Size-Optimized Ultrasmall Porous Silica Nanoparticles Depict Vasculature-Based Differential Targeting in Triple Negative Breast Cancer

Shreya Goel; Carolina A. Ferreira; Prashant Dogra; Bo Yu; Christopher J. Kutyreff; Cerise M. Siamof; Jonathan W. Engle; Todd E. Barnhart; Vittorio Cristini; Zhihui Wang; Weibo Cai

doi:10.1002/smll.201903747

Size-Optimized Ultrasmall Porous Silica Nanoparticles Depict Vasculature-Based Differential Targeting in Triple Negative Breast Cancer

Shreya Goel, Carolina A. Ferreira, Prashant Dogra, Bo Yu, Christopher J. Kutyreff, Cerise M. Siamof, Jonathan W. Engle, Todd E. Barnhart, Vittorio Cristini, Zhihui Wang^*, Weibo Cai

^*Corresponding author for this work

Radiology

Research output: Contribution to journal › Article › peer-review

38 Scopus citations

Abstract

Rapid sequestration and prolonged retention of intravenously injected nanoparticles by the liver and spleen (reticuloendothelial system (RES)) presents a major barrier to effective delivery to the target site and hampers clinical translation of nanomedicine. Inspired by biological macromolecular drugs, synthesis of ultrasmall (diameter ≈12–15 nm) porous silica nanoparticles (UPSNs), capable of prolonged plasma half-life, attenuated RES sequestration, and accelerated hepatobiliary clearance, is reported. The study further investigates the effect of tumor vascularization on uptake and retention of UPSNs in two mouse models of triple negative breast cancer with distinctly different microenvironments. A semimechanistic mathematical model is developed to gain mechanistic insights into the interactions between the UPSNs and the biological entities of interest, specifically the RES. Despite similar systemic pharmacokinetic profiles, UPSNs demonstrate strikingly different tumor responses in the two models. Histopathology confirms the differences in vasculature and stromal status of the two models, and corresponding differences in the microscopic distribution of UPSNs within the tumors. The studies demonstrate the successful application of multidisciplinary and complementary approaches, based on laboratory experimentation and mathematical modeling, to concurrently design optimized nanomaterials, and investigate their complex biological interactions, in order to drive innovation and translation.

Original language	English (US)
Article number	1903747
Journal	Small
Volume	15
Issue number	46
DOIs	https://doi.org/10.1002/smll.201903747
State	Published - Nov 1 2019

Funding

S.G., C.A.F, and P.D. contributed equally to this work. This work was supported by the University of Wisconsin – Madison and the National Institutes of Health P30CA014520, and the Brazilian Science without Borders Program SwB‐CNPq. This research was also supported in part by the National Science Foundation Grant DMS‐1716737, the National Institutes of Health (NIH) Grants 1U01CA196403, 1U01CA213759, 1R01CA226537, 1R01CA222007, and U54CA210181. S.G., C.A.F, and P.D. contributed equally to this work. This work was supported by the University of Wisconsin ? Madison and the National Institutes of Health P30CA014520, and the Brazilian Science without Borders Program SwB-CNPq. This research was also supported in part by the National Science Foundation Grant DMS-1716737, the National Institutes of Health (NIH) Grants 1U01CA196403, 1U01CA213759, 1R01CA226537, 1R01CA222007, and U54CA210181.

Keywords

mathematical modeling
pharmacokinetics
positron emission tomography
tumor microenvironment
ultrasmall porous silica

ASJC Scopus subject areas

Biotechnology
General Chemistry
Biomaterials
General Materials Science
Engineering (miscellaneous)

UN SDGs

This output contributes to the following UN Sustainable Development Goals (SDGs)

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title = "Size-Optimized Ultrasmall Porous Silica Nanoparticles Depict Vasculature-Based Differential Targeting in Triple Negative Breast Cancer",

abstract = "Rapid sequestration and prolonged retention of intravenously injected nanoparticles by the liver and spleen (reticuloendothelial system (RES)) presents a major barrier to effective delivery to the target site and hampers clinical translation of nanomedicine. Inspired by biological macromolecular drugs, synthesis of ultrasmall (diameter ≈12–15 nm) porous silica nanoparticles (UPSNs), capable of prolonged plasma half-life, attenuated RES sequestration, and accelerated hepatobiliary clearance, is reported. The study further investigates the effect of tumor vascularization on uptake and retention of UPSNs in two mouse models of triple negative breast cancer with distinctly different microenvironments. A semimechanistic mathematical model is developed to gain mechanistic insights into the interactions between the UPSNs and the biological entities of interest, specifically the RES. Despite similar systemic pharmacokinetic profiles, UPSNs demonstrate strikingly different tumor responses in the two models. Histopathology confirms the differences in vasculature and stromal status of the two models, and corresponding differences in the microscopic distribution of UPSNs within the tumors. The studies demonstrate the successful application of multidisciplinary and complementary approaches, based on laboratory experimentation and mathematical modeling, to concurrently design optimized nanomaterials, and investigate their complex biological interactions, in order to drive innovation and translation.",

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author = "Shreya Goel and Ferreira, {Carolina A.} and Prashant Dogra and Bo Yu and Kutyreff, {Christopher J.} and Siamof, {Cerise M.} and Engle, {Jonathan W.} and Barnhart, {Todd E.} and Vittorio Cristini and Zhihui Wang and Weibo Cai",

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Size-Optimized Ultrasmall Porous Silica Nanoparticles Depict Vasculature-Based Differential Targeting in Triple Negative Breast Cancer

Abstract

Funding

Keywords

ASJC Scopus subject areas

UN SDGs

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