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Targeted alpha therapy in a systemic mouse model of prostate cancer - a feasibility study
by
Dahlbom, Magnus
, Mona, Christine E.
, Lückerath, Katharina
, Wei, Liu H.
, Kim, Woosuk
, Slavik, Roger
, Stuparu, Andreea D.
, Meyer, Catherine A.L.
, Poddar, Soumya
, Radu, Caius G.
, Czernin, Johannes
, Girgis, Mark D.
, Evans-Axelsson, Susan L.
in
60 APPLIED LIFE SCIENCES
/ actinium
/ Actinium - therapeutic use
/ Alpha Particles - therapeutic use
/ Androgens
/ Animals
/ Brain cancer
/ Cancer and Oncology
/ Cancer och onkologi
/ Cancer therapies
/ Cell Line, Tumor
/ Clinical Medicine
/ Dipeptides - therapeutic use
/ Disease Models, Animal
/ Feasibility Studies
/ Heterocyclic Compounds, 1-Ring - therapeutic use
/ Humans
/ Klinisk medicin
/ Male
/ Medical and Health Sciences
/ Medicin och hälsovetenskap
/ Metastasis
/ metastatic mouse model
/ Mice
/ Prostate cancer
/ Prostate-Specific Antigen
/ Prostatic Neoplasms, Castration-Resistant - drug therapy
/ PSMA
/ RADIATION CHEMISTRY, RADIOCHEMISTRY, AND NUCLEAR CHEMISTRY
/ Radiopharmaceuticals - therapeutic use
/ Research Paper
/ Survival analysis
/ targeted alpha therapy
2020
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Targeted alpha therapy in a systemic mouse model of prostate cancer - a feasibility study
by
Dahlbom, Magnus
, Mona, Christine E.
, Lückerath, Katharina
, Wei, Liu H.
, Kim, Woosuk
, Slavik, Roger
, Stuparu, Andreea D.
, Meyer, Catherine A.L.
, Poddar, Soumya
, Radu, Caius G.
, Czernin, Johannes
, Girgis, Mark D.
, Evans-Axelsson, Susan L.
in
60 APPLIED LIFE SCIENCES
/ actinium
/ Actinium - therapeutic use
/ Alpha Particles - therapeutic use
/ Androgens
/ Animals
/ Brain cancer
/ Cancer and Oncology
/ Cancer och onkologi
/ Cancer therapies
/ Cell Line, Tumor
/ Clinical Medicine
/ Dipeptides - therapeutic use
/ Disease Models, Animal
/ Feasibility Studies
/ Heterocyclic Compounds, 1-Ring - therapeutic use
/ Humans
/ Klinisk medicin
/ Male
/ Medical and Health Sciences
/ Medicin och hälsovetenskap
/ Metastasis
/ metastatic mouse model
/ Mice
/ Prostate cancer
/ Prostate-Specific Antigen
/ Prostatic Neoplasms, Castration-Resistant - drug therapy
/ PSMA
/ RADIATION CHEMISTRY, RADIOCHEMISTRY, AND NUCLEAR CHEMISTRY
/ Radiopharmaceuticals - therapeutic use
/ Research Paper
/ Survival analysis
/ targeted alpha therapy
2020
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Targeted alpha therapy in a systemic mouse model of prostate cancer - a feasibility study
by
Dahlbom, Magnus
, Mona, Christine E.
, Lückerath, Katharina
, Wei, Liu H.
, Kim, Woosuk
, Slavik, Roger
, Stuparu, Andreea D.
, Meyer, Catherine A.L.
, Poddar, Soumya
, Radu, Caius G.
, Czernin, Johannes
, Girgis, Mark D.
, Evans-Axelsson, Susan L.
in
60 APPLIED LIFE SCIENCES
/ actinium
/ Actinium - therapeutic use
/ Alpha Particles - therapeutic use
/ Androgens
/ Animals
/ Brain cancer
/ Cancer and Oncology
/ Cancer och onkologi
/ Cancer therapies
/ Cell Line, Tumor
/ Clinical Medicine
/ Dipeptides - therapeutic use
/ Disease Models, Animal
/ Feasibility Studies
/ Heterocyclic Compounds, 1-Ring - therapeutic use
/ Humans
/ Klinisk medicin
/ Male
/ Medical and Health Sciences
/ Medicin och hälsovetenskap
/ Metastasis
/ metastatic mouse model
/ Mice
/ Prostate cancer
/ Prostate-Specific Antigen
/ Prostatic Neoplasms, Castration-Resistant - drug therapy
/ PSMA
/ RADIATION CHEMISTRY, RADIOCHEMISTRY, AND NUCLEAR CHEMISTRY
/ Radiopharmaceuticals - therapeutic use
/ Research Paper
/ Survival analysis
/ targeted alpha therapy
2020
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Targeted alpha therapy in a systemic mouse model of prostate cancer - a feasibility study
Journal Article
Targeted alpha therapy in a systemic mouse model of prostate cancer - a feasibility study
2020
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Overview
Ac-PSMA-617 targeted-therapy has demonstrated efficacy in 75-85% of patients; however, responses are not durable. We aimed to establish translatable mouse models of disseminated prostate cancer (PCa) to evaluate effectiveness of
Ac-PSMA-617 at various disease stages.
: C4-2, C4-2B, or 22Rv1 cells were injected into the left ventricle of male NSG mice. Disease progression was monitored using bioluminescence imaging (BLI). For treatment, mice were injected with 40 kBq
Ac-PSMA-617 at one (early treatment cohort) or three weeks (late treatment cohort) post-inoculation. Treatment efficacy was monitored by BLI of whole-body tumor burden. Mice were sacrificed based on body conditioning score.
: C4-2 cells yielded metastases in liver, lungs, spleen, stomach, bones, and brain - achieving a clinically relevant model of widespread metastatic disease. The disease burden in the early treatment cohort was stable over 27 weeks in 5/9 mice and progressive in 4/9 mice. These mice were sacrificed due to brain metastases. Median survival of the late treatment cohort was superior to controls (13 vs. 7 weeks; p<0.0001) but inferior to that in the early treatment cohort (13 vs. 27 weeks; p<0.001). Late cohort mice succumbed to extensive liver involvement. The 22Rv1 and C4-2B systemic models were not used for treatment due to high kidney metastatic burden or low take rate, respectively.
: C4-2 cells reproduced metastatic cancer spread most relevantly. Early treatment with
Ac-PSMA-617 prevented liver metastases and led to significant survival benefit. Late treatment improved survival without reducing tumor burden in the liver, the main site of metastasis. The current findings suggest that early
Ac-PSMA-617 intervention is more efficacious in the setting of widespread metastatic PCa.
Publisher
Ivyspring International Publisher Pty Ltd,Ivyspring,Ivyspring International Publisher
Subject
/ actinium
/ Alpha Particles - therapeutic use
/ Animals
/ Dipeptides - therapeutic use
/ Heterocyclic Compounds, 1-Ring - therapeutic use
/ Humans
/ Male
/ Mice
/ Prostatic Neoplasms, Castration-Resistant - drug therapy
/ PSMA
/ RADIATION CHEMISTRY, RADIOCHEMISTRY, AND NUCLEAR CHEMISTRY
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