HT1B /1D 작용제;
- R(+)-알파-(2,3-디메톡시-페닐)-1-[2-(4-플루오로페닐에틸)-4-피페리딘메탄올(MDL-100907)과 같은 5-HT2A 수용체 길항제;
- 이스프로닉클린(TC-1734), (E)-N-메틸-4-(3-피리디닐)-3-부텐-1-아민(RJR-2403), (R)-5-(2-아제티디닐메톡시)-2-클로로피리딘(ABT-594) 또는 니코틴과 같은 콜린성(니코틴성) 수용체;
- 트라마돌(Tramadol®);
- 5-[2-에톡시-5-(4-메틸-1-피페라지닐-설포닐)페닐]-1-메틸-3-n-프로필-1,6-디하이드로-7H-피라졸로[4,3-d]피리미딘-7-온(실데나필), (6R,12aR)-2,3,6,7,12,12a-헥사하이드로-2-메틸-6-(3,4-메틸렌디옥시페닐)-파라지노[2',1':6,1]-피리도[3,4-b]인돌-1,4-디온(IC-351 또는 타다라필), 2-[2-에톡시-5-(4-에틸-피페라진-1-일-1-설포닐)-페닐]-5-메틸-7-프로필-3H-이미다조[5,1-f][1,2,4]트라아진-4-온(바르데나필), 5-(5-아세틸-2-부톡시-3-피리디닐)-3-에틸-2-(1-에틸-3-아제티디닐)-2,6-디하이드로-7H-피라졸로[4,3-d]피리미딘-7-온, 5-(5-아세틸-2-프로폭시-3-피리디닐)-3-에틸-2-(1-이소프로필-3-아제티디닐)-2,6-디하이드로-7H-피라졸로[4,3-d]피리미딘-7-온, 5-[2-에톡시-5-(4-에틸피페라진-1-일설포닐)피리딘-3-일]-3-에틸-2-[2-메톡시에틸]-2,6-디하이드로-7H-피라졸로[4,3-d]피리미딘-7-온, 4-[(3-클로로-4-메톡시벤질)아미노]-2[(2S)-2-(하이드록시메틸)피롤리돈-1-일]-N-(피리미딘-2-일메틸)피리미딘-5-카르복스아미드, 3-(1-메틸-7-옥소-3-프로필-6,7-디하이드로-1H-피라졸로[4,3-d]피리미딘-5-일)-N-[2-(1-메틸피롤리딘-2-일)에틸]-4-포폭시벤젠설폰아미드와 같은 PDEV 저해제;
- 카나비노이드;
- 대사형 글루탐산 서브타입 1 수용체(mGluR1) 길항제;
- 세르트랄린, 세르트랄린 대사산물 데메틸세르트랄린, 플루옥세틴, 노르플루옥세틴(플로옥세틴 데스메틸 대사산물), 플루복사민, 파록세틴, 시탈로프람, 시탈로프람 대사산물 데스메틸시탈로프람, 에스시탈로프람, d,l-펜플루라민, 페목세틴, 이폭세틴, 시아노도티에핀, 리톡세틴, 다폭세틴, 네파조돈, 세리클라민 및 트라조돈과 같은 세로토닌 재흡수 저해제;
- 마프로틸린, 로페프라민, 미르타제핀, 옥사프로틸린, 페졸라민, 토목세틴, 미안세린, 부프로프리온, 부프로프리온 대사산물 하이드록시부프로프리온, 노미펜신 및 빌록사진(Vivalan®)과 같은 노르아드레날린(노르에피네프린) 재흡수 저해제, 특히 레복세틴, 특별히 (S,S)-레복세틴과 같은 선택적 노르아드레날린 재흡수 저해제;
- 벤라팍신, 벤라팍신 대사산물 O-데스메틸벤라팍신, 클로미프라민, 클로미프라민 대사산물 데스메틸클로미프라민, 듈록세틴, 밀낙프란 및 이미프라민과 같은 이중 세로토닌-노르아드레날린 재흡수 저해제;
- S-[2-[(1-이미노에틸)아미노]에틸]-L-호모시스테인, S-[2-[(1-이미노에틸)-아미노]에틸]-4,4-디옥소-L-시스테인, S-[2-[(1-이미노에틸)아미노]에틸]-2-메틸-L-시스테인, (2S,5Z)-2-아미노-2-메틸-7-[(1-이미노에틸)아미노]-5-헵탄산, 2-[[(1S,3S)-3-아미노-하이드록시-1-(5-티아졸릴)부틸]티오]-5-클로로-3-피리딘카보니트릴, 2-[[(1S,3S)-3-아미노-하이드록시-1-(5-티아졸릴)부틸]티오]-4-클로로벤조니트릴, (2S,4R)-2-아미노-4-[[2-클로로-5-(트리플루오로메틸)페닐]티오]-5-티아졸부탄올, 2-[[(1R,3S)-3-아미노-4-하이드록시-1-(5-티아졸릴) 부틸]티오]-6-(트리플루오로메틸)-3-피리딘카보니트릴, 2-[[(1R,3S)-3-아미노-4-하이드록시-1-(5-티아졸릴) 부틸]티오]-5-클로로벤조니트릴, N-[4-[2-(3-클로로벤질아미노)에틸]페닐]티오펜-2-카르복스아미딘, 또는 구아니디노에틸디설파이드와 같은 유도성 산화질소 합성효소(inducible nitric oxide synthase (iNOS)) 저해제;
- 도네페질과 같은 아세틸콜린에스테라아제;
- N-[({2-[4-(2-에틸-4,6-디메틸-1H-이미다조[4,5-c]피리딘-1-일)페닐]에틸}아미노)-카보닐]-4-메틸벤젠설폰아미드 또는 4-[(1S)-1-({[5-클로로-2-(3-플루오로페녹시)피리딘-3-일]카보닐}아미노)에틸]벤조산과 같은 프로스타글란딘 E2 서브타입 4(EP4) 길항제;
- 1-(3-비페닐-4-일메틸-4-하이드록시-크로만-7-일)-시클로펜탄카복시산(CP-105696), 5-[2-(2-카복시에틸)-3-[6-(4-메톡시페닐)-5E-헥세닐]옥시페녹시]-발레산(ONO-4057) 또는 DPC-11870과 같은 류코트리엔 B4 길항제;
- 질류톤, 6-[(3-플루오로-5-[4-메톡시-3,4,5,6-테트라하이드로-2H-vlfks-4-일])페녹시-메틸]-1-메틸-2-퀴놀론(ZD-2138), 또는 2,3,5-트리메틸-6-(3-피리딜메틸)-1,4-벤조퀴논(CV-6504)와 같은 5-리폭시게나아제 저해제;
- 리도카인과 같은 소듐 채널 차단제; 또는
- 온단세트론과 같은 5-HT3 길항제;
및 약학적으로 수용가능한 염 및 그들의 용매화물.
본 발명의 제8 측면에 따르면, 본 발명의 제1, 제2 또는 제7 측면 또는 그들의 바람직한 구현예에 따른 p75NTR(NBP), 또는 본 발명의 제3 및 제4 측면에 따른 핵산 분자 또는 벡터의 유효량을 개인에게 투여하는 것을 포함하는, 개인(individual)에게서 통증 또는 앞서 언급한 통증 및/또는 통증 증후 중 어느 하나의 치료, 예방, 완화, 제어, 발생 감소, 또는 발전 또는 진전을 지연시키기 위한 방법이 제공된다.
바람직하게 개인은 포유류이고, 예를 들면 말, 고양이 또는 개와 같은 반려동물(companion animal) 또는 양, 소 또는 돼지와 같은 농장동물이다. 가장 바람직하게 포유류는 인간이다.
본 발명의 제9 측면에 따르면, 본 발명의 제1, 제2 또는 제7 측면 또는 그들의 바람직한 구현예에 따른 p75NTR(NBP), 또는 본 발명의 제3 및 제4 측면에 따른 핵산 분자 또는 벡터 및 약학적으로 수용가능한 담체 및/또는 첨가제를 포함하는, 통증 또는 앞서 언급한 통증 및/또는 통증 증후 중 어느 하나의 치료, 예방, 완화, 제어, 발생 감소, 또는 발전 또는 진전의 지연 중 어느 하나 이상을 위한 약학적 조성물이 제공된다.
바람직하게 본 발명의 제1, 제2 또는 제7 측면에 따른 p75NTR(NBP) 또는그들의 바람직한 구현예, 또는 제3 및 제4 측면에 따른 핵산 분자 또는 벡터 또는 제9 측면에 따른 약학적 조성물이 경구, 설하, 구강(buccal), 국소적, 직장, 흡입, 경피, 피하, 정맥주사, 동맥내, 근육내, 심장내, 골내, 피내, 복강내, 경점막(transmucosal), 질, 유리체내(intravitreal), 관절내, 관절주위, 인체 일부 또는 에피큐테니어스(epicutaneous) 투여를 위해 제조되거나 또는 적합하다.
바람직하게 본 발명의 제1, 제2 또는 제7 측면 또는 그들의 바람직한 구현예에 따른 p75NTR(NBP), 또는 제3 및 제4 측면에 따른 핵산 분자 또는 벡터 또는 제9 측면에 따른 약학적 조성물이 통증의 시작에 앞서 및/또는 동안 및/또는 후에 투여를 위해 또는 그러한 용도를 위해 제조되거나 또는 적합하다.
바람직하게 본 발명의 제1, 제2 또는 제7 측면 또는 그들의 바람직한 구현예에 따른 p75NTR(NBP), 또는 제3 및 제4 측면에 따른 핵산 분자 또는 벡터 또는 제9 측면에 따른 약학적 조성물이 주당 1회에서 7회 사이의, 더 바람직하게는 월당 1회에서 4회 사이의, 더 바람직하게 6개월 기간당 1회에서 6회 사이의, 더 바람직하게 년당 1회에서 12회 사이의 투여를 위한 것이거나 또는 투여를 위해 제조된다. 바람직하게 약제는 하루에 한 번, 이틀에 한 번, 3일에 한 번, 4일에 한 번, 5일에 한 번 또는 6일에 한 번, 매주, 2주에 한 번, 3주에 한 번, 매달, 두 달에 한 번, 세 달에 한 번, 네 달에 한 번, 다섯 달에 한 번, 여섯 달에 한 번, 일곱 달에 한 번, 여덟 달에 한 번, 아홉 달에 한 번, 열 달에 한 번, 열한 달에 한 번 또는 매년에서 선택되는 기간에 투여되거나 투여되도록 제조된다.
더 바람직하게 본 발명의 제1, 제2 또는 제7 측면 또는 그들의 바람직한 구현예에 따른 p75NTR(NBP), 또는 제3 및 제4 측면에 따른 핵산 분자 또는 벡터 또는 제9 측면에 따른 약학적 조성물이 경구적으로, 설하로, 구강(buccal)으로, 국소적으로, 직장내로, 흡입으로, 경피로, 피하로, 정맥주사로, 동맥내로 또는 근육내로, 심장내 투여를 통해, 골내로, 피내로, 복강내로, 경점막(transmucosal)으로, 질로, 유리체내(intravitreal)로, 에피큐테니어스(epicutaneous)로, 관절내로, 관절주위로 또는 인체 일부로부터 선택되는 하나 이상의 경로를 통해 말초적으로 투여되거나 투여를 위해 제조된다.
바람직하게 본 발명의 제1, 제2 또는 제7 측면 또는 그들의 바람직한 구현예에 따른 p75NTR(NBP), 또는 제3 및 제4 측면에 따른 핵산 분자 또는 벡터 또는 제9 측면에 따른 약학적 조성물이 약 0.1에서 200mg/ml 사이의 농도에서 투여를 위한 것이거나 또는 투여를 위해 제조된다; 바람직하게 약 0.5, 1, 5, 10, 15, 20, 25, 30, 35, 40, 45, 50, 55, 60, 65, 70, 75, 80, 85, 90, 95, 100, 110, 120, 130, 140, 150, 160, 170, 180, 190 또는 200 mg/ml +/- 약 10% 오차 중 어느 하나에서, 가장 바람직하게는 약 50 mg/ml에서 투여되거나 투여를 위해 제조된다.
바람직하게 본 발명의 제1, 제2 또는 제7 측면 또는 그들의 바람직한 구현예에 따른 p75NTR(NBP), 또는 제3 및 제4 측면에 따른 핵산 분자 또는 벡터 또는 제9 측면에 따른 약학적 조성물이 kg 체중당 약 0.1에서 약 200mg 사이의 농도에서 투여되거나 또는 투여를 위해 제조된다; 바람직하게 약 0.5, 1, 5, 10,15 20, 25, 30, 35, 40, 45, 50, 55, 60, 65, 70, 75, 80, 85, 90, 95, 100, 110, 120, 130, 140, 150, 160, 170, 180, 190 또는 약 200 mg/체중 kg +/- 약 10% 오차 중 어느 하나에서, 가장 바람직하게는 약 10 mg/kg에서 투여되거나 투여를 위해 제조된다.
본 발명의 제10 측면에 따르면, 하기를 포함하는 키트가 제공된다:
(a) 본 발명의 제1, 제2 또는 제7 측면 또는 그들의 바람직한 구현예에 따른 p75NTR(NBP), 또는 제3 및 제4 측면에 따른 핵산 분자 또는 벡터 또는 제9 측면에 따른 약학적 조성물; 및
(b) 통증 및/또는 통증 증후의 예방 또는 치료 중 어느 하나 이상 또는 통증 및/또는 통증 증후의 완화, 제어, 발생 감소, 또는 발전 또는 진전의 지연을 위해 개인에게 상기 p75NTR(NBP), 핵산 분자, 벡터 또는 약학적 조성물의 유효량 투여에 대한 지시서(instructions).
키트는 여기에 설명된 p75NTR(NBP), 핵산, 벡터 또는 약학적 조성물을 함유하는 하나 이상의 컨테이너와 본 발명의 방법 및 용도 중 어느 것에 따르는 사용을 위한 지시서를 포함할 수 있다. 키트는 개인이 통증 또는 통증의 증후를 가지고 있는지 혹은 그것들을 가지는 위험에 처했는지를 확인하는 것에 기초하는 치료를 위해 개인에게 적합한 것을 선택하는 설명서(descriptions)를 더 포함할 수 있다. 약학적 조성물의 투여를 위한 지시서는 복용량에 대한 정보, 복용 스케줄 및 의도된 치료를 위한 투여 경로에 대한 정보를 포함할 수 있다.
본 발명의 제11 측면에 따르면, 본 발명의 제1, 제2 또는 제7 측면 또는 그들의 바람직한 구현예에 따른 p75NTR(NBP), 또는 본 발명의 제3 및 제4 측면에 따른 핵산 분자 또는 벡터 또는 제9 측면에 따른 약학적 조성물이 뉴로트로핀 NGF, BDNF, NT-3, NT-4/5 중 하나 이상과 관련된 상태 또는 상태의 증후의 예방 또는 치료 중 어느 하나 이상의 용도를 위해 또는 완화, 제어, 발생 감소, 발전 또는 진전의 지연을 위해 제공된다.
NGF(Nerve growth factor, 신경영양성장인자)는 최소한 두 종류(class)의 수용체와 결합한다: p75NTR 및 TrkA, 트랜스멤브레인 티로신 키나아제, 그것이 축삭성장, 분지(branching) 및 신장에서 수반된다. NGF와 관련된 상태 및 증후는 알려져 있다. NGF는 염증 상태 및 통증에서 그리고 염증 상태 및 통증과 관련하여 발현된다[Protein Sequence NP_002497.2, NP_038637]. 또한, NGF는 관상동맥 죽상경화증, 비만, 타입 2 당뇨와 같은 심장혈관계 질환, 및 대사증후군뿐만 아니라 다발성 경화증 모두에 역할을 하는 것을 보여준다. NGF의(그리고 또한 BDNF의) 감소된 혈장 레벨은 급성 관상동맥증후군 및 대사증후군과 관련되어 있다. NGF는 치매, 우울증, 정신분열증, 자폐증, 레트 증후군, 신경성 식욕부진증 및 폭식증과 같은 다양한 정신 질환에 관련되며, 알츠하이머 질환 및 퇴행성 질환(neurodegenerative disorders)의 발전도 시사하고 있다. NGF는 또한 상처 치유를 가속화하는 것을 보여주며 피부 궤양 및 각막 궤양의 치료에 유용할 수 있다는 증거가 있으며, 래트에서 신경 퇴행(neural degeneration)을 감소시키고 말초신경 재생을 촉진하는 것을 보여준다.
BDNF(brain-derived neurotrophic factor, 뇌유래 신경영양인자)는 신경계의 발달동안 신경 생존 및 성장(neuronal survival and growth)을 지원하는 뉴로트로핀이다[Protein Sequence NP_001137277.1, NP_001041604]. BDNF는 세포 표면 수용체 TrkB 및 p75NTR을 결속시키고 또한 알파-7 니코틴성 수용체의 활성을 조정한다. BDNF와 관련된 상태 및 증후는 알려져 있다. BDNF는 생리학적 및 병리학적 통증의 전달(transmission)에서, 특히 급성 통증, 염증성 통증 및 신경병증성 통증 모델에서 중대한 역할을 하는 것으로 나타나고 있으며, 여기서 BDNF 합성은 크게 증가되는 것으로 발견되며; 또한 BDNF는 만성 통증 상태뿐만 아니라 습진과 건선과 같은 상태에서도 상향-조절되는 것이 나타나고 있다. BDNF의 하향-조절은 우울증, 정신분열증, 강박장애, 알츠하이머 질환, 헌팅턴병, 레트 증후군 및 치매, 뿐만 아니라 신경성 식욕부진증 및 폭식증에서 보인다.
또한 뉴로트로핀-5(NT-5)로 알려져 있는 뉴로트로핀-4(NT-4)는 p75NTR 및 TrkB를 통해서 대개 신호를 보내는 신경영양인자이며 말초감각 교감뉴런(peripheral sensory sympathetic neurons)의 생존을 촉진한다. 이 단백질의 성숙한 펩티드는 인간, 돼지, 래트 및 쥐를 포함하여 조사된 모든 포유류에서 동일하다[Protein Sequence NP_006170, NP_937833]. NT-4는 배근 신경절(dorsal root ganglion, DRG)의 대부분의 뉴런과 척추앞 및 척추앞 교감신경절(prevertebral sympathetic ganglia), 척수 후각 및 전각(spinal dorsal and ventral horn) 내 뉴런에 의해 합성되며 전립선, 흉선, 태반과 골격근을 포함하는 많은 조직에서 발현되는 것이 발견된다. NT-4/5와 관련된 상태 및 증후는 알려져 있다. NT4/5에서 결함은 원발성 개방각 녹내장(primary open angle glaucoma)에 대한 감수성과 연관된다. 뉴로트로핀 4는 유방암 세포 생존에도 기여하는 것으로 나타났으며 종양 성장을 억제하기 위한 표적이다. NT-4/5는 침해성 통증과 같은 통증-신호 시스템(pain-signalling systems)에서 수반되는 것이 알려져 있으며, NT-4/5의 상향조절은 또한 피부염, 습진, 아토피성 피부염의 양진 병변과 같은 피부의 만성 염증성 상태에서 보인다. NT-4/5의 하향 조절은 알츠하이머 질환, 헌팅턴병에서 보인다.
뉴로트로핀-3(NT-3)는 베타-NGF, BDNF 및 NT-4에 구조적으로 관련되는 뉴로트로핀이며 포유류 뉴런의 생존 및 분화와 성인 신경계의 유지를 조절하고, 인간 태반에서 발현될 때 배아에서 뉴런의 발전에 영향을 줄 수 있다. NT3와 관련된 상태 및 증후는 알려져 있다. 표적 유전자에 의해 생성된 NTF3-결핍 쥐가 심각한 사지의 운동 결함을 나타낸다. NT-3는 Trk 수용체를 통해 신호를 보내고 신경 및 신경교세포의 성장 및 생존을 촉진한다[Protein Sequence NP_001096124.1 및 NP_032768]. 인간, 쥐 및 래트 NT-3의 아미노산 서열은 동일하다. NT3 및 그것의 동종(cognate) 수용체, 티로신 키나아제 C(TrkC)가 신경병증성 통증 및 침해성 통증을 조정하는 것으로 알려져 있으며 통각수용 및 고유수용성 감각의 메카니즘(mechanism of nociception and proprioception), 예를 들면 NT3 발현이 신경병증성 동물의 작은 DRG 세포에서 증가된다. NT3 발현은 또한 당뇨병성다발신경병증 및 HIV-관련 신경병증과 같은 신경병증, 위축을 포함하는 굵은 섬유 신경병증과 관련되며, 그것은 통각과민(정상적으로 유해한 자극의 역치에서 감소), 이질통(비-유해성 자극이 유해성으로 된다), 및 자발통(명백한 자극 부재에서의 통증)에서 또한 수반되며 근육통의 알려진 조절자이다.
본 발명은 하기 실시예를 참조하여 상세히 설명될 것이나, 본 발명이 이에 제한되지 않는다.
하기 실시예는 본 발명을 제한하기 위한 것이 아니라 설명하기 위해 제공된다.
실시예
실시예 1. 내생의 p75NTR(NBP)-뉴로트로핀 복합체가 인간 혈장에서 검출된다.
인간 혈장에서 p75NTR/NGF 복합체의 존재에 대한 직접 증거를 제공하기 위해 SISCAPA((Siscapa http://siscapa.com/home.html)에 이어서 NGF에 기초한 마그네틱 비드를 이용하는 분석법(Millipore Corp; MA)과 바이오티닐화된 염소 다클론성 항-인간 NGF 항체(Novus Biologicals; CO)를 이용하는 면역침강법 후에 LC-MS/MS(LLOQ 7pg/ml)에서 확인하는 방법이 채용되었다. 다클론성 항-NGF 항체가 인간 혈청/혈장 내 유리 NGF를 수량화하기 위해 사용되었다.
p75NTR의 세포외 도메인의 펩티드 서열(CAYGYYQDETTGR(SEQ ID NO. 4) VCEAGSGLVFSCQDK(SEQ ID NO. 6) WADAECEEIPGR(SEQ ID NO. 7))(도 2에 나타낸 바와 같이)이 키메라 소화에 이어서 LC-MS/MS에 의해 p75NTR 표준으로서 선택되었다. 전체 NGF 분석법(상기에서 설명된 대로)에서 검출된 p75NTR의 공동면역침강법(Co-immunoprecipitation)은 인간 혈청에서 가용성 p75-NGF 복합체의 증거를 제공하는 p75NTR 제어 펩티드(control peptides)의 존재를 입증할 수 있었다. 또한 p75NTR(NBP)와 BDNF, NT-3 및 NT4/5의 유사한 상호작용을 각각 BDNF, NT-3 및 NT4/5 항체로 공동면역침강법을 이용하여 밝혀내었다. 이들 연구는 NGF, BDNF, NT-3 및 NT4/5 중의 어느 것에 결합된 인간의 혈장 내 가용성 p75 뉴로트로핀 결합 단백질의 존재를 입증한다.
도 2에 제시된 데이터는 가용성 p75NTR(NBP) 펩티드 표준 절편과 인간 혈장에서 p75NTR(NBP)-NGF 복합체를 입증하는 p75NTR(NBP)와 NGF의 공동면역침강을 보여준다. 인간 혈장에서 p75NTR(NBP)-NGF 공동면역침강 연구의 결과에 따른 증거이며, 뉴로트로핀-p75NTR(NBP) 복합체에서 결합에 수반되는 키 펩티드는 WADAECEEIPGR(SEQ ID NO. 7), CAYGYYQDETTGR(SEQ ID NO. 4), VCEAGSGLVFSCQDK(SEQ ID NO. 6)이며, 추가적으로 서열 LDSVTSDVVSATEPCKP(SEQ ID NO. 8)가 결합시에 또한 중요하다는 것을 알아내었다.
p75NTR(NBP)의 동일한 키 결합 영역의 중요성을 보여주고 인간 혈장 내 p75NTR(NBP)-BDNF와 p75NTR(NBP)-NT-3 복합체를 입증하는 BDNF 및 NT-3와 p75NTR(NBP)의 공동면역침강을 입증하는 실험이 BDNF와 NT-3로 반복되었다.
실시예 2. 가용성 p75NTR(NBP)는 TrkA를 발현하는 U20S 세포선과 TrkA와 p75NTR을 공동 발현하는 U20S 세포선에서 NGF 기능을 저해한다.
NGF 기능에서 p75NTR(NBP)의 효과는 TrkA를 발현하는 U20S 세포선과 TrkA와 p75NTR을 공동 발현하는 U20S 세포선에서 탐색되었다(Discoverx Corp CA). 분석이 패스헌터 방법론(PathHunter methodology)(Discoverx Corp CA)에 따라서 간략하게 수행되었으며, TrkA와 TrkA+p75NTR을 발현하는 U20S 세포를 DiscoveRx Corporation에서 샀다. TrkA를 발현하는 U20S 세포와 TrkA+p75NTR을 공동 발현하는 세포를 최소 필수 배지(MEM; Sigma Aldrich)+0.5% 말 혈청(Sigma Aldrich)에 40,000세포/웰의 밀도로 깔고 37℃에서 밤새 배양했다. 플레이트를 사용에 앞서 30분 인큐베이터로부터 제거하고 실온에서 저장했다.
NGFα(Sigma Aldrich)와 p75NTR(NBP)-Fc(링커 SEQ ID NO. 17을 사용하는 IgG-Fc SEQ ID NO. 12에 연결된 p75NTR(NBP) SEQ ID NO. 2) 또는 p75NTR(NBP)(p75NTR(NBP) SEQ ID NO. 2) 또는 알부민에 연결된 p75NTR(NBP), SEQ ID NO. 10, 또는 트랜스페린에 연결된 p75NTR(NBP)(p75NTR(NBP) SEQ ID NO. 2), SEQ ID NO. 9를 행크 평형 염액 버퍼(Hanks Balanced Salt Solution Buffer)(HBSS Sigma Aldrich)를 더한 0.25% BSA에서 희석시켰다. NGF를 순차적으로 0nM에서 200nM 범위에 걸친 농도를 부여하기 위해 희석시켰다. Fc IgG, 알부민 또는 트랜스페린에 연결된 p75NTR(NBP)를 100ng/ml의 p75NTR의 농도를 부여하기 위해 HBSS에서 희석시켰다.
각 농도(0-200nM)의 NGF 5㎕와 p75NTR(NBP)+/-담체 5㎕를 각 웰에 첨가했다. p75NTR(NBP)+/-담체 및 NGF의 전배양시 영향(impact)을 이해하기 위한 시도에서 각 웰에 이 혼합물 10㎕를 첨가하기 전에 20분 동안 실온에서 배양되게 하였다. 즉시 NGF와 p75NTR(NBP)+/-담체의 첨가 후에 검출 용액(Discoverx Corp CA) 12㎕를 각 웰에 첨가하고 플레이트를 파크아드 빅터(Parkard Victor) 2 플레이트 리더에서 해독하기에 앞서 실온에서 60분 동안 배양되게 하였다. p75NTR(NBP)의 첨가에 대한 반응에서 용량반응 곡선과 곡선에서의 변화(shift)를 관찰했다. 담체없이 p75NTR(NBP)에 사용된 담체에 관계없이, NGF 용량반응 곡선에서 p75NTR(NBP)-Fc, p75NTR(NBP)-알부민 또는 p75NTR(NBP)-트랜스페린 억제와 변화를 관찰했다(도 4 참조).
실시예 3. p75NTR(NBP)는 TrkB를 발현하는 U20S 세포선과 TrkB 및 p75NTR을 공동발현하는 U20S 세포선에서 BDNF 기능을 저해한다.
BDNF 기능에서 p75NTR(NBP)의 효과를 TrkB를 발현하는 U20S 세포선과 TrkB 및 p75NTR을 공동발현하는 U20S 세포선에서 탐색하였다(Discoverx Corp CA). 분석이 패스헌터 방법론(PathHunter methodology)(Discoverx Corp CA)에 따라서 간략하게 수행되었으며, TrkB와 TrkB+p75NTR을 발현하는 U20S 세포를 DiscoveRx Corporation에서 샀다. TrkB를 발현하는 U20S 세포와 TrkB+p75NTR을 공동 발현하는 세포를 최소 필수 배지(MEM; Sigma Aldrich)+0.5% 말 혈청(Sigma Aldrich)에 40,000세포/웰의 밀도로 깔고 37℃에서 밤새 배양했다. 플레이트를 사용에 앞서 30분 인큐베이터로부터 제거하고 실온에서 저장했다.
BDNFα(Sigma Aldrich)와 p75NTR(NBP)-Fc(링커 SEQ ID NO. 17을 사용하는 IgG-Fc SEQ ID NO. 12에 연결된 p75NTR(NBP) SEQ ID NO. 2) 또는 p75NTR(NBP)(p75NTR(NBP) SEQ ID NO. 2) 또는 알부민에 연결된 p75NTR(NBP), SEQ ID NO. 10, 또는 트랜스페린에 연결된 p75NTR(NBP)(p75NTR(NBP) SEQ ID NO. 2), SEQ ID NO. 9를 행크 평형 염액 버퍼(Hanks Balanced Salt Solution Buffer)(HBSS Sigma Aldrich)를 더한 0.25% BSA에서 희석시켰다. BDNF를 순차적으로 0nM에서 200nM 범위에 걸친 농도를 부여하기 위해 희석시켰다. Fc IgG, 알부민 또는 트랜스페린에 연결된 p75NTR(NBP)를 100ng/ml의 p75NTR의 농도를 부여하기 위해 HBSS에서 희석시켰다.
각 농도(0-200nM)의 BDNF 5㎕와 p75NTR(NBP)+/-담체 5㎕를 각 웰에 첨가했다. p75NTR(NBP)+/-담체 및 BDNF의 전배양시 영향(impact)을 이해하기 위한 시도에서 각 웰에 이 혼합물 10㎕를 첨가하기 전에 20분 동안 실온에서 배양되게 하였다. 즉시 BDNF와 p75NTR(NBP)+/-담체의 첨가 후 검출 용액(Discoverx Corp CA) 12㎕를 각 웰에 첨가하고 플레이트를 파크아드 빅터(Parkard Victor) 2 플레이트 리더에서 해독하기에 앞서 실온에서 60분 동안 배양되게 하였다. p75NTR(NBP)의 첨가에 대한 반응에서 용량반응 곡선과 곡선에서의 변화(shift)를 관찰했다. 담체없이 p75NTR(NBP)에 사용된 담체에 관계없이, BDNF 용량반응 곡선에서 p75NTR(NBP)-Fc, p75NTR(NBP)-알부민 또는 p75NTR(NBP)-트랜스페린 억제와 변화를 관찰했다(도 5 참조).
실시예 4. BDNF와 결합하는 p75NTR(NBP)를 입증하는 바이오코어(boicore) 데이터 및 항-BDNF와 p75NTR(NBP) 사이의 경쟁.
p75-Fc(p75NTR(NBP)-Fc)(500㎍/ml)를 pH 5.0, 10mM 아세테이트에서 25㎍/ml의 농도로 희석하고 러닝 버퍼 HBS-P(0.005% P20)+1mg/ml BSA를 이용하는 바이오코어 칩에 고정시켰다. HBS-P(0.005% P20)+1mg/ml BSA 버퍼에서 BDNF의 스톡 용액(R 및 D 시스템으로부터) 2uM을 제조했다. BDNF 경쟁 실험을 p75와 MAB248(BDNF 항체 RandD systems)의 존재 또는 부재로 하여 하기 농도에서 수행하였다: i) MAB248(500nM) 단독, ii) BDNF(20nM)+MAB248(500nM), iii) BDNF(20NM) 단독 및 iv) BDNF(20nM)+MAB248(100nM). 모든 샘플을 스톡 용액으로부터 제조하여 러닝 버퍼에서 희석시켰다: HBS-P(0.005% P20)+1mg/ml BSA. 모든 샘플을 주입에 앞서 실온에서 30분 동안 두었다. 매뉴얼 센서그램을 50ul/min의 유속으로 바이오코어 칩에 걸쳐서 개시하였다. 각 샘플을 분리된 센서그램 사이클에서 상기 리스트된 순서대로 30초 동안 주입하였다. 12초(10ul) 사이클 동안 5mM NaOH로 필요한 곳에 재생을 수행하였다. 도 6에 묘사된 대로 p75NTR(NBP)가 BDNF와 결합한다.
실시예 5. PC 12 세포에서 p75NTR(NBP)의 NGF 활성의 저해
p75NTR(NBP)가 도 7에 나타낸 바와 같이, TrkA 및/또는 TrkA 뿐만 아니라 p75를 세포 표면에서 발현하는 PC-12와 N2OS 세포에서 NGF의 활성을 상당하게 저해하는 것으로 입증되었다.
낮은 계대 PC12 세포(계대수 20-24)를 5% 소태아혈청과 10% 열-비활성화한 말 혈청과 페니실린-스트렙토마이신(10U/ml-0.1mg/ml)으로 보충된 DMEM(Dulbecco's modified Eagle's medium) 배지에서 96-웰 플레이트 상에 직접 성장시키고, 37℃, 5% CO2를 함유하는 습한 분위기에서 배양하였다. NGF(50ng/ml)를 PC12 세포를 분화시키기 위해 성장 배지에 첨가했다. 200, 100, 50, 25, 12.5, 6.25, 3.1, 1.5, 0.78, 0.39, 0.2, 0.1 ng/ml의 p75NTR(NBP) 용량 농도를 플레이트를 가로질러 각 웰에 첨가했다. 플레이트를 37℃에서 24시간 동안 배양시키고 세포 수를 셀 카운터로 확인하였다. 도 8에 나타낸 것처럼 배지에 대한 p75NTR(NBP)의 첨가는 그들의 신경돌기 페노타입(axonal phenotype)으로 PC-12 세포가 분화하는 것을 상당하게 차단하였다. NGF의 존재하에 PC-12 세포가 분화하고 뉴런(neuronal) 유사 페노타입을 형성한다.
실시예 6. 뉴로트로픽 결합 단백질 p75NTR(NBP)는 신경 흥분 모델의 기계적 통각과민에서 BDNF 효과를 저해한다.
수컷 스프라그 돌리 래트(Male Sprague Dawley rats)를 이소플루란(유도를 위해 산소 내 5%, 유지를 위해 산소 내 1.5-2.0%)으로 마취시켰다. 척수를 척수의 L4-L6 영역이 열려 있도록 요추 후궁절제술(lumbar laminectomy)로 노출시키고, 격리된 넓은 동적 범위의 뉴런(isolated wide dynamic range neurone)으로부터 기록하기 위해 텅스텐 마이크로전극을 후근 내로 삽입하였다. 개별 WDR 뉴런을 기록된 단위의 스파이크 진폭이 최소한 기선(baseline) 노이즈 레벨의 3배가 되도록 격리시켰다. 뉴로로그 AC-커플드 앰플리파이어를 사용하여 반응을 증폭시켰고 CED 스파이크2 소프트웨어를 사용하여 기록하였다. 약물 적용에 앞서, 3 안정한 기선 반응(<10% 변형)을 자연 자극 범위(브러쉬, 본 프레이(von Frey), 핀치 및 열)에서 얻었다. 브러쉬 자극을 섬세한 면 조각으로 말초 수용 영역의 중앙을 스트로크하여 적용하였다. 본 프레이 필라멘트와 열(43도에서 고정 워터젯 세트를 사용하여)을 10초 동안 적용하였다. 핀치를 5초 동안 적용하였다. 일단 안정한 기선 반응이 얻어졌고, BDNF 단독(0.1% BSA에서 500ng) 또는 BDNF(500ng)+p75NTR(NBP)(주입에 앞서 40분 동안 전배양된 500ng)를 인슐린 시린지를 이용하여 25ul 부피로 수용 영역의 중앙에 적용하였다. 약물 효과가 150분 동안 이어졌으며 테스트를 10분 간격으로 수행하였다. 실험의 종점에서 래트를 자궁전위에 의해 희생시켰다.
도 8에서 입증되는 것처럼, BDNF는 신경 흥분에서 상당한 증가를 일으켰으며 이는 이어지는 자극을 증폭시켰다. p75NTR(NBP)의 첨가는 모든 자극에 대한 반응에서 신경 흥분을 상당히 감소시켰다; 식염수, BDNF, 브러쉬 및 핀치. p75NTR(NBP)가 신경성 흥분과 이어지는 통증을 감소시킨다는 것은 분명하다.
실시예 7. 뉴로트로픽 결합 단백질 p75NTR(NBP)는 UVIH 모델에서 통각과민을 저해한다.
동물을
UV
에 노출
찰스 리버 수컷 스프라그 듈리 래트(175-200g)을 2% 이소플루란 O2 혼합물로 마취시켰다. 오른쪽 뒷발의 발바닥 표면이 UV 300mJ/㎠으로 조사되는 동안 마취를 노즈콘(nose cone)을 통해 유지시켰다(Saalmann CupCube system, Saalmann GmbH, Germany; l=280-400 nm). 조사원을 래트의 뒷발의 발다닥 표면에 UV 소스(Pfizer Facilities Management and Engineering Team)에 부착된 형상화된 딜리버리 칼라(shaped delivery collar)(8X12mm)를 이용하여 적용하였다. UV 소스의 강도를 SEL005/WBS320/TD 필터(ABLE Instruments and Controls Ltd)로 ABLE 1400A 라이오미터를 이용하여 보정하였다. 사용된 UV 노출은 자연그대로의(naive) 래트에게 피부 홍반을 일으키고 다른 부작용은 없다(체중의 감소가 없으며, 스트레스나 명확한 불편함의 신호가 없음).
열적
통각과민의
평가
열적 통각과민을 래트의 발바닥 테스트(Ugo Basile, Italy)에 이어서 하그레이브 등(Hargreaves et al)의 수정된 방법(1988)을 이용하여 평가했다. 래트를 테스트 전에 기구에 길들여지게 했다(15-30분). 발바닥 테스트를 높은 유리 테이블 위 세 개의 개별 퍼스펙스 박스로 구성했다. 6 래트/기구를 동시에 시험할 수 있도록 두 마리의 래트를 각 박스에 두었다.
이동 적외선 열원을 직접 래트의 뒷발 발바닥 표면에 적용하였다. 발을 회피하는데 걸린 시간(paw withdrawal latency, PWL)을 래트가 열원으로부터 뒷발을 제거하는데 걸린 시간(초)으로 규정했다. 처리되지 않은 동물에 8-12초의 반응을 부여하기 위해 열원을 보정했다(105-120mW/㎠). 조직 손상을 방지하기 위해 20초의 자동 차단을 설정했다.
다섯 개의 기록을 기선 측정 동안 각각의 래트 뒷발로부터 얻었으며(UV 노출 전의 래트, 데이 0(Day 0)), 통각과민 발병을 확인하였다(데이 1(days 1)). 날마다 두 개의 세션을 데이 0과 데이 1에서 수행하였다.
2일, 3일 및 4일에서(개별적으로, UV 노출 후 48, 72 및 96시간) 약제의 효능 평가 동안 발마다 세 개의 기록을 기선과 각각의 테스트 지점에 대해 수집하였다. 부상을 입지 않은 발을 항상 먼저 평가했다.
열적 통각과민을 연구에서 선택되는 평균 PWL≤5초를 보여주는 동물로서 규정했다.
정적
이질통(Static Allodynia)의
평가
동물들을 이질통 평가에 앞서 와이어 보텀 테스트 케이지(wire bottom test cages)에 길들여지게 했다. 전체 업다운 측정이 수행되기 전에, 동물들을 습관화 첫째 날에 15g, 8g+4g 필라멘트를, 둘째 날에 4g 필라멘트를 적용하여 본 프레이 헤어에 익숙해지게 했다. 정적 이질통을 뒷발의 발바닥 표면에 대해 힘의 오름차순(0.6, 1, 1.4, 2, 4, 6, 8, 10, 15 및 26g)으로 본 프레이 헤어(Stoelting, Wood Dale, Illinois, U.S.A.)를 적용하여 평가했다. 각각의 본 프레이 헤어를 최대 6초 동안 발에 적용하거나, 또는 회피 반응(withdrawal response)이 일어날 때까지 적용했다. 본 프레이 헤어에 대해 일단 회피 반응이 확립되면, 발을 회피가 생성된 것보다 낮은 필라멘트로 시작하여, 이어서 회피가 생기지 않을 때까지 힘의 내림차순으로 필라메트를 유지하면서 재테스트했다. 26g의 최고 힘에 발이 들릴 뿐만 아니라 반응을 이끌어내고, 따라서 차단 지점을 나타내었다. 각 동물은 이 방식으로 양쪽 뒷발을 테스트했다. 반응을 이끌어내기 위해 요구되는 가장 적은 양의 힘을 그램으로 발 회피 역치(paw withdrawal threshold , PWT)로서 기록하였다. 만약 동물이 정상 래트에서 무해한 값인 4g 보다 낮은 자극에 반응하다면, 정적 이질통이 존재하는 것으로 규정하였다.
동물들을 테스트에 앞서 기초 검사를 하고 포함 기준에 부합하는 이질통을 나타내는 것들을 PWL에 근거하여 무작위로 추출하고 약물을 복용시킨다. 시험 화합물을 미리 정해진 시간(시험 화합물의 약물동력학적 특성에 의존하는)에 복용시키고, 이어서 정량 측정을 복용 후 선택된 시간에 하고 모든 데이터를 분석을 위해 수집했다. 도 9에서 입증되는 것처럼 피하로 주입된 100mg/kg의 p75NTR(NBP)에 대한 PWL 데이터(NBPP_Fc로 나타남)가 대조군, 피하로 주입된 이부프로펜 100mg/kg po 및 항-NGF 항체 10mg/kg과 비교하여 나타나 있으며, 각 경우에 열적 통각과민의 평가를 위한 데이터가 동등한 측정치를(equivalent measures) 나타내었다.
SEQUENCE LISTING
<110> LEVICEPT LTD
<120> THERAPEUTIC USE OF P75NTR NEUROTROPHIN BINDING PROTEIN
<130> LEVI01102WO.el
<150> 60/610,682
<151> 2012-03-14
<160> 19
<170> PatentIn version 3.5
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Thr Gly Gly Lys Asn Pro Asp Pro Trp Ala Lys Asn Leu Asn Glu Lys
565 570 575
Asp Tyr Glu Leu Leu Cys Leu Asp Gly Thr Arg Lys Pro Val Glu Glu
580 585 590
Tyr Ala Asn Cys His Leu Ala Arg Ala Pro Asn His Ala Val Val Thr
595 600 605
Arg Lys Asp Lys Glu Ala Cys Val His Lys Ile Leu Arg Gln Gln Gln
610 615 620
His Leu Phe Gly Ser Asn Val Thr Asp Cys Ser Gly Asn Phe Cys Leu
625 630 635 640
Phe Arg Ser Glu Thr Lys Asp Leu Leu Phe Arg Asp Asp Thr Val Cys
645 650 655
Leu Ala Lys Leu His Asp Arg Asn Thr Tyr Glu Lys Tyr Leu Gly Glu
660 665 670
Glu Tyr Val Lys Ala Val Gly Asn Leu Arg Lys Cys Ser Thr Ser Ser
675 680 685
Leu Leu Glu Ala Cys Thr Phe Arg Arg Pro
690 695
<210> 10
<211> 609
<212> PRT
<213> Homo sapiens
<400> 10
Met Lys Trp Val Thr Phe Ile Ser Leu Leu Phe Leu Phe Ser Ser Ala
1 5 10 15
Tyr Ser Arg Gly Val Phe Arg Arg Asp Ala His Lys Ser Glu Val Ala
20 25 30
His Arg Phe Lys Asp Leu Gly Glu Glu Asn Phe Lys Ala Leu Val Leu
35 40 45
Ile Ala Phe Ala Gln Tyr Leu Gln Gln Cys Pro Phe Glu Asp His Val
50 55 60
Lys Leu Val Asn Glu Val Thr Glu Phe Ala Lys Thr Cys Val Ala Asp
65 70 75 80
Glu Ser Ala Glu Asn Cys Asp Lys Ser Leu His Thr Leu Phe Gly Asp
85 90 95
Lys Leu Cys Thr Val Ala Thr Leu Arg Glu Thr Tyr Gly Glu Met Ala
100 105 110
Asp Cys Cys Ala Lys Gln Glu Pro Glu Arg Asn Glu Cys Phe Leu Gln
115 120 125
His Lys Asp Asp Asn Pro Asn Leu Pro Arg Leu Val Arg Pro Glu Val
130 135 140
Asp Val Met Cys Thr Ala Phe His Asp Asn Glu Glu Thr Phe Leu Lys
145 150 155 160
Lys Tyr Leu Tyr Glu Ile Ala Arg Arg His Pro Tyr Phe Tyr Ala Pro
165 170 175
Glu Leu Leu Phe Phe Ala Lys Arg Tyr Lys Ala Ala Phe Thr Glu Cys
180 185 190
Cys Gln Ala Ala Asp Lys Ala Ala Cys Leu Leu Pro Lys Leu Asp Glu
195 200 205
Leu Arg Asp Glu Gly Lys Ala Ser Ser Ala Lys Gln Arg Leu Lys Cys
210 215 220
Ala Ser Leu Gln Lys Phe Gly Glu Arg Ala Phe Lys Ala Trp Ala Val
225 230 235 240
Ala Arg Leu Ser Gln Arg Phe Pro Lys Ala Glu Phe Ala Glu Val Ser
245 250 255
Lys Leu Val Thr Asp Leu Thr Lys Val His Thr Glu Cys Cys His Gly
260 265 270
Asp Leu Leu Glu Cys Ala Asp Asp Arg Ala Asp Leu Ala Lys Tyr Ile
275 280 285
Cys Glu Asn Gln Asp Ser Ile Ser Ser Lys Leu Lys Glu Cys Cys Glu
290 295 300
Lys Pro Leu Leu Glu Lys Ser His Cys Ile Ala Glu Val Glu Asn Asp
305 310 315 320
Glu Met Pro Ala Asp Leu Pro Ser Leu Ala Ala Asp Phe Val Glu Ser
325 330 335
Lys Asp Val Cys Lys Asn Tyr Ala Glu Ala Lys Asp Val Phe Leu Gly
340 345 350
Met Phe Leu Tyr Glu Tyr Ala Arg Arg His Pro Asp Tyr Ser Val Val
355 360 365
Leu Leu Leu Arg Leu Ala Lys Thr Tyr Glu Thr Thr Leu Glu Lys Cys
370 375 380
Cys Ala Ala Ala Asp Pro His Glu Cys Tyr Ala Lys Val Phe Asp Glu
385 390 395 400
Phe Lys Pro Leu Val Glu Glu Pro Gln Asn Leu Ile Lys Gln Asn Cys
405 410 415
Glu Leu Phe Glu Gln Leu Gly Glu Tyr Lys Phe Gln Asn Ala Leu Leu
420 425 430
Val Arg Tyr Thr Lys Lys Val Pro Gln Val Ser Thr Pro Thr Leu Val
435 440 445
Glu Val Ser Arg Asn Leu Gly Lys Val Gly Ser Lys Cys Cys Lys His
450 455 460
Pro Glu Ala Lys Arg Met Pro Cys Ala Glu Asp Tyr Leu Ser Val Val
465 470 475 480
Leu Asn Gln Leu Cys Val Leu His Glu Lys Thr Pro Val Ser Asp Arg
485 490 495
Val Thr Lys Cys Cys Thr Glu Ser Leu Val Asn Arg Arg Pro Cys Phe
500 505 510
Ser Ala Leu Glu Val Asp Glu Thr Tyr Val Pro Lys Glu Phe Asn Ala
515 520 525
Glu Thr Phe Thr Phe His Ala Asp Ile Cys Thr Leu Ser Glu Lys Glu
530 535 540
Arg Gln Ile Lys Lys Gln Thr Ala Leu Val Glu Leu Val Lys His Lys
545 550 555 560
Pro Lys Ala Thr Lys Glu Gln Leu Lys Ala Val Met Asp Asp Phe Ala
565 570 575
Ala Phe Val Glu Lys Cys Cys Lys Ala Asp Asp Lys Glu Thr Cys Phe
580 585 590
Ala Glu Glu Gly Lys Lys Leu Val Ala Ala Ser Gln Ala Ala Leu Gly
595 600 605
Leu
<210> 11
<211> 212
<212> PRT
<213> Homo sapiens
<400> 11
Gly Gly Pro Ser Val Phe Leu Phe Pro Pro Lys Pro Lys Asp Thr Leu
1 5 10 15
Met Ile Ser Arg Thr Pro Glu Val Thr Cys Val Val Val Asp Val Ser
20 25 30
His Glu Asp Pro Glu Val Lys Phe Asn Trp Tyr Val Asp Gly Val Glu
35 40 45
Val His Asn Ala Lys Thr Lys Pro Arg Glu Glu Gln Tyr Asp Ser Thr
50 55 60
Tyr Arg Val Val Ser Val Leu Thr Val Leu His Gln Asp Trp Leu Asn
65 70 75 80
Gly Lys Glu Tyr Lys Cys Lys Val Ser Asn Lys Ala Leu Pro Ala Pro
85 90 95
Ile Glu Lys Thr Ile Ser Lys Ala Lys Gly Gln Pro Arg Glu Pro Gln
100 105 110
Val Tyr Thr Leu Pro Pro Ser Arg Glu Glu Met Thr Lys Asn Gln Val
115 120 125
Ser Leu Thr Cys Leu Val Lys Gly Phe Tyr Pro Ser Asp Ile Ala Val
130 135 140
Glu Trp Glu Ser Asn Gly Gln Pro Glu Asn Asn Tyr Lys Thr Thr Pro
145 150 155 160
Pro Val Leu Asp Ser Asp Gly Ser Phe Phe Leu Tyr Ser Lys Leu Thr
165 170 175
Val Asp Lys Ser Arg Trp Gln Gln Gly Asn Val Phe Ser Cys Ser Val
180 185 190
Met His Glu Ala Leu His Asn His Tyr Thr Gln Lys Ser Leu Ser Leu
195 200 205
Ser Pro Gly Lys
210
<210> 12
<211> 326
<212> PRT
<213> Homo sapiens
<400> 12
Ala Ser Thr Lys Gly Pro Ser Val Phe Pro Leu Ala Pro Cys Ser Arg
1 5 10 15
Ser Thr Ser Glu Ser Thr Ala Ala Leu Gly Cys Leu Val Lys Asp Tyr
20 25 30
Phe Pro Glu Pro Val Thr Val Ser Trp Asn Ser Gly Ala Leu Thr Ser
35 40 45
Gly Val His Thr Phe Pro Ala Val Leu Gln Ser Ser Gly Leu Tyr Ser
50 55 60
Leu Ser Ser Val Val Thr Val Thr Ser Ser Asn Phe Gly Thr Gln Thr
65 70 75 80
Tyr Thr Cys Asn Val Asp His Lys Pro Ser Asn Thr Lys Val Asp Lys
85 90 95
Thr Val Glu Arg Lys Cys Cys Val Glu Cys Pro Pro Cys Pro Ala Pro
100 105 110
Pro Val Ala Gly Pro Ser Val Phe Leu Phe Pro Pro Lys Pro Lys Asp
115 120 125
Thr Leu Met Ile Ser Arg Thr Pro Glu Val Thr Cys Val Val Val Asp
130 135 140
Val Ser His Glu Asp Pro Glu Val Gln Phe Asn Trp Tyr Val Asp Gly
145 150 155 160
Met Glu Val His Asn Ala Lys Thr Lys Pro Arg Glu Glu Gln Phe Asn
165 170 175
Ser Thr Phe Arg Val Val Ser Val Leu Thr Val Val His Gln Asp Trp
180 185 190
Leu Asn Gly Lys Glu Tyr Lys Cys Lys Val Ser Asn Lys Gly Leu Pro
195 200 205
Ala Pro Ile Glu Lys Thr Ile Ser Lys Thr Lys Gly Gln Pro Arg Glu
210 215 220
Pro Gln Val Tyr Thr Leu Pro Pro Ser Arg Glu Glu Met Thr Lys Asn
225 230 235 240
Gln Val Ser Leu Thr Cys Leu Val Lys Gly Phe Tyr Pro Ser Asp Ile
245 250 255
Ala Val Glu Trp Glu Ser Asn Gly Gln Pro Glu Asn Asn Tyr Lys Thr
260 265 270
Thr Pro Pro Met Leu Asp Ser Asp Gly Ser Phe Phe Leu Tyr Ser Lys
275 280 285
Leu Thr Val Asp Lys Ser Arg Trp Gln Gln Gly Asn Val Phe Ser Cys
290 295 300
Ser Val Met His Glu Ala Leu His Asn His Tyr Thr Gln Lys Ser Leu
305 310 315 320
Ser Leu Ser Pro Gly Lys
325
<210> 13
<211> 165
<212> PRT
<213> Homo sapiens
<400> 13
Cys Tyr Thr Leu Leu Leu Leu Thr Thr Pro Ser Trp Val Leu Ser Gln
1 5 10 15
Val Thr Leu Lys Glu Ser Gly Pro Val Leu Val Lys Pro Thr Glu Thr
20 25 30
Leu Thr Leu Thr Cys Thr Val Ser Gly Phe Ser Leu Ser Asn Ala Lys
35 40 45
Met Gly Val Ser Trp Ile Arg Gln Pro Pro Gly Lys Ala Leu Glu Trp
50 55 60
Leu Ala His Ile Phe Ser Asn Asp Glu Lys Ser Tyr Ser Thr Ser Leu
65 70 75 80
Lys Ser Arg Leu Thr Ile Ser Lys Asp Thr Ser Lys Ser Gln Val Val
85 90 95
Leu Thr Met Thr Asn Met Asp Pro Val Asp Thr Ala Thr Tyr Tyr Cys
100 105 110
Ala Arg Ile Phe Thr Ile Thr Tyr Ser Asn Tyr Val Leu Gln Tyr Tyr
115 120 125
Tyr Tyr Met Asp Val Trp Gly Lys Gly Thr Thr Val Thr Val Ser Ser
130 135 140
Ala Ser Thr Lys Gly Pro Ser Val Phe Pro Leu Ala Pro Cys Ser Arg
145 150 155 160
Ser Thr Ser Gly Gly
165
<210> 14
<211> 217
<212> PRT
<213> Homo sapiens
<400> 14
Ala Pro Glu Phe Leu Gly Gly Pro Ser Val Phe Leu Phe Pro Pro Lys
1 5 10 15
Pro Lys Asp Thr Leu Met Ile Ser Arg Thr Pro Glu Val Thr Cys Val
20 25 30
Val Val Asp Val Ser Gln Glu Asp Pro Glu Val Gln Phe Asn Trp Tyr
35 40 45
Val Asp Gly Val Glu Val His Asn Ala Lys Thr Lys Pro Arg Glu Glu
50 55 60
Gln Phe Asn Ser Thr Tyr Arg Val Val Ser Val Leu Thr Val Leu His
65 70 75 80
Gln Asp Trp Leu Asn Gly Lys Glu Tyr Lys Cys Lys Val Ser Asn Lys
85 90 95
Gly Leu Pro Ser Ser Ile Glu Lys Thr Ile Ser Lys Ala Lys Gly Gln
100 105 110
Pro Arg Glu Pro Gln Val Tyr Thr Leu Pro Pro Ser Gln Glu Glu Met
115 120 125
Thr Lys Asn Gln Val Ser Leu Thr Cys Leu Val Lys Gly Phe Tyr Pro
130 135 140
Ser Asp Ile Ala Val Glu Trp Glu Ser Asn Gly Gln Pro Glu Asn Asn
145 150 155 160
Tyr Lys Thr Thr Pro Pro Val Leu Asp Ser Asp Gly Ser Phe Phe Leu
165 170 175
Tyr Ser Lys Leu Thr Val Asp Lys Ser Arg Trp Gln Glu Gly Asn Val
180 185 190
Phe Ser Cys Ser Val Met His Glu Ala Leu His Asn His Tyr Thr Gln
195 200 205
Lys Ser Leu Ser Leu Ser Leu Gly Lys
210 215
<210> 15
<211> 209
<212> PRT
<213> Homo sapiens
<400> 15
Gly Gly Pro Ser Val Phe Leu Phe Pro Pro Lys Pro Lys Asp Thr Leu
1 5 10 15
Tyr Ile Thr Arg Glu Pro Glu Val Thr Cys Val Val Val Asp Val Ser
20 25 30
His Glu Asp Pro Glu Val Lys Phe Asn Trp Tyr Val Asp Gly Val Glu
35 40 45
Val His Asn Ala Lys Thr Lys Pro Arg Glu Glu Gln Tyr Asn Ser Thr
50 55 60
Tyr Arg Val Val Ser Val Leu Thr Val Leu His Gln Asp Trp Leu Asn
65 70 75 80
Gly Lys Glu Tyr Lys Cys Lys Val Ser Asn Lys Ala Leu Pro Ala Pro
85 90 95
Ile Glu Lys Thr Ile Ser Lys Ala Lys Gly Gln Pro Arg Glu Pro Gln
100 105 110
Val Tyr Thr Leu Pro Pro Ser Arg Asp Glu Leu Thr Lys Asn Gln Val
115 120 125
Ser Leu Thr Cys Leu Val Lys Gly Phe Tyr Pro Ser Asp Ile Ala Val
130 135 140
Glu Trp Glu Ser Asn Gly Gln Pro Glu Asn Asn Tyr Lys Thr Thr Pro
145 150 155 160
Pro Val Leu Asp Ser Asp Gly Ser Phe Phe Leu Tyr Ser Lys Leu Thr
165 170 175
Val Asp Lys Ser Arg Trp Gln Gln Gly Asn Val Phe Ser Cys Ser Val
180 185 190
Met His Glu Ala Leu His Asn His Tyr Thr Gln Lys Ser Leu Ser Leu
195 200 205
Ser
<210> 16
<211> 225
<212> PRT
<213> Homo sapiens
<400> 16
Thr His Thr Cys Pro Pro Cys Pro Ala Pro Glu Phe Glu Gly Gly Pro
1 5 10 15
Ser Val Phe Leu Phe Pro Pro Lys Pro Lys Asp Thr Leu Met Ile Ser
20 25 30
Arg Thr Pro Glu Val Thr Cys Val Val Val Asp Val Ser His Glu Asp
35 40 45
Pro Glu Val Lys Phe Asn Trp Tyr Val Asp Gly Val Glu Val His Asn
50 55 60
Ala Lys Thr Lys Pro Arg Glu Glu Gln Tyr Asn Ser Thr Tyr Arg Val
65 70 75 80
Val Ser Val Leu Thr Val Leu His Gln Asp Trp Leu Asn Gly Lys Glu
85 90 95
Tyr Lys Cys Lys Val Ser Asn Lys Ala Leu Pro Ala Ser Ile Glu Lys
100 105 110
Thr Ile Ser Lys Ala Lys Gly Gln Pro Arg Glu Pro Gln Val Tyr Thr
115 120 125
Leu Pro Pro Ser Arg Glu Glu Met Thr Lys Asn Gln Val Ser Leu Thr
130 135 140
Cys Leu Val Lys Gly Phe Tyr Pro Ser Asp Ile Ala Val Glu Trp Glu
145 150 155 160
Ser Asn Gly Gln Pro Glu Asn Asn Tyr Lys Thr Thr Pro Pro Val Leu
165 170 175
Asp Ser Asp Gly Ser Phe Phe Leu Tyr Ser Lys Leu Thr Val Asp Lys
180 185 190
Ser Arg Trp Gln Gln Gly Asn Val Phe Ser Cys Ser Val Met His Glu
195 200 205
Ala Leu His Asn His Tyr Thr Gln Lys Ser Leu Ser Leu Ser Pro Gly
210 215 220
Lys
225
<210> 17
<211> 5
<212> PRT
<213> Artificial
<220>
<223> Linker sequence
<220>
<221> MISC_FEATURE
<222> (1)..(5)
<223> (GGGGS)n (n = 3 to 4)
<400> 17
Gly Gly Gly Gly Ser
1 5
<210> 18
<211> 5
<212> PRT
<213> Artificial
<220>
<223> Linker sequence
<220>
<221> MISC_FEATURE
<222> (1)..(5)
<223> (EAAAK)n (n = 2 to 5)
<400> 18
Glu Ala Ala Ala Lys
1 5
<210> 19
<211> 5
<212> PRT
<213> Artificial
<220>
<223> Linker sequence
<400> 19
Gly Gly Gly Gly Ser
1 5
Claims (23)
- p75NTR 뉴로트로핀 결합 단백질(p75NTR(NBP))을 포함하는 통증을 치료하기 위한 조성물로서,
상기 p75NTR(NBP)는 20℃에서 표면 플라즈몬 공명으로 측정된 0.1nM에서 50nM 사이의 결합 친화도(Kd)로 NGF, BDNF, NT3 또는 NT4/5 중의 어느 것에 결합하고,
상기 p75NTR(NBP)는 SEQ ID No.2의 아미노산 서열을 포함하는,
p75NTR 뉴로트로핀 결합 단백질(p75NTR(NBP))을 포함하는 통증을 치료하기 위한 조성물.
- 제1항에 있어서,
상기 p75NTR(NBP)는
(a) 트랜스페린 또는 그것의 부분,
(b) 알부민 또는 그것의 부분,
(c) 면역글로불린 Fc 또는 그것의 부분,
(d) 폴리에틸렌 글리콜 폴리머 체인
으로부터 선택되는 하나 이상의 보조 분자에 연결된 p75NTR(NBP)를 포함하는, p75NTR 뉴로트로핀 결합 단백질(p75NTR(NBP))을 포함하는 통증을 치료하기 위한 조성물.
- 제2항에 있어서,
상기 p75NTR(NBP)는 하나 이상의 링커를 통해서 상기 하나 이상의 보조 분자에 연결되는, p75NTR 뉴로트로핀 결합 단백질(p75NTR(NBP))을 포함하는 통증을 치료하기 위한 조성물.
- 제1항 내지 제3항 중 어느 하나의 항에 있어서,
상기 p75NTR(NBP)는 인간 p75NTR(NBP)인, p75NTR 뉴로트로핀 결합 단백질(p75NTR(NBP))을 포함하는 통증을 치료하기 위한 조성물.
- 제1항 내지 제3항 중 어느 하나의 항에 있어서,
상기 p75NTR(NBP)는 하나 이상의 뉴로트로핀 결합 도메인 1[SEQ ID NO. 4], 2[SEQ ID NO. 5], 3[SEQ ID NO. 6], 4[SEQ ID NO. 7] 또는 5[SEQ ID NO. 8]를 포함하는, p75NTR 뉴로트로핀 결합 단백질(p75NTR(NBP))을 포함하는 통증을 치료하기 위한 조성물.
- 제1항 내지 제3항 중 어느 하나의 항에 있어서,
상기 p75NTR(NBP)는
(a) SEQ ID NO. 4, SEQ ID NO. 5, SEQ ID NO. 6, SEQ ID NO. 7 또는 SEQ ID NO. 8 중 하나 이상,
(b) SEQ ID NO. 3 또는 (a)를 포함하는 그것의 부분, 또는
(c) SEQ ID NO. 2 또는 (a)를 포함하는 그것의 부분
을 포함하는, p75NTR 뉴로트로핀 결합 단백질(p75NTR(NBP))을 포함하는 통증을 치료하기 위한 조성물.
- 제3항에 있어서,
상기 링커는
(a) 공유결합,
(b) 비공유결합,
(c) 펩티드 결합
(d) 하나의 아미노산 또는 펩티드를 포함하는 복수의 아미노산
으로부터 선택되는, p75NTR 뉴로트로핀 결합 단백질(p75NTR(NBP))을 포함하는 통증을 치료하기 위한 조성물.
- 제1항 내지 제3항 중 어느 하나의 항에 있어서,
상기 p75NTR(NBP)는 하나 이상의 보조 분자에 연결되어 있으며, 선택적으로 각각의 보조 분자는 동일하거나 상이하거나 또는 동일 및 상이한 것의 혼합물인, p75NTR 뉴로트로핀 결합 단백질(p75NTR(NBP))을 포함하는 통증을 치료하기 위한 조성물.
- 제8항에 있어서,
상기 하나 이상의 보조 분자는 링커를 통해서 p75NTR(NBP)에 연결되는 보조 분자의 다합체를 포함하며, 각각의 분자는 동일 또는 상이 또는 동일 및 상이한 것의 혼합물인, p75NTR 뉴로트로핀 결합 단백질(p75NTR(NBP))을 포함하는 통증을 치료하기 위한 조성물.
- p75NTR 뉴로트로핀 결합 단백질(p75NTR(NBP))을 포함하는 통증을 치료하기 위한 조성물로서,
상기 p75NTR(NBP)는 20℃에서 표면 플라즈몬 공명으로 측정된 0.1nM에서 50nM 사이의 결합 친화도(Kd)로 NGF, BDNF, NT3 또는 NT4/5 중의 어느 것에 결합하고,
상기 p75NTR(NBP)는
(a) 서열 SEQ ID No. 3의 p75NTR(NBP), 및 선택적으로
(b) 면역글로불린 Fc로 구성되는, p75NTR 뉴로트로핀 결합 단백질(p75NTR(NBP))을 포함하는 통증을 치료하기 위한 조성물.
- 제10항에 있어서,
상기 p75NTR(NBP)는
(a) 트랜스페린 또는 그것의 부분,
(b) 알부민 또는 그것의 부분,
(c) 면역글로불린 Fc 또는 그것의 부분,
(d) 폴리에틸렌 글리콜 폴리머 체인
으로부터 선택되는 하나 이상의 보조 분자에 연결된 p75NTR(NBP)를 포함하는, p75NTR 뉴로트로핀 결합 단백질(p75NTR(NBP))을 포함하는 통증을 치료하기 위한 조성물.
- 제11항에 있어서,
상기 p75NTR(NBP)는 하나 이상의 링커를 통해서 상기 하나 이상의 보조 분자에 연결되는, p75NTR 뉴로트로핀 결합 단백질(p75NTR(NBP))을 포함하는 통증을 치료하기 위한 조성물.
- 제10항 내지 제12항 중 어느 하나의 항에 있어서,
상기 면역글로불린 Fc는 SEQ ID No. 12, 15 및 16으로부터 선택되는, p75NTR 뉴로트로핀 결합 단백질(p75NTR(NBP))을 포함하는 통증을 치료하기 위한 조성물.
- 제10항 내지 제12항 중 어느 하나의 항에 있어서,
상기 조성물은 링커를 더 포함하는, p75NTR 뉴로트로핀 결합 단백질(p75NTR(NBP))을 포함하는 통증을 치료하기 위한 조성물.
- 제13항에 있어서,
상기 조성물은 링커를 더 포함하는, p75NTR 뉴로트로핀 결합 단백질(p75NTR(NBP))을 포함하는 통증을 치료하기 위한 조성물.
- 제14항에 있어서,
상기 링커는 SEQ ID No. 17, 18 및 19로부터 선택되는, p75NTR 뉴로트로핀 결합 단백질(p75NTR(NBP))을 포함하는 통증을 치료하기 위한 조성물.
- 제15항에 있어서,
상기 링커는 SEQ ID No. 17, 18 및 19로부터 선택되는, p75NTR 뉴로트로핀 결합 단백질(p75NTR(NBP))을 포함하는 통증을 치료하기 위한 조성물.
- p75NTR 뉴로트로핀 결합 단백질(p75NTR(NBP))을 포함하는 통증 치료에 사용하기 위한 조성물로서,
상기 p75NTR(NBP)는 통증의 치료에 사용하기 위한 하나 이상의 뉴로트로핀 결합 도메인 1[SEQ ID NO. 4], 2[SEQ ID NO. 5], 3[SEQ ID NO. 6], 4[SEQ ID NO. 7] 또는 5[SEQ ID NO. 8]를 포함하고,
상기 p75NTR(NBP)는 SEQ ID No.2의 아미노산 서열을 포함하는,
p75NTR 뉴로트로핀 결합 단백질(p75NTR(NBP))을 포함하는 통증 치료에 사용하기 위한 조성물.
- 제18항에 있어서,
상기 p75NTR(NBP)는
(a) SEQ ID NO. 4, SEQ ID NO. 5, SEQ ID NO. 6, SEQ ID NO. 7 또는 SEQ ID NO. 8 중 하나 이상,
(b) SEQ ID NO. 3 또는 (a)를 포함하는 그것의 부분, 또는
(c) SEQ ID NO. 2 또는 (a)를 포함하는 그것의 부분
을 포함하는, p75NTR 뉴로트로핀 결합 단백질(p75NTR(NBP))을 포함하는 통증 치료에 사용하기 위한 조성물.
- 제1항 또는 제18항에 있어서,
상기 통증은 하기로부터 선택되는 것인, p75NTR 뉴로트로핀 결합 단백질(p75NTR(NBP))을 포함하는 통증을 치료하기 위한 조성물:
(a) 급성 통증 및/또는 자발통,
(b) 만성 통증 및/또는 진행성 통증,
(c) 관절염 통증, 골관절염 또는 류마티스성 관절염으로부터 오는 통증, 염증성 장 질환으로부터 오는 통증, 건선 및 습진의 어느 것을 포함하는 염증성 통증,
(d) 침해성 통증,
(e) 고통스러운 당뇨병성 신경병증 또는 포진 후 신경통과 관련되는 통증을 포함하는 신경병성 통증,
(f) 통각 과민,
(g) 이질통,
(h) 중추성 통증, 뇌졸중 후 중추성 통증, 다발성 경화증으로부터 오는 통증, 척수 손상으로부터 오는 통증, 파킨슨병 또는 뇌전증으로부터 오는 통증,
(i) 암성 통증,
(j) 수술 후 통증,
(k) 소화기 내장성 통증 및 비소화기 내장성 통증을 포함하는 내장통, 위장관(GI)병에 기인하는 통증, 기능성 장질환(FBD)으로부터 오는 통증, 염증성 장질환(IBD)으로부터 오는 통증, 월경통, 골반통, 방광염, 간질성 방광염 또는 췌장염으로부터 오는 통증,
(l) 근골격계 통증, 근육통, 섬유근육통, 척추염, 혈청 음성(비류머티즘성) 관절통증, 비-관절성 류머티즘, 근이영양증, 글리코겐 분해, 다발성 근육염, 화농성 근염,
(m) 심장 또는 혈관 통증, 협심증에 의한 통증, 심근경색, 승모판막 협착증, 심낭염, 레이노 증후군, 공피증, 공피증 또는 골격근 허혈,
(n) 편두통, 조짐편두통, 무조짐편두통, 군발두통, 긴장성 두통을 포함하는 두통,
(o) 치통, 턱관절 근막통증 또는 이명을 포함하는 구강안면 통증, 또는
(p) 요통, 윤활낭염, 월경통, 편두통, 연관통, 삼차 신경병증, 하이퍼센티세이션, 척수 외상 및/또는 변성 또는 뇌졸중으로부터 오는 통증.
- 제1항 또는 제18항에 있어서,
상기 p75NTR(NBP)는 제2의 약물학적으로 활성인 화합물과 결합되는 조합에서 개별, 연속 또는 동시 사용을 위한 것이고, 상기 조합의 제2의 약물학적으로 활성인 화합물은 하기로부터 선택되는 것인 p75NTR 뉴로트로핀 결합 단백질(p75NTR(NBP))을 포함하는 통증을 치료하기 위한 조성물:
- 모르핀, 헤로인, 하이드로모르폰, 옥시모르폰, 레보파놀, 레발로판, 메타돈, 메페리딘, 펜타닐, 코카인, 코데인, 디하이드로코데인, 옥시코돈, 하이드로코돈, 프로폭시펜, 날메펜, 날로핀, 날록손, 날트렉손, 부프레노르핀, 부토르파놀, 날부핀 또는 펜타조신과 같은 오피오이드 진통제;
- 아스피린, 디클로페낙, 디플루시날, 에토돌락, 펜부펜, 페노프로렌, 플루페니살, 플루비프로펜, 이부프로펜, 인도메타신, 케토프로펜, 케토롤락, 메클로페남산, 메페남산, 멜록시캄, 나부메톤, 나프록센, 니메술리드, 니트로플루비프로펜, 올살라진, 옥사프로진, 페닐부타존, 피록시캄, 설파알라진, 술린닥, 톨메틴 또는 조메피락과 같은 비스테로이드성 항염증성 약물(NSAID);
- 아모바비탈, 아프로바비탈, 부타바비탈, 부타비탈, 메포바비탈, 메타르비탈, 메쏘헥시탈, 펜토바비탈, 페노바비탈, 세코바비탈, 탈부탈, 티아미랄(theamylal) 또는 티오펜탈과 같은 수면 진정제(barbiturate sedative);
- 클로르디아제폭시드, 클로라제페이트, 디아제팜, 플루라제팜, 로라제팜, 옥사제팜, 테마제팜 또는 트리아졸람과 같은 진정 작용이 있는 벤조디아제핀;
- 디펜히드라민, 피릴라민, 프로메타진, 클로르페니라민 또는 클로르사이클리진과 같은 진정 작용이 있는 H1 길항제;
- 글루테티이미드, 메프로바메이트, 메타쿠알론 또는 디클로랄페나존과 같은 진정제;
- 바클로펜, 카리소프로돌, 클로르족사존, 시클로벤자프린, 메토카바몰 또는 오르프레나딘과 같은 골격근이완제;
- 덱스트로메트로판(dextromethorphan)((+)-3-하이드록시-N-메틸모르피난((+)-3-hydroxy-N-methylmorphinan)) 또는 그것의 대사산물 덱스트로판(dextrorphan)((+)3-하이드록시-N-메틸모르피난), 케타민, 메만틴, 피롤로퀴놀린 퀴닌, 시스-4-(포스포노메틸)-2-피페리딘카복시산, 부디핀, EN-3231(MorphiDex®, 모르핀과 덱스트로메트로판의 조합 제제), 토피라메이트, 네라멕산 또는 이펜프로딜, 트락소프로딜 또는 (-)-(R)-6-{2-[4-(3-플루오로페닐)-4-하이드록시-1-피페리디닐]-1-하이드록시에틸-3,4-디하이드로-2(1H)-퀴놀리논과 같은 NR2B 길항제를 포함하는 페르진포텔과 같은 NMDA 수용체 길항제;
- 독사조신, 탐술로신, 클로니딘, 구안파신, 덱스메타토미딘, 모다피닐, 또는 4-아미노-6,7-디메톡시-2-(5-메탄-술폰아미도-1,2,3,4-테트라하이드로이소퀴놀-2-일)-5-(2-피리딜) 퀴나졸린)과 같은 알파-수용체;
- 데시프라민, 이미프라민, 아미트립틸린 또는 노르트립틸린과 같은 삼환계 항우울제;
- 카바마제핀, 라모트리진, 토피라트메이트 또는 발프로에이트와 같은 경련 예방제;
- (αR,9R)-7-[3,5-비스(트리플루오로메틸)벤질]-8,9,10,11-테트라하이드로-9-메틸-5-(4-메틸페닐)-7H-[1,4]디아조시노[2,1-g][1,7]-나프티리딘-6-13-디온(TAK-637), 5-[[(2R,3S)-2-[(1R)-1-[3,5-비스(트리플루오로메틸)페닐]에톡시-3-(4-플루오로페닐)-4-모르폴리닐]-메틸]-1,2-디하이드로-3H-1,2,4-트리아졸-3-온(MK-869), 아프레피탄트, 라네피탄트, 다피탄트 또는 3-[[2-메톡시-5-(트리플루오로메톡시)페닐]-메틸아미노]-2-페닐피페리딘(2S,3S)과 같은 타치키닌(NK) NK-3, NK-2 또는 NK-1 길항제;
- 옥시부티닌, 톨테로딘, 프로피베린, 염화트로스피움, 다리페나신, 솔리페나신, 테미베린 및 이프라트로피움과 같은 무스카린 길항제;
- 셀레콕시브, 로페콕시브, 파레콕시브, 발데콕시브, 데라콕시브, 에토리콕시브 또는 루미라콕시브와 같은 COX-2 선택적 저해제;
- 파라세타몰과 같은 콜-타르 수용체(coal-tar analgesic);
- 드로페리돌, 클로르프로마진, 할로페리돌, 페르페나진, 티오리다진, 메소리다진, 트리플루오페라진, 플루페나진, 클로자핀, 올란자핀, 리스페리돈, 지프라시돈, 퀘티아핀, 세르틴돌, 아리피프라졸, 소네피프라졸, 블로난세린, 일로페리돈, 페로스피론, 라클로프라이드, 조테핀, 비페프루녹스, 아세나핀, 루라시돈, 아미술프라이드, 발라페리돈, 팔린도르(palindore), 에플리반세린, 오사네탄트, 리모나반트, 메클리네르탄트(meclinertant), 미락시온(Miraxion®) 또는 사리조탄과 같은 신경이완제;
- 레신페라톡신과 같은 바닐로이드 수용체 작용제 또는 캅사제핀과 같은 길항제;
- 프로파놀롤과 같은 베타-수용체;
- 멕실레틴과 같은 국소마취제;
- 덱사메타손과 같은 코르티코스테로이드;
- 5-HT 수용체 작용제 또는 길항제
- R(+)-알파-(2,3-디메톡시-페닐)-1-[2-(4-플루오로페닐에틸)-4-피페리딘메탄올(MDL-100907)과 같은 5-HT2A 수용체 길항제;
- 이스프로닉클린(TC-1734), (E)-N-메틸-4-(3-피리디닐)-3-부텐-1-아민(RJR-2403), (R)-5-(2-아제티디닐메톡시)-2-클로로피리딘(ABT-594) 또는 니코틴과 같은 콜린성(니코틴성) 수용체;
- 트라마돌(Tramadol®);
- 5-[2-에톡시-5-(4-메틸-1-피페라지닐-설포닐)페닐]-1-메틸-3-n-프로필-1,6-디하이드로-7H-피라졸로[4,3-d]피리미딘-7-온(실데나필), (6R,12aR)-2,3,6,7,12,12a-헥사하이드로-2-메틸-6-(3,4-메틸렌디옥시페닐)-파라지노[2',1':6,1]-피리도[3,4-b]인돌-1,4-디온(IC-351 또는 타다라필), 2-[2-에톡시-5-(4-에틸-피페라진-1-일-1-설포닐)-페닐]-5-메틸-7-프로필-3H-이미다조[5,1-f][1,2,4]트라아진-4-온(바르데나필), 5-(5-아세틸-2-부톡시-3-피리디닐)-3-에틸-2-(1-에틸-3-아제티디닐)-2,6-디하이드로-7H-피라졸로[4,3-d]피리미딘-7-온, 5-(5-아세틸-2-프로폭시-3-피리디닐)-3-에틸-2-(1-이소프로필-3-아제티디닐)-2,6-디하이드로-7H-피라졸로[4,3-d]피리미딘-7-온, 5-[2-에톡시-5-(4-에틸피페라진-1-일설포닐)피리딘-3-일]-3-에틸-2-[2-메톡시에틸]-2,6-디하이드로-7H-피라졸로[4,3-d]피리미딘-7-온, 4-[(3-클로로-4-메톡시벤질)아미노]-2[(2S)-2-(하이드록시메틸)피롤리돈-1-일]-N-(피리미딘-2-일메틸)피리미딘-5-카르복스아미드, 3-(1-메틸-7-옥소-3-프로필-6,7-디하이드로-1H-피라졸로[4,3-d]피리미딘-5-일)-N-[2-(1-메틸피롤리딘-2-일)에틸]-4-포폭시벤젠설폰아미드와 같은 PDEV 저해제;
- 카나비노이드;
- 대사형 글루탐산 서브타입 1 수용체(mGluR1) 길항제;
- 세르트랄린, 세르트랄린 대사산물 데메틸세르트랄린, 플루옥세틴, 노르플루옥세틴(플로옥세틴 데스메틸 대사산물), 플루복사민, 파록세틴, 시탈로프람, 시탈로프람 대사산물 데스메틸시탈로프람, 에스시탈로프람, d,l-펜플루라민, 페목세틴, 이폭세틴, 시아노도티에핀, 리톡세틴, 다폭세틴, 네파조돈, 세리클라민 및 트라조돈과 같은 세로토닌 재흡수 저해제;
- 마프로틸린, 로페프라민, 미르타제핀, 옥사프로틸린, 페졸라민, 토목세틴, 미안세린, 부프로프리온, 부프로프리온 대사산물 하이드록시부프로프리온, 노미펜신 및 빌록사진(Vivalan®)과 같은 노르아드레날린(노르에피네프린) 재흡수 저해제, 레복세틴, (S,S)-레복세틴과 같은 선택적 노르아드레날린 재흡수 저해제;
- 벤라팍신, 벤라팍신 대사산물 O-데스메틸벤라팍신, 클로미프라민, 클로미프라민 대사산물 데스메틸클로미프라민, 듈록세틴, 밀낙프란 및 이미프라민과 같은 이중 세로토닌-노르아드레날린 재흡수 저해제;
- S-[2-[(1-이미노에틸)아미노]에틸]-L-호모시스테인, S-[2-[(1-이미노에틸)-아미노]에틸]-4,4-디옥소-L-시스테인, S-[2-[(1-이미노에틸)아미노]에틸]-2-메틸-L-시스테인, (2S,5Z)-2-아미노-2-메틸-7-[(1-이미노에틸)아미노]-5-헵탄산, 2-[[(1S,3S)-3-아미노-하이드록시-1-(5-티아졸릴)부틸]티오]-5-클로로-3-피리딘카보니트릴, 2-[[(1S,3S)-3-아미노-하이드록시-1-(5-티아졸릴)부틸]티오]-4-클로로벤조니트릴, (2S,4R)-2-아미노-4-[[2-클로로-5-(트리플루오로메틸)페닐]티오]-5-티아졸부탄올, 2-[[(1R,3S)-3-아미노-4-하이드록시-1-(5-티아졸릴) 부틸]티오]-6-(트리플루오로메틸)-3-피리딘카보니트릴, 2-[[(1R,3S)-3-아미노-4-하이드록시-1-(5-티아졸릴) 부틸]티오]-5-클로로벤조니트릴, N-[4-[2-(3-클로로벤질아미노)에틸]페닐]티오펜-2-카르복스아미딘, 또는 구아니디노에틸디설파이드와 같은 유도성 산화질소 합성효소(inducible nitric oxide synthase (iNOS)) 저해제;
- 도네페질과 같은 아세틸콜린에스테라아제;
- N-[({2-[4-(2-에틸-4,6-디메틸-1H-이미다조[4,5-c]피리딘-1-일)페닐]에틸}아미노)-카보닐]-4-메틸벤젠설폰아미드 또는 4-[(1S)-1-({[5-클로로-2-(3-플루오로페녹시)피리딘-3-일]카보닐}아미노)에틸]벤조산과 같은 프로스타글란딘 E2 서브타입 4(EP4) 길항제;
- 1-(3-비페닐-4-일메틸-4-하이드록시-크로만-7-일)-시클로펜탄카복시산(CP-105696), 5-[2-(2-카복시에틸)-3-[6-(4-메톡시페닐)-5E-헥세닐]옥시페녹시]-발레산(ONO-4057) 또는 DPC-11870과 같은 류코트리엔 B4 길항제;
- 질류톤, 6-[(3-플루오로-5-[4-메톡시-3,4,5,6-테트라하이드로-2H-vlfks-4-일])페녹시-메틸]-1-메틸-2-퀴놀론(ZD-2138), 또는 2,3,5-트리메틸-6-(3-피리딜메틸)-1,4-벤조퀴논(CV-6504)와 같은 5-리폭시게나아제 저해제;
- 리도카인과 같은 소듐 채널 차단제; 또는
- 온단세트론과 같은 5-HT3 길항제;
및 약학적으로 수용가능한 염 및 그들의 용매화물.
- 제1항 또는 제18항에 따른 p75NTR(NBP), 및 약학적으로 수용가능한 담체 및/또는 첨가제를 포함하는 통증의 예방, 완화, 제어, 발생 감소, 또는 전개 또는 진전의 지연 중 하나 이상에의 사용을 위한 약학적 조성물.
- 삭제
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