Abstract P186: Preclinical evaluation of the proteasome inhibitor ixazomib (MLN2238) on nasopharyngeal cacinoma (NPC)

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Victor Ho Fun Lee ◽  
George Sai Wah Tsao
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Wing-Yan Au ◽  
Tianhuan Guo ◽  
Kai-Yau Wong ◽  
Michelle L. Wong ◽  
...  

2019 ◽  
Vol 19 (10) ◽  
pp. e130-e131
Author(s):  
Sarah Holstein ◽  
Staci Haney ◽  
Michelle Varney ◽  
Lynette Smith

2005 ◽  
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P. Richardson ◽  
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2011 ◽  
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F Sarac ◽  
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A Gal ◽  
M Taulescu ◽  
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2011 ◽  
Vol 71 (08) ◽  
Author(s):  
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P Wilkerson ◽  
D Wetterskog ◽  
MB Lambros ◽  
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A. Faust

SummaryOptical imaging has long been considered a method for histological or microscopic investigations. Over the last 15 years, however, this method was applied for preclinical molecular imaging and, just recently, was also able to show its principal potential for clinical applications (e.g. fluorescence-guided surgery). Reviewing the development and preclinical evaluation of new fluorescent dyes and target-specific dye conjugates, these often show characteristic patterns of their routes of excretion and biodistribution, which could also be interesting for the development and optimization of radiopharmaceuticals. Especially ionic charges show a great influence on biodistribution and netcharge and charge-distribution on a conjugate often determines unspecific binding or background signals in liver, kidney or intestine, and other organs.Learning from fluorescent probe behaviour in vivo and translating this knowledge to radio-pharmaceuticals might be useful to further optimize emerging and existing radiopharmaceuticals with respect to their biodistribution and thereby availability for binding to their targets.


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