KR102282378B1 - 전립선 특이적 막 항원(psma)의 표지된 억제제, 조영제로서의 이의 용도 및 전립선암 치료용 약제 - Google Patents
전립선 특이적 막 항원(psma)의 표지된 억제제, 조영제로서의 이의 용도 및 전립선암 치료용 약제 Download PDFInfo
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Abstract
Description
LNCaP 종양 이종 이식편을 갖는 무흉선 수컷 누드 마우스의 전신 관상 마이크로PET 영상. [68Ga]MB17의 종양-표적화 효능 및 약동학적 특성을 역동적 마이크로PET 스캔에 의해 평가하였다. 마우스당 대략 15 MBq를 주사하였다. 그래프 A는 신장 및 방광의 각각의 시간-활성-곡선을 나타내며, 그래프 B는 심장, 근육 및 종양의 각각의 시간-활성-곡선을 나타낸다. 값을 평균 SUV(표준 섭취 값(standardized uptake value))으로 표현한다.
도 2: 주사 후 1시간에서의 기관 분포
0.06 nmol의 68Ga 표지된 PSMA 억제제 MB17의 주사 후 1시간에서의 기관 분포. 체중 1 kg당 2 mg의 2-PMPA의 동시 투여에 의한 PSMA-차단은 종양 및 신장에서의 PSMA-특이적 섭취를 나타낸다. 데이터를 조직 1 g당 평균 % ID ㅁ SD (n=3마리)로서 표현한다.
도 3: MB4의 PET - 영상
LNCaP 종양 이종 이식편을 갖는 무흉선 수컷 누드 마우스의 전신 관상 마이크로PET 영상. [68Ga]MB4의 종양-표적화 효능 및 약동학적 특성을 역동적 마이크로PET 스캔에 의해 평가하였다. 마우스당 대략 15 MBq를 주사하였다. 그래프 A는 신장 및 방광의 각각의 시간-활성-곡선을 나타내며, 그래프 B는 심장, 근육 및 종양의 각각의 시간-활성-곡선을 나타낸다. 값을 평균 SUV(표준 섭취 값)으로 표현한다.
도 4: 0.06 nmol의 177 Lu-표지된 MB17을 주사한지 24시간 후 조직 1 g당 % ID ㅁ SD (n=5마리)로서 표현한 기관 분포
177Lu에 의한 기관 분포는, 높은 초기 신장 섭취율이 24시간 후에 거의 완전히 없어지는 한편 (2.13 ± 1.36 % ID/g) 종양 섭취율은 여전히 높은 채로 있고 심지어 증가하였음 (10.58 ± 4.50 % ID/g)을 보여준다. 간 (0.08 ± 0.03 % ID/g), 폐 (0.11 ± 0.13 % ID/g) 및 비장 (0.13 ± 0.05 % ID/g)과 같은 다른 기관은 매우 낮은 섭취율을 보여주었다. 유리한 약동학적 특성은 24시간 후 극도로 높은 종양 대 배경 비 (종양/혈액: 1058; 종양/근육: 529)로 이어졌다.
도 5: MB 2의 PET - 영상
LNCaP 종양 이종 이식편을 갖는 무흉선 수컷 누드 마우스의 전신 관상 마이크로PET 영상. [68Ga]MB2의 종양-표적화 효능 및 약동학적 특성을 역동적 마이크로PET 스캔에 의해 평가하였다. 마우스당 대략 15 MBq를 주사하였다.
도 6: MB 3의 PET - 영상
LNCaP 종양 이종 이식편을 갖는 무흉선 수컷 누드 마우스의 전신 관상 마이크로PET 영상. [68Ga]MB 3의 종양-표적화 효능 및 약동학적 특성을 역동적 마이크로PET 스캔에 의해 평가하였다. 마우스당 대략 15 MBq를 주사하였다.
도 7: MB10의 PET - 영상
LNCaP 종양 이종 이식편을 갖는 무흉선 수컷 누드 마우스의 전신 관상 마이크로PET 영상. [68Ga]MB10의 종양-표적화 효능 및 약동학적 특성을 역동적 마이크로PET 스캔에 의해 평가하였다. 마우스당 대략 15 MBq를 주사하였다.
도 8: MB17.D의 PET - 영상
LNCaP 종양 이종 이식편을 갖는 무흉선 수컷 누드 마우스의 전신 관상 마이크로PET 영상. [68Ga]MB17.D의 종양-표적화 효능 및 약동학적 특성을 역동적 마이크로PET 스캔에 의해 평가하였다. 마우스당 대략 15 MBq를 주사하였다.
MB17D: MB17(L)의 입체이성질체; Fmoc-3(2-나프틸)-D-알라닌을 기반으로 하여 합성
도 9: MB22의 PET - 영상
LNCaP 종양 이종 이식편을 갖는 무흉선 수컷 누드 마우스의 전신 관상 마이크로PET 영상. [68Ga]MB22의 종양-표적화 효능 및 약동학적 특성을 역동적 마이크로PET 스캔에 의해 평가하였다. 마우스당 대략 15 MBq를 주사하였다.
도 10: MB 24의 PET - 영상
LNCaP 종양 이종 이식편을 갖는 무흉선 수컷 누드 마우스의 전신 관상 마이크로PET 영상. [68Ga]MB 24의 종양-표적화 효능 및 약동학적 특성을 역동적 마이크로PET 스캔에 의해 평가하였다. 마우스당 대략 15 MBq를 주사하였다.
도 11: MB25의 PET - 영상
LNCaP 종양 이종 이식편을 갖는 무흉선 수컷 누드 마우스의 전신 관상 마이크로PET 영상. [68Ga]MB25의 종양-표적화 효능 및 약동학적 특성을 역동적 마이크로PET 스캔에 의해 평가하였다. 마우스당 대략 15 MBq를 주사하였다.
도 12: MB31의 PET - 영상
LNCaP 종양 이종 이식편을 갖는 무흉선 수컷 누드 마우스의 전신 관상 마이크로PET 영상. [68Ga]MB31의 종양-표적화 효능 및 약동학적 특성을 역동적 마이크로PET 스캔에 의해 평가하였다. 마우스당 대략 15 MBq를 주사하였다.
도 13: MB33의 PET - 영상
LNCaP 종양 이종 이식편을 갖는 무흉선 수컷 누드 마우스의 전신 관상 마이크로PET 영상. [68Ga]MB33의 종양-표적화 효능 및 약동학적 특성을 역동적 마이크로PET 스캔에 의해 평가하였다. 마우스당 대략 15 MBq를 주사하였다.
도 14: MB35의 PET - 영상
LNCaP 종양 이종 이식편을 갖는 무흉선 수컷 누드 마우스의 전신 관상 마이크로PET 영상. [68Ga]MB35의 종양-표적화 효능 및 약동학적 특성을 역동적 마이크로PET 스캔에 의해 평가하였다. 마우스당 대략 15 MBq를 주사하였다.
도 15: 68 Ga-CHX-DTPA를 주사한 마우스의 PET 스캔.
좌측은 미골부 사진, 중심은 배부 사진, 그리고 우측은 측부 사진. 상기 사진은 20 내지 40분 (상부), 40 내지 60분 (중심) 및 120 내지 140분 (하부)의 시간 범위를 포함한다.
도 16: MB-17 대 MB-17.D
LNCaP 종양 이종 이식편을 갖는 무흉선 수컷 누드 마우스의 전신 관상 마이크로PET 영상. 입체이성질체인 MB-17 및 MB-17 D의 종양-표적화 효능 및 약동학적 특성을 주사 후 2시간에 직접적으로 비교하였다.
도 17: 인간 PET/CT 영상: 68 Ga-표지 MB17
(a) 68Ga-표지 MB17 PET/CT를 이용한 첫 번째 임상 경험은 주사한 지 1시간 후 소림프절 전이의 검출을 보여주는데, 이는 높은 방사성 추적자 섭취율로 인한 것이다. 적색 화살표는 주사한 지 1시간 후 36.5의 SUVmax 및 52.1의 종양 대 배경 비를 갖는 대표적인 병변을 나타낸다. MIP = 주사한 지 1시간 후의 PET의 최대 강도 투사.
(b) 68Ga-표지 MB17 PET/CT의 상당한 이점으로는 심지어 낮은 PSA 수준에서의 병변의 고감도 검출이 있다.
도 18: 다발성 전립선암 전이를 갖는 환자의 PET 영상
(a) 첫 번째 스캔은 혈중 PSA 값이 14인 다발성 전립선암 전이를 갖는 환자의 초기 PET 영상을 보여준다. 2개월 후, 3.3 GBq의 177Lu-표지 MB17을 적용하였다. 이 시점에서, 혈중 PSA의 양은 38의 값에 도달하였다. 제1 사이클 후, PSA 수준은 8로 감소하였다. 제1 사이클 3개월 후, 추가의 4 GBq의 177Lu-표지 MB17을 적용하였다. 제2 사이클 1개월 후 대조 PET 스캔을 수행하였다. 상기 치료는 종양 병변 및 PSA 값에 유의한 영향을 나타냈으며, 골통을 감소시켰다.
(b) 그래프는 치료적 용량의 177Lu-표지 MB17의 제1 적용 후 감소한 PSA 값에 대한 상당한 영향을 보여준다.
Claims (59)
- 제1항에 있어서, 상기 염은 동결건조된 것인 화합물의 염.
- 제3항에 있어서, 상기 방사성 핵종이 89Zr, 44Sc, 111In, 90Y, 66Ga, 67Ga, 68Ga, 177Lu, 99mTc, 61Cu, 62Cu, 64Cu, 67Cu, 149Tb, 152Tb, 155Tb, 161Tb, 153Gd, 155Gd, 157Gd, 213Bi, 225Ac, 230U, 223Ra, 165Er, 123I, 131I, 또는 Fe 로부터 선택되는 것인 화합물의 염.
- 제3항에 있어서, 상기 방사성 핵종이 64Cu, 67Cu, 90Y, 68Ga, 177Lu, 또는 225Ac로부터 선택되는 것인 화합물의 염.
- 제3항에 있어서, 상기 방사성 핵종이 68Ga인 것인 화합물의 염.
- 제3항에 있어서, 상기 방사성 핵종이 177Lu인 것인 화합물의 염.
- 제3항에 있어서, 상기 방사성 핵종이 225Ac인 것인 화합물의 염.
- 제3항에 있어서, 상기 방사성 핵종이 64Cu 또는 67Cu로부터 선택된 것인 화합물의 염.
- 제11항에 있어서, 상기 방사성 핵종이 89Zr, 44Sc, 111In, 90Y, 66Ga, 67Ga, 68Ga, 177Lu, 99mTc, 61Cu, 62Cu, 64Cu, 67Cu, 149Tb, 152Tb, 155Tb, 161Tb, 153Gd, 155Gd, 157Gd, 213Bi, 225Ac, 230U, 223Ra, 165Er, 123I, 131I, 또는 Fe, 또는 이들의 조합으로부터 선택되고, 상기 조성물은 부형제를 더 포함하고, 상기 부형제는 상기 제약상 허용가능한 담체와 상이한 것인 약학 조성물.
- 제11항에 있어서, 상기 방사성 핵종이 64Cu, 67Cu, 90Y, 68Ga, 177Lu, 225Ac, 또는 이들의 조합으로부터 선택되는 것인 약학 조성물.
- 제11항에 있어서, 상기 방사성 핵종이 68Ga인 것인 약학 조성물.
- 제11항에 있어서, 상기 방사성 핵종이 177Lu인 것인 약학 조성물.
- 제11항에 있어서, 상기 방사성 핵종이 225Ac인 것인 약학 조성물.
- 제11항에 있어서, 상기 방사성 핵종이 64Cu 및 67Cu로부터 선택된 것인 약학 조성물.
- 제11항에 있어서, 상기 조성물이 완충 용액인 것인 약학 조성물.
- 제18항에 있어서, 상기 방사성 핵종이 68Ga 인 것인 약학 조성물.
- 제18항에 있어서, 상기 방사성 핵종이 177Lu인 것인 약학 조성물.
- 제18항에 있어서, 상기 방사성 핵종이 225Ac인 것인 약학 조성물.
- 제18항에 있어서, 상기 방사성 핵종이 90Y인 것인 약학 조성물.
- 제18항에 있어서, 상기 방사성 핵종이 64Cu 및 67Cu로부터 선택된 것인 약학 조성물.
- 제10항에 있어서, 상기 화합물의 염 및 제약상 허용가능한 담체는 동결건조된 것인 약학 조성물.
- 제12항 또는 제13항에 있어서, 상기 조성물은 완충 용액인 것인 약학 조성물.
- 제26항에 있어서, 상기 염은 동결건조된 것인 화합물의 염.
- 제28항에 있어서, 상기 방사성 핵종이 89Zr, 44Sc, 111In, 90Y, 66Ga, 67Ga, 68Ga, 177Lu, 99mTc, 61Cu, 62Cu, 64Cu, 67Cu, 149Tb, 152Tb, 155Tb, 161Tb, 153Gd, 155Gd, 157Gd, 213Bi, 225Ac, 230U, 223Ra, 165Er, 123I, 131I, 또는 Fe 로부터 선택되는 것인 화합물의 염.
- 제28항에 있어서, 상기 방사성 핵종이 64Cu, 67Cu, 90Y, 68Ga, 177Lu, 또는 225Ac로부터 선택되는 것인 화합물의 염.
- 제28항에 있어서, 상기 방사성 핵종이 68Ga인 것인 화합물의 염.
- 제28항에 있어서, 상기 방사성 핵종이 177Lu인 것인 화합물의 염.
- 제28항에 있어서, 상기 방사성 핵종이 225Ac인 것인 화합물의 염.
- 제28항에 있어서, 상기 방사성 핵종이 64Cu 또는 67Cu로부터 선택된 것인 화합물의 염.
- 제36항에 있어서, 상기 방사성 핵종이 89Zr, 44Sc, 111In, 90Y, 66Ga, 67Ga, 68Ga, 177Lu, 99mTc, 61Cu, 62Cu, 64Cu, 67Cu, 149Tb, 152Tb, 155Tb, 161Tb, 153Gd, 155Gd, 157Gd, 213Bi, 225Ac, 230U, 223Ra, 165Er, 123I, 131I, 또는 Fe, 또는 이들의 조합으로부터 선택되고, 상기 조성물은 부형제를 더 포함하고, 상기 부형제는 상기 제약상 허용가능한 담체와 상이한 것인 약학 조성물.
- 제36항에 있어서, 상기 방사성 핵종이 64Cu, 67Cu, 90Y, 68Ga, 177Lu, 225Ac, 또는 이들의 조합으로부터 선택되는 것인 약학 조성물.
- 제36항에 있어서, 상기 방사성 핵종이 68Ga인 것인 약학 조성물.
- 제36항에 있어서, 상기 방사성 핵종이 177Lu인 것인 약학 조성물.
- 제36항에 있어서, 상기 방사성 핵종이 225Ac인 것인 약학 조성물.
- 제36항에 있어서, 상기 방사성 핵종이 64Cu 또는 67Cu로부터 선택된 것인 약학 조성물.
- 제36항에 있어서, 상기 조성물이 완충 용액인 것인 약학 조성물.
- 제43항에 있어서, 상기 방사성 핵종이 68Ga 인 것인 약학 조성물.
- 제43항에 있어서, 상기 방사성 핵종이 177Lu인 것인 약학 조성물.
- 제43항에 있어서, 상기 방사성 핵종이 225Ac인 것인 약학 조성물.
- 제43항에 있어서, 상기 방사성 핵종이 90Y인 것인 약학 조성물.
- 제43항에 있어서, 상기 방사성 핵종이 64Cu 또는 67Cu로부터 선택된 것인 약학 조성물.
- 제35항에 있어서, 상기 화합물의 염 및 제약상 허용가능한 담체는 동결건조된 것인 약학 조성물.
- 제37항 또는 제38항에 있어서, 상기 조성물은 완충 용액인 것인 약학 조성물.
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PCT/EP2014/002808 WO2015055318A1 (en) | 2013-10-18 | 2014-10-17 | Labeled inhibitors of prostate specific membrane antigen (psma), their use as imaging agents and pharmaceutical agents for the treatment of prostate cancer |
KR1020197003504A KR102210931B1 (ko) | 2013-10-18 | 2014-10-17 | 전립선 특이적 막 항원(psma)의 표지된 억제제, 조영제로서의 이의 용도 및 전립선암 치료용 약제 |
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