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	<title>Therapeutic | Nano Publications</title>
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	<title>Therapeutic | Nano Publications</title>
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		<title>2017 &#8211; Specific adaptive immune pattern induced by NBTXR3 exposed to radiation therapy in soft tissue sarcoma (STS) patients</title>
		<link>https://bibliography.nanobiotix.com/2017-specific-adaptive-immune-pattern-induced-by-nbtxr3-exposed-to-radiation-therapy-in-soft-tissue-sarcoma-patients/</link>
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		<dc:creator><![CDATA[nano-pub]]></dc:creator>
		<pubDate>Thu, 18 May 2017 13:32:46 +0000</pubDate>
				<category><![CDATA[Clinical Data NBTXR3]]></category>
		<category><![CDATA[Congress Abstracts]]></category>
		<category><![CDATA[STS]]></category>
		<category><![CDATA[Biomarkers]]></category>
		<category><![CDATA[Cell]]></category>
		<category><![CDATA[Cytokine]]></category>
		<category><![CDATA[Density]]></category>
		<category><![CDATA[Electron]]></category>
		<category><![CDATA[Hafnium]]></category>
		<category><![CDATA[Hafnium Oxide]]></category>
		<category><![CDATA[Immunity]]></category>
		<category><![CDATA[Immunoscore]]></category>
		<category><![CDATA[Immunosign]]></category>
		<category><![CDATA[Inflammatory]]></category>
		<category><![CDATA[Injection]]></category>
		<category><![CDATA[Intratumor]]></category>
		<category><![CDATA[Local]]></category>
		<category><![CDATA[Preoperative]]></category>
		<category><![CDATA[Radiation]]></category>
		<category><![CDATA[Radiotherapy]]></category>
		<category><![CDATA[Sarcoma]]></category>
		<category><![CDATA[Soft Tissue Sarcoma]]></category>
		<category><![CDATA[Therapeutic]]></category>
		<guid isPermaLink="false">http://bibliography.nanobiotix.com/?p=1128/</guid>

					<description><![CDATA[<p>NBTXR3 are functionalized hafnium oxide nanoparticles, undergoing seven clinical trials for enhancing radiation therapy (RT). The high electron density of the nanoparticles, when exposed to radiotherapy (NBTXR3 + RT), allow absorption/deposition of a high radiation dose within the cancer cells to physically kill the cells, and possibly improve outcome. Besides, NBTXR3 + RT has shown subsequent ability to enhance immunogenic cell death and immune response in preclinics. We hypothesized that NBTXR3 + RT could trigger an enhanced immune response when compared to RT in patients with STS.</p>
The post <a href="https://bibliography.nanobiotix.com/2017-specific-adaptive-immune-pattern-induced-by-nbtxr3-exposed-to-radiation-therapy-in-soft-tissue-sarcoma-patients/">2017 – Specific adaptive immune pattern induced by NBTXR3 exposed to radiation therapy in soft tissue sarcoma (STS) patients</a> first appeared on <a href="https://bibliography.nanobiotix.com">Nano Publications</a>.]]></description>
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            </div><div class="az-box-icon-content az-font-custom az-font-color-custom" style="color: #ffffff;"><h3 class="az-box-icon-title">Authors</h3><p>Jerome Galon, Marick Laé, Zsuzsanna Papai, Philippe Rochaix, Laszlo Csaba Mangel, Bernhard Mlecnik, Fabienne Hermitte, Zoltan Sapi, Martine Delannes, Tamas Tornoczky, Anne Vincent-Salomon, Sylvie Bonvalot<br />
<span class="notes">Laboratory of Integrative Cancer Immunology, INSERM, Paris, France; Institut Curie, Paris, France; Magyar Honvedseg Egeszsegugyi Kozpont, Budapest, Hungary; Institut Universitaire du Cancer &#8211; Oncopole, Toulouse, France; Pecs University, Pecs, Hungary; INSERM, Paris, France; HalioDx, Marseille, France; Semmelweis University, Budapest, Hungary</span></p>
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<div class="az-content-element-wrapper az-empty-divider hidden-lg hidden-md" style="height: 60px;"></div></div></div></div><div data-animation-type="ani-in" data-animation-in="fadeInUp" data-animation-out="none" data-animation-speed="default" data-animation-delay="300" data-offset-down="90" data-offset-up="none" class="single-clms col-md-6 az-main-col-content az-module az-col-pos-middle az-v-space-clm animate-content az-module-bg-color"><div class="az-col az-clm-padding-105" >
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            </div><div class="az-box-icon-content"><h3 class="az-box-icon-title">Summary</h3><p><strong>Background:</strong> NBTXR3 are functionalized hafnium oxide nanoparticles, undergoing seven clinical trials for enhancing radiation therapy (RT). The high electron density of the nanoparticles, when exposed to radiotherapy (NBTXR3 + RT), allow absorption/deposition of a high radiation dose within the cancer cells to physically kill the cells, and possibly improve outcome. Besides, NBTXR3 + RT has shown subsequent ability to enhance immunogenic cell death and immune response in preclinics. We hypothesized that NBTXR3 + RT could trigger an enhanced immune response when compared to RT in patients with STS.</p>
<p><strong>Methods:</strong> Tumor tissues pre- (biopsy) and/or post-treatment (resection) were collected from patients (pts) with locally advanced STS, who received either NBTXR3 as intratumor injection and RT (14 pts) or RT (12 pts), as preoperative treatment (NCT02379845). Immunohistochemistry and Digital Pathology for immune biomarkers and for Immunoscore (CD3/CD8) were analyzed. Gene expression profiling and pre-optimized immune-gene signatures called Immunosign were also used.</p>
<p><strong>Results:</strong> A significant increase of T cells (CD3+, CD8+) and a marked increase of CD103+ immune cell infiltration post- vs pre-treatment were observed for NBTXR3 + RT (P&lt; 0.01), while no differences were seen for RT. Post-treatment, an increased Immunoscore (CD3 + CD8 cell densities) was observed for NBTXR3 + RT compared to RT (P &lt; 0.07). Consistently, the up-regulation of pan immune genes expression and specifically expression of adaptive immunity genes between pre- and post-treatment, was pronounced for NBTXR3 + RT when compared to RT. Functional analysis of genes up-regulated in NBTXR3 + RT showed an enrichment of cytokine activity (IL7, IFNA, IL16, IL11, IFNG), adaptive immunity (RAG1, GZMA, TAP1, TAP2, TBX21, STAT4, IFNG, LCK, LTK, CD37, CD22) and T cell receptor signaling pathway (CD28, CTLA4, CD274, BTLA, TIGIT, CD40LG, CD5, CD3E, ZAP70).</p>
<p><strong>Conclusions:</strong> NBTXR3 + RT induces a specific adaptive immune pattern. As such, it may contribute to convert “cold” tumor into “hot” tumor and be effectively combined with immunotherapeutic agents across oncology. These data warrant more tissue samples evaluation to reinforce these findings.</p>
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</div>
<div class="az-content-element-wrapper az-empty-divider hidden-lg hidden-md" style="height: 60px;"></div></div></div></div></div></div></div></div></div></div></div>The post <a href="https://bibliography.nanobiotix.com/2017-specific-adaptive-immune-pattern-induced-by-nbtxr3-exposed-to-radiation-therapy-in-soft-tissue-sarcoma-patients/">2017 – Specific adaptive immune pattern induced by NBTXR3 exposed to radiation therapy in soft tissue sarcoma (STS) patients</a> first appeared on <a href="https://bibliography.nanobiotix.com">Nano Publications</a>.]]></content:encoded>
					
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		<item>
		<title>2015 &#8211; Metals as radio-enhancers in oncology &#8211; Pottier et al.</title>
		<link>https://bibliography.nanobiotix.com/2015-metals-as-radio-enhancers-in-oncology-pottier-et-al/</link>
					<comments>https://bibliography.nanobiotix.com/2015-metals-as-radio-enhancers-in-oncology-pottier-et-al/#respond</comments>
		
		<dc:creator><![CDATA[nano-pub]]></dc:creator>
		<pubDate>Tue, 14 Feb 2017 15:25:15 +0000</pubDate>
				<category><![CDATA[Miscellaneous]]></category>
		<category><![CDATA[NO-RIGHTS]]></category>
		<category><![CDATA[Publications]]></category>
		<category><![CDATA[Cellular]]></category>
		<category><![CDATA[Industry]]></category>
		<category><![CDATA[Ionizing]]></category>
		<category><![CDATA[Metal]]></category>
		<category><![CDATA[Oncology]]></category>
		<category><![CDATA[Radiation]]></category>
		<category><![CDATA[Radionenhancer]]></category>
		<category><![CDATA[Therapeutic]]></category>
		<category><![CDATA[Tumor]]></category>
		<guid isPermaLink="false">http://bibliography.nanobiotix.com/?p=547</guid>

					<description><![CDATA[<p>Radio-enhancers, metal-based nanosized agents, could play a key role in oncology. They may unlock the potential of radiotherapy by enhancing the radiation dose deposit within tumors when the ionizing radiation source is ‘on’, while exhibiting chemically inert behavior in cellular and subcellular systems when the radiation beam is ‘off’. Important decision points support the development of these new type of therapeutic agents originated from nanotechnology. Here, we discuss from an industry perspective, the interest of developing radio-enhancer agents to improve tumor control, the relevance of nanotechnology to achieve adequate therapeutic attributes, and present some considerations for their development in oncology.</p>
The post <a href="https://bibliography.nanobiotix.com/2015-metals-as-radio-enhancers-in-oncology-pottier-et-al/">2015 – Metals as radio-enhancers in oncology – Pottier et al.</a> first appeared on <a href="https://bibliography.nanobiotix.com">Nano Publications</a>.]]></description>
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            </div><div class="az-box-icon-content az-font-custom az-font-color-custom" style="color: #ffffff;"><h3 class="az-box-icon-title">Authors</h3><p>Agnès Pottier<span class="notes up">1</span>, Elsa Borghi<span class="notes up">1</span>, Laurent Levy<span class="notes up">1</span><br />
<span class="notes">1 – Nanobiotix, Paris, France</span></p>
<p>0006-291X/© 2015 Published by Elsevier Inc.<br />
<a href="https://dx.doi.org/10.1016/j.bbrc.2015.09.027" target="_blank" rel="noopener noreferrer">https://dx.doi.org/10.1016/j.bbrc.2015.09.027<br />
</a><a href="https://www.sciencedirect.com/science/journal/0006291X" target="_blank" rel="noopener noreferrer">https://www.sciencedirect.com/science/journal/0006291X</a></p>
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<div class="az-content-element-wrapper az-empty-divider hidden-lg hidden-md" style="height: 60px;"></div></div></div></div><div data-animation-type="ani-in" data-animation-in="fadeInUp" data-animation-out="none" data-animation-speed="default" data-animation-delay="300" data-offset-down="90" data-offset-up="none" class="single-clms col-md-6 az-main-col-content az-module az-col-pos-middle az-v-space-clm animate-content az-module-bg-color"><div class="az-col az-clm-padding-105" >
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            </div><div class="az-box-icon-content"><h3 class="az-box-icon-title">Summary</h3><p>Radio-enhancers, metal-based nanosized agents, could play a key role in oncology. They may unlock the potential of radiotherapy by enhancing the radiation dose deposit within tumors when the ionizing radiation source is ‘on’, while exhibiting chemically inert behavior in cellular and subcellular systems when the radiation beam is ‘off’. Important decision points support the development of these new type of therapeutic agents originated from nanotechnology. Here, we discuss from an industry perspective, the interest of developing radio-enhancer agents to improve tumor control, the relevance of nanotechnology to achieve adequate therapeutic attributes, and present some considerations for their development in oncology.</p>
</div></div>
</div>
<div class="az-content-element-wrapper az-empty-divider hidden-lg hidden-md" style="height: 60px;"></div></div></div></div></div></div></div></div></div></div></div>The post <a href="https://bibliography.nanobiotix.com/2015-metals-as-radio-enhancers-in-oncology-pottier-et-al/">2015 – Metals as radio-enhancers in oncology – Pottier et al.</a> first appeared on <a href="https://bibliography.nanobiotix.com">Nano Publications</a>.]]></content:encoded>
					
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		<title>2014 &#8211; Metals as Nanosized Radioenhancers &#8211; Pottier et al.</title>
		<link>https://bibliography.nanobiotix.com/2014-metals-as-nanosized-radioenhancers-pottier-et-al/</link>
					<comments>https://bibliography.nanobiotix.com/2014-metals-as-nanosized-radioenhancers-pottier-et-al/#respond</comments>
		
		<dc:creator><![CDATA[nano-pub]]></dc:creator>
		<pubDate>Mon, 06 Feb 2017 11:19:46 +0000</pubDate>
				<category><![CDATA[Clinical Data NBTXR3]]></category>
		<category><![CDATA[Head & Neck]]></category>
		<category><![CDATA[NO-RIGHTS]]></category>
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		<category><![CDATA[Chemotherapy]]></category>
		<category><![CDATA[Cisplatin]]></category>
		<category><![CDATA[Metal]]></category>
		<category><![CDATA[Physicochemical]]></category>
		<category><![CDATA[Shape]]></category>
		<category><![CDATA[Soft Tissue Sarcoma]]></category>
		<category><![CDATA[Therapeutic]]></category>
		<guid isPermaLink="false">http://localhost:8888/nano-publications/?p=108</guid>

					<description><![CDATA[<p>Since the discovery of cisplatin about 40 years ago, the design of innovative metal-based anticancer drugs is a growing area of research. Transition metal coordination complexes offer potential advantages over the more common organic-based drugs, including a wide range of coordination number and geometries, accessible redox states, tunability of the thermodynamics and kinetics of ligand substitution, as well as a wide structural diversity. Metal-based substances interact with cell molecular targets, affecting biochemical functions resulting in cancer cell destruction. Radionuclides are another way to use metals as anticancer therapy.</p>
The post <a href="https://bibliography.nanobiotix.com/2014-metals-as-nanosized-radioenhancers-pottier-et-al/">2014 – Metals as Nanosized Radioenhancers – Pottier et al.</a> first appeared on <a href="https://bibliography.nanobiotix.com">Nano Publications</a>.]]></description>
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        <div class="az-module-wrap-bg">
            <div class="az-module-wrapper-bg  az-imagesLoadedBg" style="background-image: url(https://bibliography.nanobiotix.com/wp-content/uploads/2017/02/Working-it.jpg); background-position: center center; background-repeat: no-repeat; background-size: cover;">
            
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            </div><div class="az-box-icon-content az-font-custom az-font-color-custom" style="color: #ffffff;"><h3 class="az-box-icon-title">Authors</h3><p>Agnes Pottier, Elsa Borghi, Laurent Levy<br />
<span class="notes">Nanobiotix, 60 rue de wattignies, 75012 Paris, France</span></p>
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            <div class="az-icon-container" style="color: #28282e; font-size: 50px;"><i class="az-icon az-icon-layers2"></i>
            </div><div class="az-box-icon-content"><h3 class="az-box-icon-title">Summary</h3><p>Since the discovery of cisplatin about 40 years ago, the design of innovative metal-based anticancer drugs is a growing area of research. Transition metal coordination complexes offer potential advantages over the more common organic-based drugs, including a wide range of coordination number and geometries, accessible redox states, tunability of the thermodynamics and kinetics of ligand substitution, as well as a wide structural diversity. Metal-based substances interact with cell molecular targets, affecting biochemical functions resulting in cancer cell destruction. Radionuclides are another way to use metals as anticancer therapy. The metal nucleus of the unstable radionuclide becomes stable by emitting energy. The biological effect in different tissues is obtained by the absorption of this energy from the radiation emitted by the radionuclide, the principal target generally agreed for ionizing radiations being DNA.</p>
<p>A new area of clinical research is now emerging using the same experimental metal elements, but in a radically different manner: metals and metal oxides used as crystalline nanosized particles. In this field, man-made functionalized nanoparticles of high electron density and well-defined size and shape offer the possibility of entering cancer cells and depositing high amounts of energy in the tumor only when exposed to ionizing radiations (on/off activity). These nanoparticles, such as hafnium oxide engineered as 50 nmsized spheres, functionalized with a negative surface (NBTXR3 nanoparticles), have been developed as selective radioenhancers, which represents a breakthrough approach for the local treatment of solid tumors. The properties of NBTXR3 nanoparticles, their chemistry, size, shape and surface charge, have been designed for efficient tumor cell uptake. NBTXR3 brings a physical mode of action, that of radiotherapy, within the cancer cells themselves. Physicochemical characteristics of NBTXR3 have demonstrated a very promising benefit-risk ratio for human healthcare across a broad non-clinical program. NBTXR3 has entered clinical development in therapy of advanced soft tissue sarcomas and head and neck cancer.</p>
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<div class="az-content-element-wrapper az-empty-divider hidden-lg hidden-md" style="height: 60px;"></div></div></div></div></div></div></div></div></div></div></div>The post <a href="https://bibliography.nanobiotix.com/2014-metals-as-nanosized-radioenhancers-pottier-et-al/">2014 – Metals as Nanosized Radioenhancers – Pottier et al.</a> first appeared on <a href="https://bibliography.nanobiotix.com">Nano Publications</a>.]]></content:encoded>
					
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		<title>2011 &#8211; AACR Abstract &#8211; NBTXR3 radioenhancement and anti-tumor effect in vitro &#8211; Magiorella et al.</title>
		<link>https://bibliography.nanobiotix.com/2011-aacr-abstract-nbtxr3-radioenhancement-and-anti-tumor-effect-in-vitro-magiorella-et-al/</link>
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		<dc:creator><![CDATA[nano-pub]]></dc:creator>
		<pubDate>Tue, 07 Feb 2017 16:56:54 +0000</pubDate>
				<category><![CDATA[Congress Abstracts]]></category>
		<category><![CDATA[In Vitro]]></category>
		<category><![CDATA[In Vitro in Vivo NBTXR3]]></category>
		<category><![CDATA[Clinical]]></category>
		<category><![CDATA[Enhancement]]></category>
		<category><![CDATA[Hafnium]]></category>
		<category><![CDATA[Ionizing]]></category>
		<category><![CDATA[Local]]></category>
		<category><![CDATA[Oxide]]></category>
		<category><![CDATA[Radiation]]></category>
		<category><![CDATA[Therapeutic]]></category>
		<category><![CDATA[Tumor]]></category>
		<guid isPermaLink="false">http://localhost:8888/nano-publications/?p=210</guid>

					<description><![CDATA[<p>Local and systemic control of Soft Tissue Sarcoma (STS) remains a clinical challenge. Radiation therapy is part of the standard of care of STS. The narrowness of its therapeutic window represents the main concern for different clinical settings. Thus, local delivery of radiation doses is critical to ensure optimal benefit-risk ratio. NBTXR3, biocompatible hafnium oxide nanoparticles were designed as therapeutics to be activated by ionizing radiation to achieve tumor control by enhancement of local energy deposition.</p>
The post <a href="https://bibliography.nanobiotix.com/2011-aacr-abstract-nbtxr3-radioenhancement-and-anti-tumor-effect-in-vitro-magiorella-et-al/">2011 – AACR Abstract – NBTXR3 radioenhancement and anti-tumor effect in vitro – Magiorella et al.</a> first appeared on <a href="https://bibliography.nanobiotix.com">Nano Publications</a>.]]></description>
										<content:encoded><![CDATA[<div class="az-main-section-content az-module az-padding-top-0 az-padding-bottom-0 az-section-default az-section-with-equal no-animate-content az-module-bg-color">
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            </div><div class="az-box-icon-content az-font-custom az-font-color-custom" style="color: #ffffff;"><h3 class="az-box-icon-title">Authors</h3><p>Maggiorella Laurence<span class="notes up">1</span>, Darmon Audrey<span class="notes up">1</span>, Sonia Vivet<span class="notes up">1</span>, Zhang Ping<span class="notes up">1</span>, Polrot Melanie<span class="notes up">2</span>, Deutsch Eric<span class="notes up">3</span>, Bourhis Jean<span class="notes up">3</span>, Pottier Agnes<span class="notes up">1</span>, Borghi Elsa<span class="notes up">1</span>, Levy Laurent<span class="notes up">1</span><br />
<span class="notes">1 – Nanobiotix, 60 rue de Wattignies 75012 Paris<br />
2 – Institut Gustave Roussy, IRCV, 114 rue Edouard Vaillant, 94805 Villejuif Cedex<br />
3 – Institut Gustave Roussy, Laboratoire UPRES EA 27-10, Radiosensibilité des tumeurs et tissus sains,<br />
114 rue Edouard Vaillant, 94805 Villejuif Cedex</span></p>
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<div class="az-content-element-wrapper az-empty-divider hidden-lg hidden-md" style="height: 60px;"></div></div></div></div><div data-animation-type="ani-in" data-animation-in="fadeInUp" data-animation-out="none" data-animation-speed="default" data-animation-delay="300" data-offset-down="90" data-offset-up="none" class="single-clms col-md-6 az-main-col-content az-module az-col-pos-middle az-v-space-clm animate-content az-module-bg-color"><div class="az-col az-clm-padding-105" >
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            </div><div class="az-box-icon-content"><h3 class="az-box-icon-title">Summary</h3><p><strong>Full Title: </strong>NBTXR3 hafnium oxide nanoparticle activated by ionizing radiation demonstrates marked radioenhancement and antitumor effect via high energy deposit in human soft tissue sarcoma</p>
<p><strong>Content:</strong> Local and systemic control of Soft Tissue Sarcoma (STS) remains a clinical challenge. Radiation therapy is part of the standard of care of STS. The narrowness of its therapeutic window represents the main concern for different clinical settings. Thus, local delivery of radiation doses is critical to ensure optimal benefit-risk ratio. NBTXR3, biocompatible hafnium oxide nanoparticles were designed as therapeutics to be activated by ionizing radiation to achieve tumor control by enhancement of local energy deposition.</p>
</div></div>
</div>
<div class="az-content-element-wrapper az-empty-divider hidden-lg hidden-md" style="height: 60px;"></div></div></div></div></div></div></div></div></div></div></div>The post <a href="https://bibliography.nanobiotix.com/2011-aacr-abstract-nbtxr3-radioenhancement-and-anti-tumor-effect-in-vitro-magiorella-et-al/">2011 – AACR Abstract – NBTXR3 radioenhancement and anti-tumor effect in vitro – Magiorella et al.</a> first appeared on <a href="https://bibliography.nanobiotix.com">Nano Publications</a>.]]></content:encoded>
					
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		<title>2010 &#8211; Combinations of proteins with Nano-Systems &#8211; Di Marco et al.</title>
		<link>https://bibliography.nanobiotix.com/2010-combinations-of-proteins-with-nano-systems-di-marco-et-al/</link>
					<comments>https://bibliography.nanobiotix.com/2010-combinations-of-proteins-with-nano-systems-di-marco-et-al/#respond</comments>
		
		<dc:creator><![CDATA[nano-pub]]></dc:creator>
		<pubDate>Mon, 06 Feb 2017 12:30:17 +0000</pubDate>
				<category><![CDATA[Miscellaneous]]></category>
		<category><![CDATA[NO-RIGHTS]]></category>
		<category><![CDATA[Publications]]></category>
		<category><![CDATA[Biomolecules]]></category>
		<category><![CDATA[Chemotherapeutic]]></category>
		<category><![CDATA[Delivery]]></category>
		<category><![CDATA[Design]]></category>
		<category><![CDATA[Drug]]></category>
		<category><![CDATA[Encapsulate]]></category>
		<category><![CDATA[Pharmacokinetics]]></category>
		<category><![CDATA[Protein]]></category>
		<category><![CDATA[Therapeutic]]></category>
		<category><![CDATA[Versatile]]></category>
		<guid isPermaLink="false">http://localhost:8888/nano-publications/?p=132</guid>

					<description><![CDATA[<p>The latest development of protein engineering allows the production of proteins having desired properties and large potential markets, but the clinical advances of therapeutical proteins are still limited by their fragility. Nanotechnology could provide optimal vectors able to protect from degradation therapeutical biomolecules such as proteins, enzymes or specific polypeptides.</p>
The post <a href="https://bibliography.nanobiotix.com/2010-combinations-of-proteins-with-nano-systems-di-marco-et-al/">2010 – Combinations of proteins with Nano-Systems – Di Marco et al.</a> first appeared on <a href="https://bibliography.nanobiotix.com">Nano Publications</a>.]]></description>
										<content:encoded><![CDATA[<div class="az-main-section-content az-module az-padding-top-0 az-padding-bottom-0 az-section-default az-section-with-equal no-animate-content az-module-bg-color">
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            </div><div class="az-box-icon-content az-font-custom az-font-color-custom" style="color: #ffffff;"><h3 class="az-box-icon-title">Authors</h3><p>Mariagrazia Di Marco<span class="notes up">1</span>, Shaharum Shamsuddin<span class="notes up">2</span>, Khairunisak Abdul Razak<span class="notes up">3</span>, Azlan Abdul Aziz<span class="notes up">4</span>, Corinne Devaux<span class="notes up">1</span>, Elsa Borghi<span class="notes up">1</span>, Laurent Levy<span class="notes up">1</span>, Claudia Sadun<span class="notes up">5</span><br />
<span class="notes">1 – Nanobiotix, Paris, France<br />
2 – School of Health Sciences, Health Campus Universiti Sains Malaysia, Kelantan, Malaysia<br />
3 – School of Materials and Mineral Resources Engineering, Engineering Campus<br />
4 – School of Physics, Universiti Sains Malaysia, Penang, Malaysia<br />
5 – Department of Chemistry, Sapienza, University of Rome, Rome, Italy</span></p>
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            </div><div class="az-box-icon-content"><h3 class="az-box-icon-title">Summary</h3><p><strong>Abstract:</strong> The latest development of protein engineering allows the production of proteins having desired properties and large potential markets, but the clinical advances of therapeutical proteins are still limited by their fragility. Nanotechnology could provide optimal vectors able to protect from degradation therapeutical biomolecules such as proteins, enzymes or specific polypeptides.</p>
<p>On the other hand, some proteins can be also used as active ligands to help nanoparticles loaded with chemotherapeutic or other drugs to reach particular sites in the body. The aim of this review is to provide an overall picture of the general aspects of the most successful approaches used to combine proteins with nanosystems. This combination is mainly achieved by absorption, bioconjugation and encapsulation. Interactions of nanoparticles with biomolecules and caveats related to protein denaturation are also pointed out. A clear understanding of nanoparticle-protein interactions could make possible the design of precise and versatile hybrid nanosystems. This could further allow control of their pharmacokinetics as well as activity, and safety.</p>
<p><strong>Keywords:</strong> nanoparticles, drug delivery, proteins, polypeptides, absorption, bioconjugation, encapsulation</p>
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</div>
<div class="az-content-element-wrapper az-empty-divider hidden-lg hidden-md" style="height: 60px;"></div></div></div></div></div></div></div></div></div></div></div>The post <a href="https://bibliography.nanobiotix.com/2010-combinations-of-proteins-with-nano-systems-di-marco-et-al/">2010 – Combinations of proteins with Nano-Systems – Di Marco et al.</a> first appeared on <a href="https://bibliography.nanobiotix.com">Nano Publications</a>.]]></content:encoded>
					
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