Inhibition of CCL2 Signaling in Combination with Docetaxel Treatment Has Profound Inhibitory Effects on Prostate Cancer Growth in Bone

The C-C chemokine ligand 2 (CCL2) stimulates migration, proliferation, and invasion of prostate cancer (PCa) cells, and its signaling also plays a role in the activation of osteoclasts. Therefore targeting CCL2 signaling in regulation of tumor progression in bone metastases is an area of intense res...

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Main Authors: Eva Corey, Robert L. Vessella, Linda A. Snyder, Holly M. Nguyen, Lisha G. Brown, Theodore Koreckij, Peter S. Kirk
Format: Article
Language:English
Published: MDPI AG 2013-05-01
Series:International Journal of Molecular Sciences
Subjects:
Online Access:http://www.mdpi.com/1422-0067/14/5/10483
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spelling doaj-1ff6ffeea7b24c3f8ebcd3eff6e1a2c02020-11-25T00:20:32ZengMDPI AGInternational Journal of Molecular Sciences1422-00672013-05-01145104831049610.3390/ijms140510483Inhibition of CCL2 Signaling in Combination with Docetaxel Treatment Has Profound Inhibitory Effects on Prostate Cancer Growth in BoneEva CoreyRobert L. VessellaLinda A. SnyderHolly M. NguyenLisha G. BrownTheodore KoreckijPeter S. KirkThe C-C chemokine ligand 2 (CCL2) stimulates migration, proliferation, and invasion of prostate cancer (PCa) cells, and its signaling also plays a role in the activation of osteoclasts. Therefore targeting CCL2 signaling in regulation of tumor progression in bone metastases is an area of intense research. The objective of our study was to investigate the efficacy of CCL2 blockade by neutralizing antibodies to inhibit the growth of PCa in bone. We used a preclinical model of cancer growth in the bone in which PCa C4-2B cells were injected directly into murine tibiae. Animals were treated for ten weeks with neutralizing anti-CCL2 antibodies, docetaxel, or a combination of both, and then followed an additional nine weeks. CCL2 blockade inhibited the growth of PCa in bone, with even more pronounced inhibition in combination with docetaxel. CCL2 blockade also resulted in increases in bone mineral density. Furthermore, our results showed that the tumor inhibition lasted even after discontinuation of the treatment. Our data provide compelling evidence that CCL2 blockade slows PCa growth in bone, both alone and in combination with docetaxel. These results support the continued investigations of CCL2 blockade as a treatment for advanced metastatic PCa.http://www.mdpi.com/1422-0067/14/5/10483prostate cancerbone metastaseschemokineCCL2docetaxelbone metastases
collection DOAJ
language English
format Article
sources DOAJ
author Eva Corey
Robert L. Vessella
Linda A. Snyder
Holly M. Nguyen
Lisha G. Brown
Theodore Koreckij
Peter S. Kirk
spellingShingle Eva Corey
Robert L. Vessella
Linda A. Snyder
Holly M. Nguyen
Lisha G. Brown
Theodore Koreckij
Peter S. Kirk
Inhibition of CCL2 Signaling in Combination with Docetaxel Treatment Has Profound Inhibitory Effects on Prostate Cancer Growth in Bone
International Journal of Molecular Sciences
prostate cancer
bone metastases
chemokine
CCL2
docetaxel
bone metastases
author_facet Eva Corey
Robert L. Vessella
Linda A. Snyder
Holly M. Nguyen
Lisha G. Brown
Theodore Koreckij
Peter S. Kirk
author_sort Eva Corey
title Inhibition of CCL2 Signaling in Combination with Docetaxel Treatment Has Profound Inhibitory Effects on Prostate Cancer Growth in Bone
title_short Inhibition of CCL2 Signaling in Combination with Docetaxel Treatment Has Profound Inhibitory Effects on Prostate Cancer Growth in Bone
title_full Inhibition of CCL2 Signaling in Combination with Docetaxel Treatment Has Profound Inhibitory Effects on Prostate Cancer Growth in Bone
title_fullStr Inhibition of CCL2 Signaling in Combination with Docetaxel Treatment Has Profound Inhibitory Effects on Prostate Cancer Growth in Bone
title_full_unstemmed Inhibition of CCL2 Signaling in Combination with Docetaxel Treatment Has Profound Inhibitory Effects on Prostate Cancer Growth in Bone
title_sort inhibition of ccl2 signaling in combination with docetaxel treatment has profound inhibitory effects on prostate cancer growth in bone
publisher MDPI AG
series International Journal of Molecular Sciences
issn 1422-0067
publishDate 2013-05-01
description The C-C chemokine ligand 2 (CCL2) stimulates migration, proliferation, and invasion of prostate cancer (PCa) cells, and its signaling also plays a role in the activation of osteoclasts. Therefore targeting CCL2 signaling in regulation of tumor progression in bone metastases is an area of intense research. The objective of our study was to investigate the efficacy of CCL2 blockade by neutralizing antibodies to inhibit the growth of PCa in bone. We used a preclinical model of cancer growth in the bone in which PCa C4-2B cells were injected directly into murine tibiae. Animals were treated for ten weeks with neutralizing anti-CCL2 antibodies, docetaxel, or a combination of both, and then followed an additional nine weeks. CCL2 blockade inhibited the growth of PCa in bone, with even more pronounced inhibition in combination with docetaxel. CCL2 blockade also resulted in increases in bone mineral density. Furthermore, our results showed that the tumor inhibition lasted even after discontinuation of the treatment. Our data provide compelling evidence that CCL2 blockade slows PCa growth in bone, both alone and in combination with docetaxel. These results support the continued investigations of CCL2 blockade as a treatment for advanced metastatic PCa.
topic prostate cancer
bone metastases
chemokine
CCL2
docetaxel
bone metastases
url http://www.mdpi.com/1422-0067/14/5/10483
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