KR20200091961A - 체액 내에서 질병 또는 병태의 시그너쳐의 검출 방법 - Google Patents
체액 내에서 질병 또는 병태의 시그너쳐의 검출 방법 Download PDFInfo
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Abstract
Description
도 1은 살아있는 CTC, 세포자멸성 CTC, 단편화된 (fragmented) CTC, 생육가능 및/또는 세포자멸성 종양 세포에 의해 방출된 종양 DNA, RNA, 단백질, 및 지질의 탐식 후에 포식세포에 의한 종양-특이적 DNA, RNA, 단백질 및/또는 지질 시그너쳐의 획득을 야기하는 제시된 경로를 개략적으로 도시한 것이다. 포식세포만 (비-포식세포가 아니라) 종양 시그너쳐를 획득함에 주목한다.
도 2는 난소암 (OC) 환자의 포식세포에서/포식세포에 의해 발현된 암 시그너쳐의 확인에 사용되는 분석 방법을 개략적으로 도시한 것이다.
도 3은 본 발명의 방법의 한 실시태양의 일반적인 흐름도를 개략적으로 도시한 것이다.
도 4는 살아있는 CTC, 세포자멸성 CTC, 단편화된 CTC, 생육가능 및/또는 세포자멸성 종양 세포에 의해 방출된 종양 DNA, RNA, 단백질 및 지질의 탐식 후에 혈액 포식세포에 의한 종양-특이적 DNA, RNA, 단백질 및 지질 시그너쳐의 획득을 야기하는 제시된 경로를 개략적으로 도시한 것이다. 포식작용 후의 포식세포의 DNA 함량은 >2n임을 주목한다.
도 5는 유방암 (BC)-보유 동물에서 유방암 (BC) 시그너쳐의 확인에 사용되는 분석 방법을 개략적으로 도시한 것이다.
도 6은 본 발명의 방법의 다른 실시태양의 일반적인 흐름도를 개략적으로 도시한 것이다.
도 7은 LNCaP 및 LLC1 세포로부터 단리된 총 RNA의 겔 전기영동 분석을 도시한 것이다.
도 8은 마우스 백혈구 (WBC)로부터 얻은 RNA의 수율 및 질을 나열한 것이다.
도 9A-9D는 LNCaP (인간 전립선암) 종양 보유 누드 마우스로부터의 호중구에서 검출된 7개의 상향조절된 (2배 이상) 암 관련 유전자를 보여주는 어레이를 도시한 것이다. (A) LNCaP 종양. (B) LNCaP 종양 보유 누드 마우스로부터 얻은 호중구 (NT). (C) LNCaP 종양 보유 누드 마우스로부터 얻은 T 세포 (TT). (D) 비-종양 보유 누드 마우스로부터 얻은 호중구 (NN). 원으로 표시된 시그너쳐는 종양 세포 (A)에서 및 종양 보유 마우스로부터의 호중구 (B)에서 발현되고, 비-종양 보유 마우스로부터의 호중구 (D)에서 및 비-포식성 T 세포 (C)에서 최소로 발현된 것이다. NT에서의 발현은 NN 및 TT에서보다 2배 이상 더 컸다.
도 10A-10D은 LNCaP (인간 전립선암) 종양 보유 누드 마우스로부터의 대식세포에서 검출된 3개의 상향조절된 암 관련 유전자를 보여주는 어레이를 도시한 것이다. (A) LNCaP 종양. (B) LNCaP 종양 보유 누드 마우스로부터 얻은 대식세포 (MT). (C) LNCaP 종양 보유 누드 마우스로부터 얻은 T 세포 (TT). (D) 비-종양 보유 누드 마우스로부터 얻은 대식세포 (MN). 원으로 표시된 시그너쳐는 종양 세포 (A)에서 및 종양 보유 마우스로부터의 대식세포 (B)에서 발현되고, 비-종양 보유 마우스로부터의 대식세포 (D)에서 및 비-포식성 T 세포 (C)에서 최소로 발현된 것이다. MT에서의 발현은 MN 및 TT에서보다 2배 이상 더 컸다.
도 11A-11D는 LS174T (인간 결장암) 종양 보유 누드 마우스로부터의 호중구에서 검출된 4개의 상향조절된 (2배 이상) 암 관련 유전자를 보여주는 어레이를 도시한 것이다. (A) LS174T 종양. (B) LS174T 종양 보유 누드 마우스로부터 얻은 호중구 (NT). (C) LS174T 종양 보유 누드 마우스로부터 얻은 T 세포 (TT). (D) 비-종양 보유 누드 마우스로부터 얻은 호중구 (NN). 원으로 표시된 시그너쳐는 종양 세포 (A)에서 및 종양 보유 마우스로부터의 호중구 (B)에서 발현되고, 비-종양 보유 마우스로부터의 호중구 (D)에서 및 비-포식성 T 세포 (C)에서 최소로 발현된 것이다. NT에서의 발현은 NN 및 TT에서보다 2배 이상 더 컸다.
도 12A-12D는 LS174T (인간 결장암) 종양 보유 누드 마우스로부터의 대식세포에서 검출된 3개의 상향조절된 (2배 이상) 암 관련 유전자를 보여주는 어레이를 도시한 것이다. (A) LS174T 종양. (B) LS174T 종양 보유 누드 마우스로부터 얻은 대식세포 (MT). (C) LS174T 종양 보유 누드 마우스로부터 얻은 T 세포 (TT). (D) 비-종양 보유 누드 마우스로부터 얻은 대식세포 (MN). 원으로 표시된 시그너쳐는 종양 세포 (A)에서 및 종양 보유 마우스로부터의 대식세포 (B)에서 발현되고, 비-종양 보유 마우스로부터의 대식세포 (D)에서 및 비-포식성 T 세포 (C)에서 최소로 발현된 것이다. MT에서의 발현은 MN 및 TT에서보다 2배 이상 더 컸다.
도 13A-13D는 LLC1 (마우스 전이성 폐암) 종양-보유 C57/B1 마우스로부터의 호중구에서 검출된 5개의 상향조절된 (2배 이상) 암 관련 유전자를 보여주는 어레이를 도시한 것이다. (A) LLC1 종양. (B) LLC1 종양 보유 C57/B1 마우스로부터 얻은 호중구 (NT). (C) LLC1 종양 보유 C57/B1 마우스로부터 얻은 T 세포 (TT). (D) 비-종양 보유 C57/B1 마우스로부터 얻은 호중구 (NN). 원으로 표시된 시그너쳐는 종양 세포 (A)에서 및 종양 보유 마우스로부터의 호중구 (B)에서 발현되고, 비-종양 보유 마우스로부터의 호중구 (D)에서 및 비-포식성 T 세포 (C)에서 최소로 발현된 것이다. NT에서의 발현은 NN 및 TT에서보다 2배 이상 더 컸다.
도 14A-14D는 LLC1 (마우스 전이성 폐암) 종양-보유 C57/B1 마우스로부터의 대식세포에서 검출된 2개의 상향조절된 (2배 이상) 암 관련 유전자를 보여주는 어레이를 도시한 것이다. (A) LLC1 종양. (B) LLC1 종양 보유 C57/B1 마우스로부터 얻은 대식세포 (MT). (C) LLC1 종양 보유 C57/B1 마우스로부터 얻은 T 세포 (TT). (D) 비-종양 보유 C57/B1 마우스로부터 얻은 대식세포 (MN). 원으로 표시된 시그너쳐는 종양 세포 (A)에서 및 종양 보유 마우스로부터의 호중구 (B)에서 발현되고, 비-종양 보유 마우스로부터의 호중구 (D)에서 및 비-포식성 T 세포 (C)에서 최소로 발현된 것이다. MT에서의 발현은 MN 및 TT에서보다 2배 이상 더 컸다.
도 15A-15D는 B16F10 (마우스 전이성 흑색종) 종양 보유 C57/B1 마우스로부터의 호중구에서 검출된 2개의 상향조절된 (2배 이상) 암 관련 유전자를 보여주는 어레이를 도시한 것이다. (A) B16F10 종양. (B) B16F10 종양 보유 C57/B1 마우스로부터 얻은 호중구 (NT). (C) B16F10 종양 보유 C57/B1 마우스로부터 얻은 T 세포 (TT). (D) 비-종양 보유 C57/B1 마우스로부터 얻은 호중구 (NN). 원으로 표시된 시그너쳐는 종양 세포 (A)에서 및 종양 보유 마우스로부터의 호중구 (B)에서 발현되고, 비-종양 보유 마우스로부터의 호중구 (D)에서 및 비-포식성 T 세포 (C)에서 최소로 발현된 것이다. NT에서의 발현은 NN 및 TT에서보다 2배 이상 더 컸다.
도 16A-16D는 B16F10 (마우스 전이성 흑색종) 종양-보유 C57/B1 마우스로부터의 대식세포에서 검출된 1개의 상향조절된 (2배 이상) 암 관련 유전자를 보여주는 어레이를 도시한 것이다. (A) B16F10 종양. (B) B16F10 종양 보유 C57/B1 마우스로부터 얻은 대식세포 (MT). (C) B16F10 종양 보유 C57/B1 마우스로부터 얻은 T 세포 (TT). (D) 비-종양 보유 C57/B1 마우스로부터 얻은 대식세포 (MN). 원으로 표시된 시그너쳐는 종양 세포 (A)에서 및 종양 보유 마우스로부터의 대식세포 (B)에서 발현되고, 비-종양 보유 마우스로부터의 대식세포 (D)에서 및 비-포식성 T 세포 (C)에서 최소로 발현된 것이다. MT에서의 발현은 MN 및 TT에서보다 2배 이상 더 컸다.
도 17A-17D는 두경부암 (편평세포 암종)의 환자로부터의 호중구에서 검출된 5개의 상향조절된 (2배 이상) 암 관련 유전자를 보여주는 어레이를 도시한 것이다. (A) 정상 조직 (피부) 생검. (B) 종양 조직 생검. (C) 환자 혈액으로부터 얻은 호중구 (NT), (D) 환자 혈액으로부터 얻은 T 세포 (TT). 원으로 표시된 시그너쳐는 종양 세포 (B)에서 및 환자 혈액으로부터의 호중구 (C)에서 발현되고, 정상 피부 (A)에서 또는 비-포식성 T 세포 (D)에서 최소로 발현되거나 발현되지 않은 것이다. NT에서의 발현은 TT 및 피부에서보다 2배 이상 더 컸다.
도 18A-18D는 난소암 (선암종)의 환자로부터의 대식세포에서 검출된 23개의 상향조절된 (2배 이상) 암 관련 유전자를 보여주는 어레이를 도시한 것이다. (A) 환자 혈액으로부터 얻은 대식세포 (MT). (B) 환자 혈액으로부터 얻은 T 세포 (TT). 원으로 표시된 시그너쳐는 환자로부터 얻은 대식세포 (A)에서 발현되고, 비-포식성 T 세포 (B)에서 최소로 발현된 것이다. MT에서의 발현은 TT에서보다 2배 이상 더 컸다.
도 19는 포식세포 내의 종양 시그너쳐를 확인하기 위해 사용되는 방법을 도시한 것이다. 본 예에서, 종양 보유 동물로부터의 대식세포 (MT)에서의 암 연관 유전자의 발현 강도를 동일한 동물로부터의 T 세포 (TT)에서의 강도와 비교하여 정량하였고, 2배 초과로 과다발현된 유전자가 확인되었다. 이어서, MT에서 발현된 모든 유전자의 강도를 비-종양 보유 동물로부터 얻은 대식세포 (MNT)에서의 강도와 비교하여 정량하였고, 2배 초과로 과다발현된 유전자가 확인되었다. 두 목록에 공통적인 유전자를 선택하여, 동일한 종양에 의해 발현된 것과 비교하였다 (음영 영역).
도 20A-20B는 (A) LNCaP 인간 전립선 종양 보유 누드 마우스로부터 얻은 대식세포 (MLNCaP) 및 동일한 동물로부터의 T 세포 (T 세포LNCaP), (B) MLNCaP 및 비-종양 보유 마우스로부터 얻은 대식세포 (M비-종양), (C) LNCaP 인간 전립선 종양 보유 누드 마우스로부터 얻은 호중구 (NLNCaP) 및 동일한 동물로부터의 T 세포 (T 세포LNCaP), 및 (D) NLNCaP 및 비-종양 보유 마우스로부터 얻은 대식세포 (N비-종양)에서 유전자 발현 강도 비교를 도시한 것이다. 적색의 유전자는 2배 초과로 과다발현되었고; 녹색의 유전자는 2배 초과로 과소발현되었다.
도 21은 포식성 호중구 (N) 및 대식세포 (M) 내에서 암 관련 유전자의 발현을 나열한 것이다.
도 22는 비-포식성 T 세포에 비해 난소암 환자의 포식성 대식세포에서 상향조절된 (2배 초과) 암 관련 유전자를 나열한 것이다.
도 23은 마우스 WBC로부터 얻은 단백질 샘플 (5.9 ㎍)의 SDS 겔 (10%) 전기영동을 도시한 것이다.
도 24는 종양 보유 마우스로부터 얻은 T 세포 및 단핵구/대식세포 (M/M)에서 TAG-72 및 PSA 발현에 대한 웨스턴 블롯 (Western blot) 분석을 도시한 것으로, 포식세포 내에만 시그너쳐가 존재함을 입증한다.
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| WO2012012693A2 (en) | 2010-07-23 | 2012-01-26 | President And Fellows Of Harvard College | Methods for detecting signatures of disease or conditions in bodily fluids |
| EP2596349B1 (en) | 2010-07-23 | 2017-12-13 | President and Fellows of Harvard College | Methods of detecting cardiovascular diseases or conditions |
| AU2011280997A1 (en) | 2010-07-23 | 2013-02-28 | President And Fellows Of Harvard College | Methods of detecting autoimmune or immune-related diseases or conditions |
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