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	<title>IMRT | Nano Publications</title>
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	<title>IMRT | Nano Publications</title>
	<link>https://bibliography.nanobiotix.com/fr/</link>
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	<item>
		<title>2020 – RT-activated hafnium oxide nanoparticles in cisplatin-ineligible locally advanced HNSCC patients</title>
		<link>https://bibliography.nanobiotix.com/fr/2020-rt-activated-hafnium-oxide-nanoparticles-in-cisplatin-ineligible-locally-advanced-hnscc-patients/</link>
		
		<dc:creator><![CDATA[nano-pub]]></dc:creator>
		<pubDate>Thu, 26 May 2022 14:30:38 +0000</pubDate>
				<category><![CDATA[Abstracts]]></category>
		<category><![CDATA[Donnée clinique de NBTXR3]]></category>
		<category><![CDATA[NO-RIGHTS]]></category>
		<category><![CDATA[Tête & Cou]]></category>
		<category><![CDATA[Dose]]></category>
		<category><![CDATA[Head & Neck]]></category>
		<category><![CDATA[IMRT]]></category>
		<category><![CDATA[NBTXR3]]></category>
		<category><![CDATA[Radiotherapy]]></category>
		<category><![CDATA[Toxicity]]></category>
		<guid isPermaLink="false">https://bibliography.nanobiotix.com/?p=2740</guid>

					<description><![CDATA[<p>Elderly and frail patients (pts) with head and neck squamous cell carcinoma (HSNCC) remain a challenging population to manage due to the lack of evidence-based recommendations. Despite representing approximately 20% of the HNSCC population no consensus exists on the optimal treatment for these pts with locally advanced (LA) disease […]</p>
The post <a href="https://bibliography.nanobiotix.com/fr/2020-rt-activated-hafnium-oxide-nanoparticles-in-cisplatin-ineligible-locally-advanced-hnscc-patients/">2020 – RT-activated hafnium oxide nanoparticles in cisplatin-ineligible locally advanced HNSCC patients</a> first appeared on <a href="https://bibliography.nanobiotix.com/fr/">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>C. Le Tourneau , V. Calugaru, E. Borcoman, V. Moreno, E. Calvo, X. Liem, S. Salas, B. Doger, T. Jouffroy, X. Mirabel, J. Rodriguez, A. Chilles, K. Bernois, M. De Rink, N. Fafhry, S. Wong Hee Kam, C. Hoffmann</p>
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            </div><div class="az-box-icon-content"><h3 class="az-box-icon-title">Summary</h3><p><b>Purpose/Objective:</b> Elderly and frail patients (pts) with head and neck squamous cell carcinoma (HSNCC) remain a challenging population to manage due to the lack of evidence-based recommendations. Despite representing approximately 20% of the HNSCC population no consensus exists on the optimal treatment for these pts with locally advanced (LA) disease, vulnerable to current standard of care treatment-induced toxicities. New approaches are thus needed to improve clinical outcomes without adding toxicity. NBTXR3 hafnium oxide nanoparticles injected intratumorally may represent such an option. Otherwise inert, this first-in-class radioenhancer augments the radiotherapy (RT) dose within tumor cells when activated by RT, increasing tumor cell death compared to RT alone. The results presented here demonstrate the feasibility and safety of NBTXR3 activated by RT in elderly patients, a population with few therapeutic options.</p>
<p><b>Material/Methods:</b> Patients with Stage III-IV LA HNSCC of the oropharynx or oral cavity ineligible for platinum-based chemoradiation received a single intratumoral injection of NBTXR3 and intensity modulated radiation therapy (IMRT; 70 Gy/35 fractions/7 weeks). This is a 3+3 design dose escalation study to test NBTXR3 dose levels equivalent to 5, 10, 15, and 22% of baseline theoretical tumor volume, followed by a dose expansion. Primary endpoints include Recommended Phase 2 Dose (RP2D) determination and early dose limiting toxicities (DLT). NBTXR3 presence in surrounding healthy tissues and anti-tumor activity (RECIST 1.1) were also evaluated.</p>
<p><b>Results:</b> Enrollment was completed at all dose levels: 5% (3 pts), 10% (3 pts), 15% (5 pts), and 22% (8 pts). No early DLT or SAE related to NBTXR3 or injection were observed. One G1 AE (asthenia; 22%) related to NBTXR3 and four AEs (G2 oral pain, G1 tumor hemorrhage, asthenia, and injection site hemorrhage) related to injection were observed. RT-related toxicity was as expected with IMRT. The RP2D was determined to be 22% by the DSMB. CT-scan assessment demonstrated localization of NBTXR3 intratumorally without presence in surrounding healthy tissues. At a median follow-up of 231 days, 9/13 (2 unconfirmed) evaluable pts receiving doses ≥10%, achieved a complete response of the treated tumors. The final dose escalation safety and efficacy results will be presented herein.</p>
<p><b>Conclusion:</b> NBTXR3 was well tolerated at all tested doses and demonstrated preliminary anti-tumor activity. The dose expansion part at the RP2D is ongoing. These results highlight the potential of NBTXR3 as a novel treatment option for elderly pts with LA HNSCC and address an unmet medical need.</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/fr/2020-rt-activated-hafnium-oxide-nanoparticles-in-cisplatin-ineligible-locally-advanced-hnscc-patients/">2020 – RT-activated hafnium oxide nanoparticles in cisplatin-ineligible locally advanced HNSCC patients</a> first appeared on <a href="https://bibliography.nanobiotix.com/fr/">Nano Publications</a>.]]></content:encoded>
					
		
		
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		<title>2019 – NBTXR3 for the treatment of locally advanced HNSCC in frail and/or elderly patients: a phase I/II study</title>
		<link>https://bibliography.nanobiotix.com/fr/2019-nbtxr3-for-the-treatment-of-locally-advanced-hnscc-in-frail-and-or-elderly-patients-a-phase-i-ii-study/</link>
		
		<dc:creator><![CDATA[nano-pub]]></dc:creator>
		<pubDate>Thu, 26 May 2022 08:26:57 +0000</pubDate>
				<category><![CDATA[Abstracts]]></category>
		<category><![CDATA[Donnée clinique de NBTXR3]]></category>
		<category><![CDATA[Tête & Cou]]></category>
		<category><![CDATA[Dose]]></category>
		<category><![CDATA[Elderly]]></category>
		<category><![CDATA[Frail]]></category>
		<category><![CDATA[Head & Neck]]></category>
		<category><![CDATA[IMRT]]></category>
		<category><![CDATA[Radiotherapy]]></category>
		<guid isPermaLink="false">https://bibliography.nanobiotix.com/?p=2645</guid>

					<description><![CDATA[<p>Elderly head and neck squamous cell carcinoma (HSNCC) patients (pts) ineligible for standard of care treatment require new therapeutic approaches. NBTXR3, hafnium oxide nanoparticles, may represent such an option. NBTXR3 is activated by radiotherapy, enhancing its effects, leading to physical destruction of cancer cells. […]</p>
The post <a href="https://bibliography.nanobiotix.com/fr/2019-nbtxr3-for-the-treatment-of-locally-advanced-hnscc-in-frail-and-or-elderly-patients-a-phase-i-ii-study/">2019 – NBTXR3 for the treatment of locally advanced HNSCC in frail and/or elderly patients: a phase I/II study</a> first appeared on <a href="https://bibliography.nanobiotix.com/fr/">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>Le Tourneau<span class="notes up">1</span>, V. Calugaru<span class="notes up">1</span>, V. Moreno Garcia<span class="notes up">2</span>, X. Mirabel<span class="notes up">3</span>, B. Doger<span class="notes up">2</span>, E. Calvo<span class="notes up">2</span>, J. Fijuth<span class="notes up">4</span>, T. Rutkowski<span class="notes up">5</span>, N. Magne<span class="notes up">6</span>, M. Sanz Taberna<span class="notes up">7</span>, J. Contreras<span class="notes up">8</span>, I. Brana Garcia<span class="notes up">9</span>, Z. Papai1<span class="notes up">0</span>, Z. Takacsi-Nagy1<span class="notes up">1</span>, X. Liem<span class="notes up">3</span>, S. Salas1<span class="notes up">2</span>, S. Wong Hee Kam1<span class="notes up">3</span>, C. Florescu1<span class="notes up">4</span>, J.O. Thariat1<span class="notes up">5</span>, and C. Hoffmann<span class="notes up">1</span><br />
<span class="notes"><br />
1 — Institut Curie, Paris, France<br />
2 — START Madrid, Madrid, Spain<br />
3 — Centre Oscar Lambret, Lille, France<br />
4 — Provita Prolife, Tomaszow Mazowiecki, Poland<br />
5 — Skłodowska-Curie Institute of Oncology, Gliwice, Poland<br />
6 — Lucien Neuwirth Cancer Institute, Saint Priest en Jarez, France<br />
7 — Institut Catala d’Oncologia (ICO L’Hospitalet) Hospital Duran i Reynals, Barcelona, Spain<br />
8 — Hospital Universitario Regional de Malaga, Malaga, Spain<br />
9 — Vall D’Hebron Institute of Oncology, Barcelona, Spain<br />
10 — Magyar Honvedseg Egeszsegugyi Kozpont, Budapest, Hungary<br />
11 — National Institute of Oncology, Budapest, Hungary<br />
12 — Assistance Publique Hôpitaux de Marseille, Timone Hospital, Marseille, France<br />
13 — Hôpital Timone, APHM, Marseille, France<br />
14 — Unicancer &#8211; François Baclesse Center, Caen, France<br />
15 — Centre François Baclesse, Caen, France<br />
</span></p>
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            </div><div class="az-box-icon-content"><h3 class="az-box-icon-title">Summary</h3><p><b>Purpose:</b> Elderly head and neck squamous cell carcinoma (HSNCC) patients (pts) ineligible for standard of care treatment require new therapeutic approaches. NBTXR3, hafnium oxide nanoparticles, may represent such an option. NBTXR3 is activated by radiotherapy, enhancing its effects, leading to physical destruction of cancer cells. A Phase I/II trial [NCT01946867] is underway to evaluate NBTXR3 in elderly (≥70 years) or frail pts with HNSCC of the oral cavity and oropharynx ineligible for cisplatin or intolerant to cetuximab.<br />
Method and materials: Pts received a single intratumoral injection of NBTXR3 and intensity modulated radiation therapy (IMRT; 70 Gy/35 fractions/7 weeks). The study was a 3 + 3 dose escalation to test the NBTXR3 dose equivalent to 5, 10, 15, and 22% of baseline tumor volume, followed by a dose expansion. Primary endpoints include Recommended Phase 2 Dose (RP2D) determination and early dose limiting toxicities (DLT). Presence of NBTXR3 in surrounding healthy tissues and efficacy (RECIST 1.1 principles) were also evaluated.</p>
<p><b>Results:</b> Enrollment for the dose escalation phase was completed at all dose levels: 5% (3 pts), 10% (3 pts), 15% (5 pts), and 22% (8 pts). No early DLT or SAE related to NBTXR3 or injection were observed. One G1 AE (asthenia; 22%) related to NBTXR3 and four AEs (G2 oral pain, G1 tumor hemorrhage, G1 asthenia, and G1 injection site hemorrhage) related to injection were reported. RT-related toxicity was as expected. The RP2D has been determined to be 22%. CT-scan assessment demonstrated absence of NBTXR3 in surrounding tissues. Among 13 evaluable pts treated at doses ≥10%, 9 achieved complete response of the injected lesion. The final dose escalation safety results will be presented herein.</p>
<p><b>Conclusion:</b> NBTXR3 was well tolerated at all tested doses and demonstrated a good safety profile. A dose expansion phase has started with the identified RP2D.<br />
NBTXR3 is currently being evaluated in a phase II/III trial in soft tissue sarcoma [NCT02379845] and phase I/II trials in prostate [NCT02805894], liver [NCT02721056] and rectal [NCT02465593] cancers.</p>
<p><b>Clinical relevance:</b> The results of this study highlight the potential of NBTXR3 as a novel treatment option for elderly and/or frail pts with locally advanced HNSCC and address an unmet medical need.</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/fr/2019-nbtxr3-for-the-treatment-of-locally-advanced-hnscc-in-frail-and-or-elderly-patients-a-phase-i-ii-study/">2019 – NBTXR3 for the treatment of locally advanced HNSCC in frail and/or elderly patients: a phase I/II study</a> first appeared on <a href="https://bibliography.nanobiotix.com/fr/">Nano Publications</a>.]]></content:encoded>
					
		
		
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		<title>2019 – Phase I study of hafnium oxide nanoparticles activated by Intensity Modulated Radiation Therapy (IMRT) as a new therapeutic option for elderly or frail HNSCC patients</title>
		<link>https://bibliography.nanobiotix.com/fr/2019-phase-i-study-of-hafnium-oxide-nanoparticles-activated-by-intensity-modulated-radiation-therapy-imrt-as-a-new-therapeutic-option-for-elderly-or-frail-hnscc-patients/</link>
		
		<dc:creator><![CDATA[nano-pub]]></dc:creator>
		<pubDate>Thu, 26 May 2022 07:57:53 +0000</pubDate>
				<category><![CDATA[Abstracts]]></category>
		<category><![CDATA[Donnée clinique de NBTXR3]]></category>
		<category><![CDATA[NO-RIGHTS]]></category>
		<category><![CDATA[Tête & Cou]]></category>
		<category><![CDATA[Elderly]]></category>
		<category><![CDATA[Frail]]></category>
		<category><![CDATA[Head & Neck]]></category>
		<category><![CDATA[IMRT]]></category>
		<category><![CDATA[NBTXR3]]></category>
		<category><![CDATA[Radiotherapy]]></category>
		<category><![CDATA[RP2D]]></category>
		<guid isPermaLink="false">https://bibliography.nanobiotix.com/?p=2639</guid>

					<description><![CDATA[<p>New therapeutic approaches are needed for elderly or frail head and neck squamous cell carcinoma (HNSCC) patients (pts) ineligible for standard of care. NBTXR3, hafnium oxide nanoparticles injected intratumorally, may represent an option. Otherwise inert, NBTXR3 augments the radiation therapy (RT) dose within tumor cells when activated by RT, increasing tumor cell death compared to RT alone. […]</p>
The post <a href="https://bibliography.nanobiotix.com/fr/2019-phase-i-study-of-hafnium-oxide-nanoparticles-activated-by-intensity-modulated-radiation-therapy-imrt-as-a-new-therapeutic-option-for-elderly-or-frail-hnscc-patients/">2019 – Phase I study of hafnium oxide nanoparticles activated by Intensity Modulated Radiation Therapy (IMRT) as a new therapeutic option for elderly or frail HNSCC patients</a> first appeared on <a href="https://bibliography.nanobiotix.com/fr/">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>C. Le Tourneau, V.Moreno Garcia, B. Doger, A. Urban, K. Bernois, X. Liem, S. Salas, S. Wong, N. Fakhry, M. Dimitriu, V. Calugaru, C. Hoffmann</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><b>Introduction:</b> New therapeutic approaches are needed for elderly or frail head and neck squamous cell carcinoma (HNSCC) patients (pts) ineligible for standard of care. NBTXR3, hafnium oxide nanoparticles injected intratumorally, may represent an option. Otherwise inert, NBTXR3 augments the radiation therapy (RT) dose within tumor cells when activated by RT, increasing tumor cell death compared to RT alone.</p>
<p><b>Objectives:</b> The purpose of this Phase I was to evaluate safety (dose limiting toxicity; DLT) and determine the NBTXR3 recommended phase 2 dose (RP2D) in elderly or frail HNSCC pts.</p>
<p><b>Methods:</b> Eligible pts had stage III or IV HNSCC of oral cavity or oropharynx, were aged ≥70 years or ≥65 years and unable to receive cisplatin but eligible for RT [NCT01946867]. A 3+3 dose escalation design was employed, with NBTRX3 dose levels of 5%, 10%, 15% and 22% of baseline tumor volume. Following intratumoral NBTXR3 injection, pts received IMRT (70 Gy; 35 fractions/7 weeks). Primary endpoints were RP2D and DLT. Localization of NBTXR3 and preliminary efficacy (RECIST 1.1) were also evaluated.</p>
<p><b>Results and Conclusion:</b> Dose escalation is complete; 19 pts received NBTXR3: 3 at 5%, 3 at 10%, 5 at 15% and 8 at 22%. No NBTXR3-related DLTs or SAEs were observed. Four related AEs were reported: one AE at 15% (G1 tumor hemorrhage) and 3 AEs at 22% (G2 oral pain; G1 asthenia, G1 injection site hemorrhage). IMRT toxicity was as expected and post-injection CT scan showed NBTXR3 localized within the injected tumor. DSMB determined RP2D to be 22%. Among 13 evaluable pts at doses ≥10%, 9 had a complete response of injected tumor. Results demonstrate that NBTXR3 activated by RT is a well-tolerated therapy with encouraging anti-tumor activity. RP2D expansion is ongoing. NBTXR3 may be an option for elderly or frail pts with locally advanced HNSCC.</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/fr/2019-phase-i-study-of-hafnium-oxide-nanoparticles-activated-by-intensity-modulated-radiation-therapy-imrt-as-a-new-therapeutic-option-for-elderly-or-frail-hnscc-patients/">2019 – Phase I study of hafnium oxide nanoparticles activated by Intensity Modulated Radiation Therapy (IMRT) as a new therapeutic option for elderly or frail HNSCC patients</a> first appeared on <a href="https://bibliography.nanobiotix.com/fr/">Nano Publications</a>.]]></content:encoded>
					
		
		
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		<title>2019 – ESMO IO – NBTXR3 with anti-PD-1</title>
		<link>https://bibliography.nanobiotix.com/fr/2019-esmo-io-nbtxr3-with-anti-pd-1/</link>
					<comments>https://bibliography.nanobiotix.com/fr/2019-esmo-io-nbtxr3-with-anti-pd-1/#respond</comments>
		
		<dc:creator><![CDATA[nano-pub]]></dc:creator>
		<pubDate>Tue, 25 Feb 2020 15:22:38 +0000</pubDate>
				<category><![CDATA[Abstracts]]></category>
		<category><![CDATA[Donnée clinique de NBTXR3]]></category>
		<category><![CDATA[Foie]]></category>
		<category><![CDATA[Poumon]]></category>
		<category><![CDATA[Tête & Cou]]></category>
		<category><![CDATA[Abscopal Effect]]></category>
		<category><![CDATA[Anti-PD-1]]></category>
		<category><![CDATA[Biomarkers]]></category>
		<category><![CDATA[Checkpoint Inhibitor]]></category>
		<category><![CDATA[Hafnium Oxide]]></category>
		<category><![CDATA[Head and Neck Squamous Cell Carcinoma]]></category>
		<category><![CDATA[HNSCC]]></category>
		<category><![CDATA[Immunotherapy]]></category>
		<category><![CDATA[IMRT]]></category>
		<category><![CDATA[IO]]></category>
		<category><![CDATA[liver metastasis]]></category>
		<category><![CDATA[lung metastases]]></category>
		<category><![CDATA[Nanoparticle]]></category>
		<category><![CDATA[NBTXR3]]></category>
		<category><![CDATA[Radiation Therapy]]></category>
		<category><![CDATA[Radiotherapy]]></category>
		<guid isPermaLink="false">https://bibliography.nanobiotix.com/?p=2107</guid>

					<description><![CDATA[<p>The majority of cancer patients are resistant to immune therapy; only around 15% respond to immune checkpoint inhibitors (ICI). Thus, strategies able to increase ICI response are of great interest. Recent work suggests radiotherapy (RT) can act as an immunomodulator to increase the proportion of ICI responders and improve clinical outcomes. However, RT dose and ultimate efficacy are limited by toxicity related to exposure of healthy tissues.  […]</p>
The post <a href="https://bibliography.nanobiotix.com/fr/2019-esmo-io-nbtxr3-with-anti-pd-1/">2019 – ESMO IO – NBTXR3 with anti-PD-1</a> first appeared on <a href="https://bibliography.nanobiotix.com/fr/">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>Colette Shen<span class="notes up">1</span>, Katherine Jameson<span class="notes up">2</span>, Jared Weiss<span class="notes up">1</span>, Trevor Hackman<span class="notes up">1</span>, Daniel Corum<span class="notes up">2</span>, Jason A. Akulian<span class="notes up">1</span>, Robert Dixon<span class="notes up">1</span>, Alexander Pearson<span class="notes up">3</span>, Jessica Frakes<span class="notes up">4</span>, Patricia Said<span class="notes up">2</span>, Hichem Miraoui<span class="notes up">2</span>, Edwina Baskin-Bey<span class="notes up">2</span>, Tanguy Seiwert<span class="notes up">5</span><br />
<span class="notes"><br />
1 – University of North Carolina School of Medicine, Chapel Hill, North Carolina, USA<br />
2 – Nanobiotix, Paris, France<br />
3 – University of Chicago Medicine, Chicago, Illinois, USA<br />
4 – Moffitt Cancer Center, Tampa, Florida, USA<br />
5 – Johns Hopkins Medicine, Baltimore, Maryland, USA<br />
</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><strong>Background:</strong> The majority of cancer patients are resistant to immune therapy; only around 15% respond to immune checkpoint inhibitors (ICI). Thus, strategies able to increase ICI response are of great interest. Recent work suggests radiotherapy (RT) can act as an immunomodulator to increase the proportion of ICI responders and improve clinical outcomes. However, RT dose and ultimate efficacy are limited by toxicity related to exposure of healthy tissues. NBTXR3 is a first-in-class radioenhancer administered by intratumoral injection, designed at the nanoscale to increase RT energy dose deposition within the tumor. The result is increased radiation-dependent tumor cell killing, without increasing radiation exposure of healthy tissues. Preclinical and early clinical data suggest NBTXR3 activated by RT can increase the anti-tumor immune response, producing both local and systemic (abscopal) effects. We hypothesize that NBTXR3 activated by RT, in combination with anti-PD-1 therapy (R3/RT/PD-1), will act synergistically to maximize the local RT effect while also producing a systemic response sufficient to increase the proportion of ICI responders or convert ICI non-responders to responders.</p>
<p><strong>Trial Design:</strong> NANORAY-1100 [NCT03589339] is a multicenter, open-label, phase 1 study to evaluate safety and tolerability of R3/RT/PD-1 in three cohorts: (1) Locoregional recurrent or recurrent and metastatic head and neck squamous cell carcinoma (HNSCC) amenable to re-irradiation of the HN field, (2) Lung metastases from any primary cancer eligible for anti-PD-1, or (3) Liver metastases from any primary cancer eligible for anti-PD-1. Approximately two-thirds of each cohort will be composed of anti-PD-1 non-responders. NBTXR3 injection volume is based on a percentage of gross tumor volume (GTV) determined by central review. The primary objective is to determine R3/RT/PD-1 RP2D. Secondary objectives are to evaluate anti-tumor response (objective response rate; ORR) of R3/RT/PD-1, safety and feasibility of NBTXR3 injection, and NBTXR3 body kinetic profile. Exploratory objectives will assess biomarkers of R3/RT/PD-1 response, including PD-L1 status by IHC, mRNA and cytokine immune marker profiling.</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/fr/2019-esmo-io-nbtxr3-with-anti-pd-1/">2019 – ESMO IO – NBTXR3 with anti-PD-1</a> first appeared on <a href="https://bibliography.nanobiotix.com/fr/">Nano Publications</a>.]]></content:encoded>
					
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		<title>2019 – RSNA – Treatment of locally advanced HNSCC by NBTXR3</title>
		<link>https://bibliography.nanobiotix.com/fr/2019-rsna-treatment-of-locally-advanced-hnscc-by-nbtxr3/</link>
					<comments>https://bibliography.nanobiotix.com/fr/2019-rsna-treatment-of-locally-advanced-hnscc-by-nbtxr3/#respond</comments>
		
		<dc:creator><![CDATA[nano-pub]]></dc:creator>
		<pubDate>Fri, 06 Dec 2019 12:57:29 +0000</pubDate>
				<category><![CDATA[Abstracts]]></category>
		<category><![CDATA[Donnée clinique de NBTXR3]]></category>
		<category><![CDATA[Tête & Cou]]></category>
		<category><![CDATA[Dose]]></category>
		<category><![CDATA[Elderly]]></category>
		<category><![CDATA[Frail]]></category>
		<category><![CDATA[Hafnium Oxide]]></category>
		<category><![CDATA[Head and Neck Squamous Cell Carcinoma]]></category>
		<category><![CDATA[HNSCC]]></category>
		<category><![CDATA[IMRT]]></category>
		<category><![CDATA[Intensity Modulated]]></category>
		<category><![CDATA[Nanoparticle]]></category>
		<category><![CDATA[NBTXR3]]></category>
		<category><![CDATA[Oral Cavity]]></category>
		<category><![CDATA[Oropharynx]]></category>
		<category><![CDATA[Patients]]></category>
		<category><![CDATA[Phase II]]></category>
		<category><![CDATA[Radiation Therapy]]></category>
		<category><![CDATA[Radiotherapy]]></category>
		<category><![CDATA[Recommended]]></category>
		<category><![CDATA[RP2D]]></category>
		<guid isPermaLink="false">https://bibliography.nanobiotix.com/?p=2085</guid>

					<description><![CDATA[<p>Elderly head and neck squamous cell carcinoma (HSNCC) patients (pts) ineligible for standard of care treatment require new therapeutic approaches. NBTXR3, hafnium oxide nanoparticles, may represent such an option. NBTXR3 is activated by radiotherapy, enhancing its effects, leading to physical destruction of cancer cells. A Phase I/II trial [NCT01946867] is underway to evaluate NBTXR3 in elderly (≥70 years) or frail pts with HNSCC of the oral cavity and oropharynx ineligible for cisplatin or intolerant to cetuximab. […]</p>
The post <a href="https://bibliography.nanobiotix.com/fr/2019-rsna-treatment-of-locally-advanced-hnscc-by-nbtxr3/">2019 – RSNA – Treatment of locally advanced HNSCC by NBTXR3</a> first appeared on <a href="https://bibliography.nanobiotix.com/fr/">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>Christophe Le Tourneau<span class="notes up">1</span>, Valentin Calugaru<span class="notes up">1</span>, Victor Moreno Garcia<span class="notes up">2</span>, Xavier Mirabel<span class="notes up">3</span>, Bernard Doger<span class="notes up">2</span>, Emiliano Calvo<span class="notes up">2</span>, Jacek Fijuth<span class="notes up">4</span>, Tomasz Rutkowski<span class="notes up">5</span>, Nicolas Magné<span class="notes up">6</span>, Miren Sanz Taberna<span class="notes up">7</span>, Jorge Contreras<span class="notes up">8</span>, Irene Brana<span class="notes up">9</span>, Zsuzsanna Papai<span class="notes up">10</span>, Zoltán Takacsi-Nagy<span class="notes up">11</span>, Xavier Liem<span class="notes up">3</span>, Sébastien Salas<span class="notes up">12</span>, Stéphanie Wong<span class="notes up">12</span>, Carmen Florescu<span class="notes up">13</span>, Juliette Thariat<span class="notes up">13</span>, Caroline Hoffmann<span class="notes up">1</span><br />
<span class="notes"><br />
1 – Institut Curie, Paris, France<br />
2 – START Madrid, Madrid, Spain<br />
3 – Centre Oscar Lambret, Lille, France<br />
4 – Provita Prolife, Tomaszów Mazowiecki, Poland<br />
5 – Maria Skłodowska-Curie Institute of Oncology, Gliwice, Poland<br />
6 – Institut de Cancérologie Lucien Neuwirt, Saint-Priest-en-Jarez, France<br />
7 – Institut Catala d’Oncologia, Barcelona, Spain<br />
8 – University Regional Hospital of Malaga, Malaga, Spain<br />
9 – Vall d&rsquo;Hebron University Hospital, Bacelona, Spain<br />
10 – Hungarian Defense Forces Military Hospital, Budapest, Hungary<br />
11 – National Institute of Oncology, Budapest, Hungary<br />
12 – Hôpital Timone, APHM, Marseille<br />
13 – Unicancer &#8211; François Baclesse Center, Caen, France<br />
</span></p>
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            </div><div class="az-box-icon-content"><h3 class="az-box-icon-title">Summary</h3><p><strong>Purpose:</strong> Elderly head and neck squamous cell carcinoma (HSNCC) patients (pts) ineligible for standard of care treatment require new therapeutic approaches. NBTXR3, hafnium oxide nanoparticles, may represent such an option. NBTXR3 is activated by radiotherapy, enhancing its effects, leading to physical destruction of cancer cells. A Phase I/II trial [NCT01946867] is underway to evaluate NBTXR3 in elderly (≥70 years) or frail pts with HNSCC of the oral cavity and oropharynx ineligible for cisplatin or intolerant to cetuximab.</p>
<p><strong>Method &amp; Materials:</strong> Pts received a single intratumoral injection of NBTXR3 and intensity modulated radiation therapy (IMRT; 70 Gy/35 fractions/7 weeks). The study was a 3 + 3 dose escalation to test the NBTXR3 dose equivalent to 5, 10, 15, and 22% of baseline tumor volume, followed by a dose expansion. Primary endpoints include Recommended Phase 2 Dose (RP2D) determination and early dose limiting toxicities (DLT). Presence of NBTXR3 in surrounding healthy tissues and efficacy (RECIST 1.1 principles) were also evaluated.</p>
<p><strong>Results:</strong> Enrollment for the dose escalation phase was completed at all dose levels: 5% (3 pts), 10% (3 pts), 15% (5 pts), and 22% (8 pts). No early DLT or SAE related to NBTXR3 or injection were observed. One G1 AE (asthenia; 22%) related to NBTXR3 and four AEs (G2 oral pain, G1 tumor hemorrhage, G1 asthenia, and G1 injection site hemorrhage) related to injection were reported. RT-related toxicity was as expected. The RP2D has been determined to be 22%. CT-scan assessment demonstrated absence of NBTXR3 in surrounding tissues. Among 13 evaluable pts treated at doses ≥10%, 9 achieved complete response of the injected lesion. The final dose escalation safety results will be presented herein.</p>
<p><strong>Conclusion:</strong> NBTXR3 was well tolerated at all tested doses and demonstrated a good safety profile. A dose expansion phase has started with the identified RP2D. NBTXR3 is currently being evaluated in a phase II/III trial in soft tissue sarcoma [NCT02379845] and phase I/II trials in prostate [NCT02805894], liver [NCT02721056] and rectal [NCT02465593] cancers.</p>
<p><strong>Clinical Relevance &amp; Application:</strong> The results of this study highlight the potential of NBTXR3 as a novel treatment option for elderly and/or frail pts with locally advanced HNSCC and address an unmet medical need.</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/fr/2019-rsna-treatment-of-locally-advanced-hnscc-by-nbtxr3/">2019 – RSNA – Treatment of locally advanced HNSCC by NBTXR3</a> first appeared on <a href="https://bibliography.nanobiotix.com/fr/">Nano Publications</a>.]]></content:encoded>
					
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		<title>2019 – SIOG – NBTXR3 for the treatment of elderly/frail HNSCC patients</title>
		<link>https://bibliography.nanobiotix.com/fr/2019-siog-nbtxr3-for-the-treatment-of-elderly-frail-hnscc-patients/</link>
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		<dc:creator><![CDATA[nano-pub]]></dc:creator>
		<pubDate>Thu, 05 Dec 2019 07:51:40 +0000</pubDate>
				<category><![CDATA[Abstracts]]></category>
		<category><![CDATA[Donnée clinique de NBTXR3]]></category>
		<category><![CDATA[Tête & Cou]]></category>
		<category><![CDATA[Dose]]></category>
		<category><![CDATA[Elderly]]></category>
		<category><![CDATA[Frail]]></category>
		<category><![CDATA[Hafnium Oxide]]></category>
		<category><![CDATA[Head and Neck Squamous Cell Carcinoma]]></category>
		<category><![CDATA[HNSCC]]></category>
		<category><![CDATA[IMRT]]></category>
		<category><![CDATA[Intensity Modulated]]></category>
		<category><![CDATA[Nanoparticle]]></category>
		<category><![CDATA[NBTXR3]]></category>
		<category><![CDATA[Oral Cavity]]></category>
		<category><![CDATA[Oropharynx]]></category>
		<category><![CDATA[Patients]]></category>
		<category><![CDATA[Phase I]]></category>
		<category><![CDATA[Phase II]]></category>
		<category><![CDATA[Radiotherapy]]></category>
		<category><![CDATA[RP2D]]></category>
		<guid isPermaLink="false">https://bibliography.nanobiotix.com/?p=2054</guid>

					<description><![CDATA[<p>New therapeutic approaches are needed for elderly or frail head and neck squamous cell carcinoma (HNSCC) patients (pts) ineligible for standard of care. NBTXR3, hafnium oxide nanoparticles injected intratumorally, may represent an option. Otherwise inert, NBTXR3 augments the radiation therapy (RT) dose within tumor cells when activated by RT, increasing tumor cell death compared to RT alone. […]</p>
The post <a href="https://bibliography.nanobiotix.com/fr/2019-siog-nbtxr3-for-the-treatment-of-elderly-frail-hnscc-patients/">2019 – SIOG – NBTXR3 for the treatment of elderly/frail HNSCC patients</a> first appeared on <a href="https://bibliography.nanobiotix.com/fr/">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>Christophe Le Tourneau<span class="notes up">1</span>, Victor Moreno Garcia<span class="notes up">2</span>, Bernard Doger<span class="notes up">2</span>, Andrzej Urban<span class="notes up">3</span>, Katell Bernois<span class="notes up">3</span>, Xavier Liem<span class="notes up">4</span>, Sébastien Salas<span class="notes up">5</span>, Stéphanie Wong<span class="notes up">5</span>, Nicolas Fakhry<span class="notes up">5</span>, Mikaela Dimitriu<span class="notes up">3</span>, Valentin Calugaru<span class="notes up">1</span>, Caroline Hoffmann<span class="notes up">1</span><br />
<span class="notes"><br />
1 – Institut Curie, Paris, France<br />
2 – START Madrid, Madrid, Spain<br />
3 – Nanobiotix, SA ; Paris, France<br />
4 – Centre Oscar Lambret, Lille, France<br />
5 – Hôpital Timone, APHM, Marseille, France </p>
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            </div><div class="az-box-icon-content"><h3 class="az-box-icon-title">Summary</h3><p><strong>Introduction:</strong> New therapeutic approaches are needed for elderly or frail head and neck squamous cell carcinoma (HNSCC) patients (pts) ineligible for standard of care. NBTXR3, hafnium oxide nanoparticles injected intratumorally, may represent an option. Otherwise inert, NBTXR3 augments the radiation therapy (RT) dose within tumor cells when activated by RT, increasing tumor cell death compared to RT alone.</span></p>
<p><strong>Objectives:</strong> The purpose of this Phase I was to evaluate safety (dose limiting toxicity; DLT) and determine the NBTXR3 recommended phase 2 dose (RP2D) in elderly or frail HNSCC pts.</p>
<p><strong>Methods:</strong> Eligible pts had stage III or IV HNSCC of oral cavity or oropharynx, were aged ≥70 years or ≥65 years and unable to receive cisplatin but eligible for RT [NCT01946867]. A 3+3 dose escalation design was employed, with NBTRX3 dose levels of 5%, 10%, 15% and 22% of baseline tumor volume. Following intratumoral NBTXR3 injection, pts received IMRT (70 Gy; 35 fractions/7 weeks). Primary endpoints were RP2D and DLT. Localization of NBTXR3 and preliminary efficacy (RECIST 1.1) were also evaluated.</p>
<p><strong>Results and Conclusion:</strong> Dose escalation is complete; 19 pts received NBTXR3: 3 at 5%, 3 at 10%, 5 at 15% and 8 at 22%. No NBTXR3-related DLTs or SAEs were observed. Four related AEs were reported: one AE at 15% (G1 tumor hemorrhage) and 3 AEs at 22% (G2 oral pain; G1 asthenia, G1 injection site hemorrhage). IMRT toxicity was as expected and post-injection CT scan showed NBTXR3 localized within the injected tumor. DSMB determined RP2D to be 22%. Among 13 evaluable pts at doses ≥10%, 9 had a complete response of injected tumor. Results demonstrate that NBTXR3 activated by RT is a well-tolerated therapy with encouraging anti-tumor activity. RP2D expansion is ongoing. NBTXR3 may be an option for elderly or frail pts with locally advanced HNSCC.</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/fr/2019-siog-nbtxr3-for-the-treatment-of-elderly-frail-hnscc-patients/">2019 – SIOG – NBTXR3 for the treatment of elderly/frail HNSCC patients</a> first appeared on <a href="https://bibliography.nanobiotix.com/fr/">Nano Publications</a>.]]></content:encoded>
					
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		<title>2019 – ASTRO – NBTXR3 for the treatment of solid tumors</title>
		<link>https://bibliography.nanobiotix.com/fr/2019-astro-nbtxr3-for-the-treatment-of-solid-tumors/</link>
		
		<dc:creator><![CDATA[nano-pub]]></dc:creator>
		<pubDate>Thu, 19 Sep 2019 13:00:08 +0000</pubDate>
				<category><![CDATA[Abstracts]]></category>
		<category><![CDATA[Donnée clinique de NBTXR3]]></category>
		<category><![CDATA[Foie]]></category>
		<category><![CDATA[Rectum]]></category>
		<category><![CDATA[STM]]></category>
		<category><![CDATA[Tête & Cou]]></category>
		<category><![CDATA[Brachytherapy]]></category>
		<category><![CDATA[EBRT]]></category>
		<category><![CDATA[Hafnium Oxide]]></category>
		<category><![CDATA[Head and Neck Squamous Cell Carcinoma]]></category>
		<category><![CDATA[HNSCC]]></category>
		<category><![CDATA[IMRT]]></category>
		<category><![CDATA[Liver Cancer]]></category>
		<category><![CDATA[Nanoparticles]]></category>
		<category><![CDATA[NBTXR3]]></category>
		<category><![CDATA[Prostate]]></category>
		<category><![CDATA[SBRT]]></category>
		<category><![CDATA[Soft Tissue Sarcoma]]></category>
		<category><![CDATA[STS]]></category>
		<guid isPermaLink="false">https://bibliography.nanobiotix.com/?p=1897</guid>

					<description><![CDATA[<p>Local interventional treatments of cancers include interventional radiology and radiotherapy (RT). NBTXR3, hafnium oxide nanoparticles, is deeply associated to both. Given as a single local administration it increases energy dose deposit inside tumor cells only when activated by ionizing radiation. Various interventional treatments have been used to treat cancers such as liver, lung, bone. Because entirely new therapies such as NBTXR3 are being introduced, implementation of interventional approaches is continuously growing. […]</p>
The post <a href="https://bibliography.nanobiotix.com/fr/2019-astro-nbtxr3-for-the-treatment-of-solid-tumors/">2019 – ASTRO – NBTXR3 for the treatment of solid tumors</a> first appeared on <a href="https://bibliography.nanobiotix.com/fr/">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>A. P. Dicker<span class="notes up">1</span>, C. Shen<span class="notes up">2</span>, T. De Baere<span class="notes up">3</span>, C. Hoffmann<span class="notes up">4</span>, J. W. Welsh<span class="notes up">5</span>, Y. Rolland<span class="notes up">6</span>, B. Doger<span class="notes up">7</span>, R. B. Den<span class="notes up">1</span>, E. Trabulsi<span class="notes up">1</span>, C. Lallas<span class="notes up">1</span>, T. Y. Seiwert<span class="notes up">8</span>, N. Fernando<span class="notes up">9</span>, A. Iannessi<span class="notes up">10</span>, F. Pilleul<span class="notes up">11</span>, Z. Papai<span class="notes up">12</span>, R. Tetreau<span class="notes up">13</span>, P. Rutkowski<span class="notes up">14</span>, and H. Brisse<span class="notes up">4</span><br />
<span class="notes"><br />
1 – Thomas Jefferson University, Philadelphia, PA<br />
2 – University of North Carolina Hospitals, Chapel Hill, NC<br />
3 – Institut Gustave Roussy, Villejuif, France<br />
4 – Institut Curie, Paris, France<br />
5 – MD Anderson Cancer Center, Division of Radiation Oncology, Houston, TX, 6Centre Eugène Marquis, Rennes, France<br />
7 – START Madrid, Madrid, Spain<br />
8 – Department of Medicine, Section of Hematology/Oncology, The University of Chicago Medicine, Chicago, IL<br />
9 – Northside Hospital, Atlanta, GA<br />
10 – Centre Anticancer Antoine Lacassagne, Nice, France<br />
11 – Unicancer &#8211; Leon Berard Cancer Center, Lyon, France<br />
12 – Magyar Honvedseg Egeszsegugyi Kozpont, Budapest, Hungary<br />
13 – Montpellier Cancer Institute, Montpellier, France<br />
14 – Centrum Onkologii-Instytut im. Sklodowskiej-Curie w Warszawie, Warszawa, Poland<br />
</span></p>
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            </div><div class="az-box-icon-content"><h3 class="az-box-icon-title">Summary</h3><p><strong>Purpose/Objective(s):</strong> Local interventional treatments of cancers include interventional radiology and radiotherapy (RT). NBTXR3, hafnium oxide nanoparticles, is deeply associated to both. Given as a single local administration it increases energy dose deposit inside tumor cells only when activated by ionizing radiation. Various interventional treatments have been used to treat cancers such as liver, lung, bone. Because entirely new therapies such as NBTXR3 are being introduced, implementation of interventional approaches is continuously growing.</p>
<p><strong>Materials/Methods:</strong> NBTXR3 is being evaluated in soft tissue sarcoma (STS, extremity, trunk wall) [NCT02379845], head and neck (HN) [NCT01946867, NCT02901483], prostate [NCT02805894], liver [NCT02721056] and rectal cancers [NCT02465593]. NBTXR3 injected volume is a percentage of baseline tumor volume, and therefore heterogeneous. Image guidance allowed for accurate injection. Standard catheters, needles, and syringes were used for preparation and injection. Importantly, percutaneous needle positioning was done within the region to be irradiated to control potential seeding of cancer cells. NBTXR3 was then activated by IMRT (STS, HN), EBRT or combination brachytherapy/EBRT boost (prostate), SBRT (liver), IMRT or IMAT (rectum).</p>
<p><strong>Results:</strong> Thus far, NBTXR3 has been administered to 171 patients by intratumoral/lesional, and intraprostate injections depending on indication. NBTXR3 injections have been demonstrated safe and very well tolerated. Local infection, ulceration or massive tumor necrosis were never observed. This has been confirmed by adequate application of treatment schedules, fitting planned irradiation onset 1 to 5 days post-injection. Importantly, grade 1 ecchymosis and hematoma at puncture site (needle entry) observed in few cases always resolved spontaneously and did not impact dosimetry. Indeed, change of tumor/lesion/prostate volume resolved when water (NBTXR3 vehicle) was drained via lymphatic system. So far, inflammatory response to injection procedure itself was mild. Concerning AEs, grade 3 pain was observed in conscious patients under local anesthesia with STS close to joints (limited extensibility), and in needle shift in injection within a subcapsular liver tumor.</p>
<p><strong>Conclusion:</strong> Across 7 clinical trials involving tumors in extremity, trunk wall, liver, rectum, prostate and HN, NBTXR3 injection was well tolerated and demonstrated a very good safety profile. The savoir faire of interventional radiology for local treatment of cancers supported implementation of injection procedures with specific parameters according to anatomy. Intratumoral/lesional or intraprostate injection ensures optimum bioavailability at site of irradiation, protecting patients from systemic toxicity. Future clinical research will involve other anatomical sites such as lymph nodes and lung lesions [NCT03589339].</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/fr/2019-astro-nbtxr3-for-the-treatment-of-solid-tumors/">2019 – ASTRO – NBTXR3 for the treatment of solid tumors</a> first appeared on <a href="https://bibliography.nanobiotix.com/fr/">Nano Publications</a>.]]></content:encoded>
					
		
		
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		<title>2019 – ASCO – Phase I NBTXR3 in elderly/frail HNSCC patients</title>
		<link>https://bibliography.nanobiotix.com/fr/2019-asco-phase-i-nbtxr3-in-elderly-frail-hnscc-patients/</link>
		
		<dc:creator><![CDATA[nano-pub]]></dc:creator>
		<pubDate>Mon, 01 Jul 2019 13:26:40 +0000</pubDate>
				<category><![CDATA[Abstracts]]></category>
		<category><![CDATA[Donnée clinique de NBTXR3]]></category>
		<category><![CDATA[Tête & Cou]]></category>
		<category><![CDATA[Elderly]]></category>
		<category><![CDATA[Frail]]></category>
		<category><![CDATA[Hafnium Oxide]]></category>
		<category><![CDATA[Head and Neck Squamous Cell Carcinoma]]></category>
		<category><![CDATA[HNSCC]]></category>
		<category><![CDATA[IMRT]]></category>
		<category><![CDATA[Intensity Modulated]]></category>
		<category><![CDATA[Nanoparticles]]></category>
		<category><![CDATA[NBTXR3]]></category>
		<category><![CDATA[Oral Cavity]]></category>
		<category><![CDATA[Oropharynx]]></category>
		<category><![CDATA[Radiation Therapy]]></category>
		<category><![CDATA[Radiotherapy]]></category>
		<category><![CDATA[RP2D]]></category>
		<guid isPermaLink="false">https://bibliography.nanobiotix.com/?p=1815</guid>

					<description><![CDATA[<p>New therapeutic approaches are needed for elderly or frail head and neck squamous cell carcinoma (HNSCC) patients (pts) ineligible for standard of care treatment. NBTXR3, a crystalline solution of hafnium oxide nanoparticles may represent such an option. Injected intratumorally, NBTXR3 enters tumor cells and yields an increased cell-localized energy deposit upon exposure to radiotherapy (RT), leading to increased tumor cell death compared to the same dose of RT alone. […]</p>
The post <a href="https://bibliography.nanobiotix.com/fr/2019-asco-phase-i-nbtxr3-in-elderly-frail-hnscc-patients/">2019 – ASCO – Phase I NBTXR3 in elderly/frail HNSCC patients</a> first appeared on <a href="https://bibliography.nanobiotix.com/fr/">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>Christophe Le Tourneau<span class="notes up">1</span>, Victor Moreno Garcia<span class="notes up">2</span>, Sébastien Salas<span class="notes up">3</span>, Xavier Mirabel<span class="notes up">4</span>, Emiliano Calvo<span class="notes up">2</span>, Bernard Doger<span class="notes up">2</span>, Carmen Florescu<span class="notes up">5</span>, Juliette Thariat<span class="notes up">5</span>, Jacek Fijuth<span class="notes up">6</span>, Tomasz Rutkowski<span class="notes up">7</span> Nicolas Magné<span class="notes up">8</span>, Xavier Liem<span class="notes up">4</span>, Nicolas Fakhry<span class="notes up">3</span>, Stéphanie Wong<span class="notes up">3</span>, Valentin Calugaru<span class="notes up">1</span>, Caroline Hoffmann<span class="notes up">1</span><br />
<span class="notes"><br />
1 – Institut Curie, Paris, France<br />
2 – START Madrid, Madrid, Spain<br />
3 – Hôpital Timone, APHM, Marseille, France<br />
4 – Centre Oscar Lambret, Lille, France<br />
5 – Unicancer &#8211; François Baclesse Center, Caen, France<br />
6 – Provita Prolife, Tomaszów Mazowiecki, Poland<br />
7 – Maria Skłodowska-Curie Institute of Oncology, Gliwice, Poland<br />
8 – Institut de Cancérologie Lucien Neuwirth, Saint-Priest-en-Jarez, France<br />
</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><strong>Background:</strong> New therapeutic approaches are needed for elderly or frail head and neck squamous cell carcinoma (HNSCC) patients (pts) ineligible for standard of care treatment. NBTXR3, a crystalline solution of hafnium oxide nanoparticles may represent such an option. Injected intratumorally, NBTXR3 enters tumor cells and yields an increased cell-localized energy deposit upon exposure to radiotherapy (RT), leading to increased tumor cell death compared to the same dose of RT alone.</p>
<p><strong>Methods:</strong> Phase I study of NBTXR3 activated by RT in pts ≥70 years old or ≥65 years old and unable to receive cisplatin, eligible for exclusive RT with stage III or IV HNSCC of the oral cavity or oropharynx [NCT01946867]. A 3+3 dose escalation design was implemented with dose levels corresponding to 5%, 10%, 15% and 22% of baseline tumor volume, followed by an expansion phase. Pts received an intratumoral (IT) injection of NBTXR3 and intensity modulated RT (IMRT; 70 Gy/35fractions/7 weeks). Determination of Recommended Phase 2 Dose (RP2D) and Dose Limiting Toxicities (DLT) were primary endpoints of phase I. Absence of NBTXR3 leakage and preliminary efficacy using RECIST 1.1 principles were also evaluated.</p>
<p><strong>Results:</strong> The doseescalation is complete. Nineteen pts were enrolled: 3 at 5%, 3 at 10%; 5 at 15% and 8 at 22% with no observed DLT or SAE related to NBTXR3 or IT injection. One grade 1 NBTXR3-related AE (asthenia at 22%) and four IT injection-related AE (grade 2 oral pain; grade 1 tumor hemorrhage; grade 1 asthenia, and grade 1 injection site hemorrhage) were reported. RT-related toxicity was as expected with IMRT. RP2D has been determined to be 22%. CTscan assessment between 24h and 7 weeks post-IT injection demonstrated absence of NBTXR3 leakage in the surrounding tissues. Among 13 evaluable pts treated at doses ≥10%, 9 achieved a complete response of the injected lesion.</p>
<p><strong>Conclusions:</strong> These results show that NBTXR3 activated by RT is safe and well tolerated at all doses with preliminary encouraging efficacy results. It thus represents a promising future treatment for frail and elderly pts with locally advanced HNSCC with limited therapeutic options. Expansion phase has started at the RP2D.</p>
<p><strong>Clinical trial information:</strong> NCT01946867</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/fr/2019-asco-phase-i-nbtxr3-in-elderly-frail-hnscc-patients/">2019 – ASCO – Phase I NBTXR3 in elderly/frail HNSCC patients</a> first appeared on <a href="https://bibliography.nanobiotix.com/fr/">Nano Publications</a>.]]></content:encoded>
					
		
		
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		<title>2019 – ICHNO – Phase I/II NBTXR3 in HNSCC</title>
		<link>https://bibliography.nanobiotix.com/fr/2019-ichno-phase-i-ii-nbtxr3-in-hnscc/</link>
		
		<dc:creator><![CDATA[nano-pub]]></dc:creator>
		<pubDate>Tue, 02 Apr 2019 08:22:48 +0000</pubDate>
				<category><![CDATA[Abstracts]]></category>
		<category><![CDATA[Donnée clinique de NBTXR3]]></category>
		<category><![CDATA[Tête & Cou]]></category>
		<category><![CDATA[Elderly]]></category>
		<category><![CDATA[Frail]]></category>
		<category><![CDATA[Hafnium Oxide]]></category>
		<category><![CDATA[HNSCC]]></category>
		<category><![CDATA[IMRT]]></category>
		<category><![CDATA[Intensity Modulated]]></category>
		<category><![CDATA[Nanoparticles]]></category>
		<category><![CDATA[NBTXR3]]></category>
		<category><![CDATA[Radiation]]></category>
		<category><![CDATA[Therapy]]></category>
		<guid isPermaLink="false">https://bibliography.nanobiotix.com/?p=1746</guid>

					<description><![CDATA[<p>Hafnium oxide nanoparticles, NBTXR3, were developed to augment tumor-localized high energy deposit once activated by ionizing radiation such as Intensity Modulated Radiation Therapy (IMRT) and thus to increase tumor cell death compared to the same dose of radiation. NBTXR3 is characterized by a single intratumoral (IT) administration and fits into standard radiotherapy schedule with no change in patient’s care pathway, treatment protocol or equipment. […]</p>
The post <a href="https://bibliography.nanobiotix.com/fr/2019-ichno-phase-i-ii-nbtxr3-in-hnscc/">2019 – ICHNO – Phase I/II NBTXR3 in HNSCC</a> first appeared on <a href="https://bibliography.nanobiotix.com/fr/">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>C. Hoffmann<span class="notes up">1</span>, V. Calgaru<span class="notes up">1</span>, V. Moreno Garcia<span class="notes up">2</span>, X. Mirabel<span class="notes up">3</span>, B. Dodger de Spéville<span class="notes up">2</span>, E. Calvo<span class="notes up">2</span>, T. Jouffroy<span class="notes up">1</span>, J. Rodriguez<span class="notes up">1</span>, A. Chilles<span class="notes up">1</span>, M. Yemi<span class="notes up">1</span>, M. Lesnik<span class="notes up">1</span>, N. Badois<span class="notes up">1</span>, X. Liem<span class="notes up">3</span>, S. Salas<span class="notes up">4</span>, N. Fakhry<span class="notes up">4</span>, S. Wong<span class="notes up">4</span>, C. Le Tourneau<span class="notes up">1</span><br />
<span class="notes"><br />
1 – Institut Curie, Paris, France<br />
2 – START Madrid, Madrid, Spain<br />
3 – Centre Oscar Lambret, Lille, France<br />
4 – Hôpital Timone, APHM, Marseille<br />
</span></p>
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            </div><div class="az-box-icon-content"><h3 class="az-box-icon-title">Summary</h3><p><strong>Purpose/Objective:</strong> Hafnium oxide nanoparticles, NBTXR3, were developed to augment tumor-localized high energy deposit once activated by ionizing radiation such as <em>Intensity Modulated Radiation Therapy (IMRT)</em> and thus to increase tumor cell death compared to the same dose of radiation. NBTXR3 is characterized by a single intratumoral (IT) administration and fits into standard radiotherapy schedule with no change in patient’s care pathway, treatment protocol or equipment. A phase I trial is currently evaluating NBTXR3 in elderly patients (pts) with locally advanced head and neck squamous cell carcinoma (HNSCC) of the oral cavity and oropharynx not eligible for cisplatin or intolerant to cetuximab [NCT01946867].</p>
<p><strong>Material/Methods:</strong> In this phase I open-label, non-randomized trial, elderly frail pts (65 years and older) were treated with an IT injection of NBTXR3 followed by IMRT (70 Gy in 35 fractions over 7 weeks) with a follow-up period until disease progression or study cut-off date. The study was designed as a 3 + 3 escalation dose with tested NBTXR3 dose levels at 5%, 10%, 15% and 22% of baseline tumor volume. Primary endpoints included the determination of recommended dose and early dose limiting toxicity (DLT). Presence of NBTXR3 in the surrounding healthy tissues and efficacy as per RECIST 1.1 tumor response were also evaluated.</p>
<p><strong>Results:</strong> The inclusion was completed at all dose levels 22% (7 pts), 15% (5 pts), 10% (3 pts) and at 5% (3 pts). All patients that completed the DLT evaluation period did not present any early DLTs or serious adverse events (SAEs) related to NBTXR3 or the injection procedure. So far, two AEs (asthenia, grade 1; pain, grade 2) related to NBTXR3 were reported in patients at the 22% dose level. Additionally, four AEs related to the injection procedure (tumor hemorrhage, grade 1; oral pain, grade 2; asthenia, grade 1, hemorrhage, grade 1) occurred in patients at the 15% and 22% dose levels.</p>
<p><strong>Conclusion:</strong> NBTXR3 was well tolerated even at the highest dose with an overall positive safety profile. As the last dose level was reached, a dose expansion group will start in this clinical setting once the recommended dose is identified. These results open a promising perspective in frail HNSCC pts with advanced age, which is a population not often evaluated in clinical trials. NBTXR3 was also evaluated in a phase II/III clinical trial in soft tissue sarcoma [NCT02379845] with positive results and is currently being evaluated in prostate cancer [NCT02805894], liver cancer [NCT02721056], rectal cancer [NCT02465593] and recurrent/metastatic HNSCC or metastatic non-small cell lung cancer [NCT03589339].</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/fr/2019-ichno-phase-i-ii-nbtxr3-in-hnscc/">2019 – ICHNO – Phase I/II NBTXR3 in HNSCC</a> first appeared on <a href="https://bibliography.nanobiotix.com/fr/">Nano Publications</a>.]]></content:encoded>
					
		
		
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		<title>2018 – SIOG – NBTXR3 In Elderly With HNSCC</title>
		<link>https://bibliography.nanobiotix.com/fr/2018-siog-nbtxr3-in-elderly-with-hnscc/</link>
		
		<dc:creator><![CDATA[nano-pub]]></dc:creator>
		<pubDate>Tue, 27 Nov 2018 09:21:05 +0000</pubDate>
				<category><![CDATA[Abstracts]]></category>
		<category><![CDATA[Donnée clinique de NBTXR3]]></category>
		<category><![CDATA[Tête & Cou]]></category>
		<category><![CDATA[Hafnium Oxide]]></category>
		<category><![CDATA[HNSCC]]></category>
		<category><![CDATA[IMRT]]></category>
		<category><![CDATA[Nanomedicine]]></category>
		<category><![CDATA[NBTXR3]]></category>
		<guid isPermaLink="false">http://bibliography.nanobiotix.com/2018-siog-nbtxr3-in-elderly-with-hnscc/</guid>

					<description><![CDATA[<p>Compared to younger individuals, elderly patients with head and neck squamous cell carcinoma (HNSCC) have limited therapeutic options. Despite representing approximately 47% of the affected population with an increasing incidence, older patients are underrepresented from HNSCC prospective clinical trials further limiting their therapeutic options. […]</p>
The post <a href="https://bibliography.nanobiotix.com/fr/2018-siog-nbtxr3-in-elderly-with-hnscc/">2018 – SIOG – NBTXR3 In Elderly With HNSCC</a> first appeared on <a href="https://bibliography.nanobiotix.com/fr/">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>C. Hoffmann<span class="notes up">1</span>, V. Calgaru<span class="notes up">1</span>, V. Moreno<span class="notes up">2</span>, X. Mirabel<span class="notes up">3</span>, B. Dodger<span class="notes up">2</span>, E. Calvo<span class="notes up">2</span>, T. Jouffroy<span class="notes up">1</span>, J. Rodriguez<span class="notes up">1</span>, A. Chilles<span class="notes up">1</span>, M. Yemi<span class="notes up">1</span>, C. Le Tourneau<span class="notes up">1</span><br />
<span class="notes"><br />
1 – Institut Curie, Paris, France<br />
2 – START Madrid, Madrid, Spain<br />
3 – Centre Oscar Lambret, Lille, France<br />
</span></p>
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            </div><div class="az-box-icon-content"><h3 class="az-box-icon-title">Summary</h3><p>Compared to younger individuals, elderly patients with head and neck squamous cell carcinoma (HNSCC) have limited therapeutic options. Despite representing approximately 47% of the affected population with an increasing incidence, older patients are underrepresented from HNSCC prospective clinical trials further limiting their therapeutic options.</p>
<p>Intensity-modulated radiation therapy (IMRT) represents a viable treatment. Yet, like with all radiation therapy (RT) techniques, the energy dose deposit to tumor cells is limited by the surrounding healthy tissues. Injectable hafnium oxide nanoparticles, NBTXR3, were developed to increase the deposited dose of ionizing radiation within tumor cells when activated by RT. This phase I clinical study evaluates NBTXR3 in the treatment of locally advanced HNSCC of the oral cavity and oropharynx in frail elderly patients ineligible for surgery and cisplatin, the non-surgical standard of care, or intolerant to cetuximab.</p>
<p>Overall, preliminary results show a very good safety profile with favorable signs of efficacy, indicating NBTXR3 as a promising future treatment for frail and elderly patients with locally advanced HNSCC burdened from limited therapeutic options.</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/fr/2018-siog-nbtxr3-in-elderly-with-hnscc/">2018 – SIOG – NBTXR3 In Elderly With HNSCC</a> first appeared on <a href="https://bibliography.nanobiotix.com/fr/">Nano Publications</a>.]]></content:encoded>
					
		
		
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