SR-B1-targeted nanodelivery of anti-cancer agents: a promising new approach to treat triple-negative breast cancer

SR-B1-targeted nanodelivery of anti-cancer agents: a promising new approach to treat triple-negative breast cancer

Rebecca Johnson,1 Nirupama Sabnis,2 Xiangle Sun,1 Ruhani Ahluwalia,3 Andras G Lacko2,4 1Institute of Molecular Medicine, 2Institute for Cardiovascular and Metabolic Diseases, University of North Texas Health Science Center, 3Harmony School of Innovation, 4Department of Pediatrics, University of Nort...

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Main Authors: Johnson R, Sabnis N, Sun X, Ahluwalia R, Lacko AG
Format: Article
Language:English
Published: Dove Medical Press 2017-06-01
Series:Breast Cancer : Targets and Therapy
Subjects:
breast cancer
TNBC
rHDL nanoparticles
SR-B1 receptors
targeted drug delivery
lapatinib
valrubicin
Online Access:https://www.dovepress.com/sr-b1-targeted-nanodelivery-of-anti-cancer-agents-a-promising-new-appr-peer-reviewed-article-BCTT
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spelling doaj-f7262946c78546ec9f27e10edded8f4c2020-11-24T22:09:30ZengDove Medical PressBreast Cancer : Targets and Therapy1179-13142017-06-01Volume 938339233064SR-B1-targeted nanodelivery of anti-cancer agents: a promising new approach to treat triple-negative breast cancerJohnson RSabnis NSun XAhluwalia RLacko AGRebecca Johnson,1 Nirupama Sabnis,2 Xiangle Sun,1 Ruhani Ahluwalia,3 Andras G Lacko2,4 1Institute of Molecular Medicine, 2Institute for Cardiovascular and Metabolic Diseases, University of North Texas Health Science Center, 3Harmony School of Innovation, 4Department of Pediatrics, University of North Texas Health Science Center, Fort Worth, TX, USA Abstract: Patients with triple-negative breast cancer (TNBC) have a considerably less favorable prognosis than those with hormone-positive breast cancers. TNBC patients do not respond to current endocrine treatment and have a 5-year survival prognosis of <30%. The research presented here is intended to fill a void toward the much needed development of improved treatment strategies for metastatic TNBC. The overall goal of this research was to evaluate the effectiveness of reconstituted high-density lipoprotein (rHDL) nanoparticles (NPs) as delivery agents for anti-TNBC drugs. Using lapatinib and valrubicin as components of the rHDL/drug complexes resulted in a significantly better performance of the NP-transported drugs compared with their free (unencapsulated) counterparts. The enhancement of the therapeutic effect and the protection of normal cells (cardiomyocytes) achieved via the rHDL NPs were likely due to the overexpression of the high-density lipoprotein (HDL) (scavenger receptor class B type 1 [SR-B1]) receptor by the TNBC cells. Keywords: breast cancer, TNBC, rHDL nanoparticles, SR-B1 receptors, targeted drug delivery, lapatinib, valrubicinhttps://www.dovepress.com/sr-b1-targeted-nanodelivery-of-anti-cancer-agents-a-promising-new-appr-peer-reviewed-article-BCTTbreast cancerTNBCrHDL nanoparticlesSR-B1 receptorstargeted drug deliverylapatinibvalrubicin
collection DOAJ
language English
format Article
sources DOAJ
author Johnson R
Sabnis N
Sun X
Ahluwalia R
Lacko AG
spellingShingle Johnson R
Sabnis N
Sun X
Ahluwalia R
Lacko AG
SR-B1-targeted nanodelivery of anti-cancer agents: a promising new approach to treat triple-negative breast cancer
Breast Cancer : Targets and Therapy
breast cancer
TNBC
rHDL nanoparticles
SR-B1 receptors
targeted drug delivery
lapatinib
valrubicin
author_facet Johnson R
Sabnis N
Sun X
Ahluwalia R
Lacko AG
author_sort Johnson R
title SR-B1-targeted nanodelivery of anti-cancer agents: a promising new approach to treat triple-negative breast cancer
title_short SR-B1-targeted nanodelivery of anti-cancer agents: a promising new approach to treat triple-negative breast cancer
title_full SR-B1-targeted nanodelivery of anti-cancer agents: a promising new approach to treat triple-negative breast cancer
title_fullStr SR-B1-targeted nanodelivery of anti-cancer agents: a promising new approach to treat triple-negative breast cancer
title_full_unstemmed SR-B1-targeted nanodelivery of anti-cancer agents: a promising new approach to treat triple-negative breast cancer
title_sort sr-b1-targeted nanodelivery of anti-cancer agents: a promising new approach to treat triple-negative breast cancer
publisher Dove Medical Press
series Breast Cancer : Targets and Therapy
issn 1179-1314
publishDate 2017-06-01
description Rebecca Johnson,1 Nirupama Sabnis,2 Xiangle Sun,1 Ruhani Ahluwalia,3 Andras G Lacko2,4 1Institute of Molecular Medicine, 2Institute for Cardiovascular and Metabolic Diseases, University of North Texas Health Science Center, 3Harmony School of Innovation, 4Department of Pediatrics, University of North Texas Health Science Center, Fort Worth, TX, USA Abstract: Patients with triple-negative breast cancer (TNBC) have a considerably less favorable prognosis than those with hormone-positive breast cancers. TNBC patients do not respond to current endocrine treatment and have a 5-year survival prognosis of <30%. The research presented here is intended to fill a void toward the much needed development of improved treatment strategies for metastatic TNBC. The overall goal of this research was to evaluate the effectiveness of reconstituted high-density lipoprotein (rHDL) nanoparticles (NPs) as delivery agents for anti-TNBC drugs. Using lapatinib and valrubicin as components of the rHDL/drug complexes resulted in a significantly better performance of the NP-transported drugs compared with their free (unencapsulated) counterparts. The enhancement of the therapeutic effect and the protection of normal cells (cardiomyocytes) achieved via the rHDL NPs were likely due to the overexpression of the high-density lipoprotein (HDL) (scavenger receptor class B type 1 [SR-B1]) receptor by the TNBC cells. Keywords: breast cancer, TNBC, rHDL nanoparticles, SR-B1 receptors, targeted drug delivery, lapatinib, valrubicin
topic breast cancer
TNBC
rHDL nanoparticles
SR-B1 receptors
targeted drug delivery
lapatinib
valrubicin
url https://www.dovepress.com/sr-b1-targeted-nanodelivery-of-anti-cancer-agents-a-promising-new-appr-peer-reviewed-article-BCTT
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