KR930702372A - 유전자 발현 억제용 화합물 및 방법 - Google Patents

유전자 발현 억제용 화합물 및 방법

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KR930702372A
KR930702372A KR1019930700317A KR930700317A KR930702372A KR 930702372 A KR930702372 A KR 930702372A KR 1019930700317 A KR1019930700317 A KR 1019930700317A KR 930700317 A KR930700317 A KR 930700317A KR 930702372 A KR930702372 A KR 930702372A
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hydrogen
alkyl
oxygen
integer
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알렉산더 루드빅 웨이스
프레데릭 헤르만 하우셔
프라사드 벤카타 칼라 카투르베둘라
다니엘 죠셉 델레키
폴프랜시스 쥬니어 카바나프
패트리시아 수잔 모스콰
프레드 테리 오아키스
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파울 이. 듀폰
스터얼링 윈드롭 아이엔씨
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    • C07HSUGARS; DERIVATIVES THEREOF; NUCLEOSIDES; NUCLEOTIDES; NUCLEIC ACIDS
    • C07H21/00Compounds containing two or more mononucleotide units having separate phosphate or polyphosphate groups linked by saccharide radicals of nucleoside groups, e.g. nucleic acids

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Abstract

본원은 유전자 발현 억제용 화합물, 조성물 및 방법에 관한 것으로, 본원 화합물은 1) 3원자 인터누클레오지드 연쇄를 지니는 올리고누클레오지드 배열(약6개에서 약200개의 염기들로 이루어지는) 또는 2)양말단중 어느 한 말단(또는 양말단 모두)에 디올을 지니는 올리고누클레오타이드 배열(약9개에서 약200개의 염기들로 이루어지는)을 포함한다.

Description

유전자 발현 억제용 화합물 및 방법
본 내용은 요부공개 건이므로 전문내용을 수록하지 않았음
제1a도는 누클레오지드 알데하이드(화합물Ⅰ)제조용 합성경로를 보여준다. 제1b도는 포스포니움 아이어다이드(iodide)누클레오지드(화합물Ⅱ)제조용 합성 경로를 보여준다. 제2도는 알데하이드 누클레오지드(제1a도)와 포스포니움 아이어다이드 누클레오지드를 이용하는 누클레오지드 다이머(3탄소 인터누클레오지드 연쇄로 연결된 제조용 합성 경로를 보여준다. 제3도는 키미딘 알데하이드(화합물Ⅰ)와 포스포니움 아이어다이드 티미딘 (화합물Ⅱ)를 이용하는 티미린 다이머 제조용 합성 경로를 보여준다.

Claims (54)

  1. 하기식의 3원자 인터누클레오지드 연쇄를 지니는 올리고누클레오지드 배열 (약6개에서 약200개의 염기들로 이루어진)포함 화합물;
  2. -D-D-D-
  3. 식중 각각의 D는 독립하여CHR, 산소 또는 NR6를 R은 독립하여 수소, OH,SH 또는 NH2를, R6는 하나의 D가 산소 또는 NR6일 것을 조건으로 수소 또는 C1-C2알킬을 나타낸다.
  4. 제1항에 있어서, 양말단중 어느 한 말단(또는 양말단 모두)에 디올을 지니는 화합물.
  5. 제1항에 있어서, 디올이 테트라에에틸렌글리콜 또는 헥사에틸렌글리콜인 화합물.
  6. 하기식의 올리고누클레오지드 배열을 포함하는 화합물:
  7. 식중 W는 -D-D-D-를, 각각의 D는 독립하여 CHR, 산소 또는 NR6를 R은 독립하여 수소, OH,SH 또는 NH2를, R6는 하나의 D가 산소 또는 NR6일 것을 조건으로 수소 또는 C1-C2알킬을 : 각각의 W1은 독립하여 W또는를; 각각의 R1은 독립하여 OH, SH, NR2R3를 R2와 R3는 독립하여 수소 또는 C1-C6알킬 또는 NHR4를, R4는 C1-C12아실을 : 각각의 y는 독립하여 수소 또는 OH를 : 각각의 B는 독립하여 아데닌,시토신. 구아닌, 티민, 우라실 또는 이들의 수정체를 : j는 1에서 약 200까지의 정수를; k는 0또는 1에서 약 197까지의 정수를; 그리고 q는 j+k+q의 합이 약4에서 약200일 것을 조건으로, 0또는 1에서 약 197까지의 정수를 나타낸다.
  8. 하기식의 올리고누클레오지드 배열(약6개에서 약 200개의 염기들로 이루어지는)을 포함하는 화합물.
  9. 식중, 각각의 Z는 독립하여 R1또는를; 는 -D-D-D-를, 각각의 D는 독립하여 CHR, 산소 또는 NR6를 R은 독립하여 수소, OH,SH 또는 NH2를, R6는 하나의 D가 산소 또는 NR6일 것을 조건으로 수소 또는 C1-C2알킬을 : 각각의 W1은 독립하여 W 또는를; 각각의 R1은 독립하여 OH, SH, NR2R3를 R2와 R3는 독립하여 수소 또는 C1-C6알킬 또는 NHR4를, R4는 C1-C12아실을 : 각각의 R5는 독립하여 수소 또는 C1-C12알킬을 : 각각의 y는 독립하여 수소 또는 OH를; 각각의 B는 독립하여 아데닌, 시토신, 구아닌, 티민, 우라실 또는 이들의 수정체를 : e와 f 각각은 독립하여 최소한 e와 f 중 하나가 최소한 1일 것을 조건으로 0에서 50을 : j는 1에서 약 200까지의 정수를; k는 0또는 1에서 약 197까지의 정수를; 그리고 m과 n 각각은 독립하여 1에서 200을 : 그리고 각각의 p는 j+k+q의 합이 약4에서 약200일 것을 조건으로, 0또는 1에서 약 197까지의 정수를 나타낸다.
  10. 양말단중 어느 한 말단(또는 양말단 모두)에 디올을 지니는 올리고누클레오 타이드 배열 (약9개에서 약 200개의 염기들로 이루어지는)을 포함하는 누클리아제 저항성 화합물.
  11. 제6항에 있어서, 디올이 헥사에킬렌글리콜 또는 테트라에틸렌글리콜인 화합물,
  12. 하기식의 올리고노클레오타이드를 포함하는 화합물.
  13. 식중, R은 OH,SH,NR2R3를 또는 R2와 R3는 독립하여 수소 또는 C1-C6알킬 또는 NHR4를, R4는 C1-C12아실을 ; R1은 수소 또는 C1-C12알킬을 : 올리고(N)은 약9개에서 약 200개의 염기들로 이루어진 본래의 천연 또는 수정된 올리고누클레오타이드 배열을 : e와 f 각각은 독립하여 e와 f 중 최소한 하나가 1일 것을 조건으로 0에서 50을 : m과 n 각각은 독립하여 1에서 200을 : 그리고 각각의 p는 독립하여 2에서 4를 나타낸다.
  14. 하기식의 올리고누클레오타이드를 포함하는 화합물.
  15. 식중, R은 OH,SH,NR2R3를 R2와 R3는 독립하여 수소 또는 C1-C6알킬 또는 NHR4를, R4는 C1-C12아실을 :올리고(N)은 약9개에서 약 50개의 염기들로 이루어진 올리고누클레오타이드 배열을 : e와 f 각각은 독립하여 e와 f 중 최소한 하나가 최소한 1일 것을 조건으로 0에서 50을 : m과 n 각각은 독립하여 m과 n중 최소한 하나가 1에서 200일 것을 조건으로 0에서 200을 나타낸다.
  16. 하기식의 3원자 인터누클레오지드 연쇄를 지닌 올리고누클레오지드 배열(약6개에서 약200개의 염기들로 이루어진)제조를 포함하는 화합물들의 누클리아제 분해억제 방법.
  17. -D-D-D-
  18. 식중, 각각의 D는 독립하여 CHR, 산소 또는 NR6를 R은 독립하여 수소, OH,SH 또는 NH2를, R4는 하나의 D가 산소 또는 NR6일 것을 조건으로 수소 또는 C1-C2알킬을 나타낸다.
  19. 제10항에 있어서, 올리고누클레오지드 배열이 하기식을 지니는 방법.
  20. 식중 W는 -D-D-D-를, 각각의 D는 독립하여 CHR, 산소 또는 NR6를 R은 독립하여 수소, OH,SH 또는 NH2를, R6는 하나의 D가 산소 또는 NR6일 것을 조건으로 수소 또는 C1-C2알킬을 : 각각의 W1은 독립하여 W 또는를; 각각의 R1은 독립하여 OH, SH, NR2R3를 R2와 R3는 독립하여 수소 또는 C1-C6알킬 또는 NHR4를, R4는 C1-C12아실을 : 각각의 y는 독립하여 수소 또는 OH를 : 각각의 B는 독립하여 아데닌, 시토신, 구아닌, 티민, 우라실 또는 이들의 수정체를 : J는 1에서 약 200까지의 정수를; k는 0또는 1에서 약 197까지의 정수를; 그리고 q는 j+k+q의 합이 약4에서 약200일 것을 조건으로, 0또는 1에서 약 197까지의 정수를 나타낸다.
  21. 상기 누클레오타이드 또는 올리고누클레오지드 배열의 양말단중 어느 한 말단(또는 양말단 모두)에 대한 디올 부착을 포함하는누클레오타이드 또는 올리고누클레오지드를 안정화시키는 방법.
  22. 제12항에 있어서, 트리틸디올시아노포스핀이 상기 화합물의 5'말단 보호용으로 사용되는 방법.
  23. 하기식의 3원자 인터누클레오지드 연쇄(포스페이트를 함유하지 아니하는)를 지니는 올리고누클레오지드 배열(약6개에서 약200개의 염기들로 이루어지는)포함 화합물과 생리학적으로 용인되는 담체를 포함하는유전자 발현 억제용으로 유용한 조성물.
  24. -D-D-D-
  25. 식중, 각각의 D는 독립하여 CHR, 산소 또는 NR6를 R은 독립하여 수소, OH,SH 또는 NH2를, R4는 하나의 D가 산소 또는 NR6일 것을 조건으로 수소 또는 C1-C2알킬을 나타낸다.
  26. 제14항에 있어서, 올리고누클레오지드 배열이 하기식을 지니는 방법.
  27. 식중 W는 -D-D-D-를, 각각의 D는 독립하여 CHR, 산소 또는 NR6를 R은 독립하여 수소, OH,SH 또는 NH2를, R6는 하나의 D가 산소 또는 NR6일 것을 조건으로 수소 또는 C1-C2알킬을 : 각각의 W1은 독립하여 W 또는를; 각각의 R1은 독립하여 OH, SH, NR2R3를 R2와 R3는 독립하여 수소 또는 C1-C6알킬 또는 NHR4를, R4는 C1-C12아실을 : 각각의 y는 독립하여 수소 또는 OH를 : 각각의 B는 독립하여 아데닌, 시토신, 구아닌, 티민, 우라실 또는 이들의 수정체를 : J는 1에서 약 200까지의 정수를; k는 0또는 1에서 약 197까지의 정수를; 그리고 q는 j+k+q의 합이 약4에서 약200일 것을 조건으로, 0또는 1에서 약 197까지의 정수를 나타낸다.
  28. 양말단중 어느 한 말단(또는 양말단 모두)에 디올을 지니는 올리고누클레오타이드 배열(약9개에서 약 200개의 염기들로 이루어지는)포함하는 누클리아제 저항성 화합물과 생리학적으로 용인되는 담체를 포함하는 유전자 발현 억제용으로 유용한 조성물.
  29. 제16항에 있어서, 디올이 헥사에틸렌글리콜 또는 테트라에틸렌글리콜인 조성물.
  30. 제16항에 있어서, 화합물이 하기식의 올리고누클레오타이드를포함하는 화합물.
  31. 식중, R은 OH,SH,NR2R3를 R2와 R3는 독립하여 수소 또는 C1-C6알킬 또는 NHR4를, R4는 C1-C12아실을 : R1은 수소 또는 C1-C12알킬을 : 올리고(N)은 약9개에서 약 200개의 염기들로 이루어진 본래의 천연 또는 수정된 올리고누클레오타이드 배열을 : e와 f 각각은 독립하여 e와 f 중 최소한 하나가 최소한 1일 것을 조건으로 0에서 50을 : m과 n 각각은 독립하여 1에서 200을; 그리고 각각의 p는 독립하여 2에서 4를 나타낸다.
  32. 치료시 필요로되는 유효량의 올리고누클레오지드 배열(하기식의 3원자 인터누클레오지드 연쇄를 지니고, 약6개에서 약200개의 염기들로 이루어진)포함 화합물을 포유동물에 투여하는 것을 포함하는 포유류내 유전자 발현 억제방법.
  33. 식중, 각각의 D는 독립하여 CHR, 산소 또는 NR6를, R은 독립하여 수소, OH,SH 또는 NH2를, R4는 하나의 D가 산소 또는 NR6일 것을 조건으로 수소 또는 C1-C2알킬을 나타낸다.
  34. 제19항에 있어서, 올리고누클레오지드 배열이 하기식을 지니는 방법.
  35. 식중, W는 -D-D-D-를, 각각의 D는 독립하여 CHR, 산소 또는 NR6를 R은 독립하여 수소, OH,SH 또는 NH2를, R6는 하나의 D가 산소 또는 NR6일 것을 조건으로 수소 또는 C1-C2알킬을 : 각각의 W1은 독립하여 W 또는를; 각각의 R1은 독립하여 OH, SH, NR2R3를 R2와 R3는 독립하여 수소 또는 C1-C6알킬 또는 NHR4를, R4는 C1-C12아실을 : 각각의 y는 독립하여 수소 또는 OH를 : 각각의 B는 독립하여 아데닌, 시토신, 구아닌, 티민, 우라실 또는 이들의 수정체를 : J는 1에서 약 200까지의 정수를; k는 0또는 1에서 약 197까지의 정수를; 그리고 q는 j+k+q의 합이 약4에서 약200일 것을 조건으로, 0또는 1에서 약 197까지의 정수를 나타낸다.
  36. 제20항에 있어서, 화합물이 양말단중 어느 한 말단(또는 양말단 모두)에 디올을 지니는 방법.
  37. 제19항에 있어서, 화합물이 하기식의 올리고누클레오타이를 포함하는 방법.
  38. 식중, R은 OH,SH,NR2R3를, R2와 R3는 독립하여 수소 또는 C1-C6알킬 또는 NHR4를, R4는 C1-C12아실을 ; R1은 수소 또는 C1-C12알킬을 ; 올리고(N)은 약9개에서 약 200개의 염기들로 이루어진 본래의 천연 또는 수정된 올리고누클레오타이드 배열을 ; e와 f 각각은 독립하여 e와 f 중 최소한 하나가 최소한 1일 것을 조건으로 0에서 50을 ; m과 n 각각은 독립하여 1에서 200을; 그리고 각각의 p는 독립하여 2에서 4를 나타낸다.
  39. 하기식의 누클레오지드 다이머(dimer)를 포함하는 방법.
  40. 식중, W는 -D-D-D-를, 각각의 D는 독립하여 CHR, 산소 또는 NR6를 R은 독립하여 수소, OH,SH 또는 NH2를, R6는 하나의 D가 산소 또는 NR6일 것을 조건으로 수소 또는 C1-C2알킬을 : 각각의 B는 독립하여 아데닌, 시토신, 구아닌, 티민, 우라실 또는 이들의 수정체들을; R7은 OH, t-부틸디메틸실리옥시 또는 포스포아미다이트를 ; 그리고 R8은 OH, 어떤 보호그룹 또는 t-부틸디메틸실옥시를 나타낸다.
  41. 하기식 화합물
  42. 5'Xn CCT CGA CCA CCG CAT Xn(A)3'
  43. 식중, X 는 테트라에틸렌글리콜; 그리고 n은 1또는 2.
  44. ※ 참고사항 : 최초출원 내용에 의하여 공개하는 것임.
KR1019930700317A 1990-08-03 1991-08-02 유전자 발현 억제용 화합물 및 방법 KR100211552B1 (ko)

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US07/562,180 US5245022A (en) 1990-08-03 1990-08-03 Exonuclease resistant terminally substituted oligonucleotides
US562,180 1990-08-03
US262,180 1990-08-03
US58245690A 1990-09-13 1990-09-13
US58245790A 1990-09-13 1990-09-13
US58228790A 1990-09-13 1990-09-13
US582,287 1990-09-13
US582,457 1990-09-13
US582,456 1990-09-13
US68278491A 1991-04-09 1991-04-09
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US5677439A (en) 1997-10-14
TW222641B (ko) 1994-04-21
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AU8521791A (en) 1992-03-02
ES2083593T3 (es) 1996-04-16
DE69115702T2 (de) 1996-06-13
IL99066A0 (en) 1992-07-15
FI930455A0 (fi) 1993-02-02
IL113519A0 (en) 1995-07-31
NZ239247A (en) 1993-11-25
EP0541722A1 (en) 1993-05-19
IL99066A (en) 1996-01-31
GR3018881T3 (en) 1996-05-31
AU692532B2 (en) 1998-06-11
IL121421A0 (en) 1998-01-04
AU2008195A (en) 1995-10-12
WO1992002534A3 (en) 1992-06-11
PT98562B (pt) 1999-01-29
JPH06502300A (ja) 1994-03-17
IL113519A (en) 1997-11-20
PT98562A (pt) 1992-06-30
HUT67834A (en) 1995-05-29
MY107332A (en) 1995-11-30
ATE131827T1 (de) 1996-01-15
HU211668A9 (en) 1995-12-28
KR100211552B1 (ko) 1999-08-02
AU667459B2 (en) 1996-03-28
HU9300282D0 (en) 1993-04-28
WO1992002534A2 (en) 1992-02-20
EP0541722B1 (en) 1995-12-20
CA2088673A1 (en) 1992-02-04
DE69115702D1 (de) 1996-02-01
HU217036B (hu) 1999-11-29
BR9106729A (pt) 1993-07-20

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