Photothermal Therapy Generates a Thermal Window of Immunogenic Cell Death in Neuroblastoma

被引:213
作者
Sweeney, Elizabeth E. [1 ,2 ]
Cano-Mejia, Juliana [1 ,2 ,3 ]
Fernandes, Rohan [1 ,2 ,3 ,4 ]
机构
[1] George Washington Univ, George Washington Canc Ctr, 800 22nd St NW,8th Floor,Sci & Engn Hall, Washington, DC 20052 USA
[2] Childrens Natl Hlth Syst, Sheikh Zayed Inst Pediat Surg Innovat, 111 Michigan Ave NW,6th Floor Main Hosp, Washington, DC 20010 USA
[3] Univ Maryland, Fischell Dept Bioengn, Room 2330,Jeong H Kim Engn Bldg, College Pk, MD 20742 USA
[4] George Washington Univ, Dept Med, 2150 Penn Ave NW,Suite 8-416, Washington, DC 20037 USA
关键词
immunogenic cell death; neuroblastoma; photothermal therapy; Prussian blue nanoparticles; thermal dose; PRUSSIAN BLUE NANOPARTICLES; QUANTITATIVE-DETERMINATION; FERRIC HEXACYANOFERRATE; CARBON NANOTUBES; CANCER; RESPONSES; BINDING; DAMAGE; OXIDE; HMGB1;
D O I
10.1002/smll.201800678
中图分类号
O6 [化学];
学科分类号
0703 ;
摘要
A thermal window of immunogenic cell death (ICD) elicited by nanoparticle-based photothermal therapy (PTT) in an animal model of neuroblastoma is described. In studies using Prussian blue nanoparticles to administer photothermal therapy (PBNP-PTT) to established localized tumors in the neuroblastoma model, it is observed that PBNP-PTT conforms to the more is better paradigm, wherein higher doses of PBNP-PTT generates higher cell/local heating and thereby more cell death, and consequently improved animal survival. However, in vitro analysis of the biochemical correlates of ICD (ATP, high-motility group box 1, and calreticulin) elicited by PBNP-PTT demonstrates that PBNP-PTT triggers a thermal window of ICD. ICD markers are highly expressed within an optimal temperature (thermal dose) window of PBNP-PTT (63.3-66.4 degrees C) as compared with higher (83.0-83.5 degrees C) and lower PBNP-PTT (50.7-52.7 degrees C) temperatures, which both yield lower expression. Subsequent vaccination studies in the neuroblastoma model confirm the in vitro findings, wherein PBNP-PTT administered within the optimal temperature window results in long-term survival (33.3% at 100 d) compared with PBNP-PTT administered within the higher (0%) and lower (20%) temperature ranges, and controls (0%). The findings demonstrate a tunable immune response to heat generated by PBNP-PTT, which should be critically engaged in the administration of PTT for maximizing its therapeutic benefits.
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页数:8
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