Jacques Cluzel scite author profile

Jacques Cluzel

3Publications

73Citation Statements Received

84Citation Statements Given

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Affiliations

Clermont Université, Inserm, Laboratoire de Météorologie Physique

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In vivo efficacy of melanoma internal radionuclide therapy with a ¹³¹I‐labelled melanin‐targeting heteroarylcarboxamide molecule

Degoul

Borel

Jacquemot

et al. 2013

Intl Journal of Cancer

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The development of alternative therapies for melanoma treatment is of great interest as long-term tumour regression is not achieved with new targeted chemotherapies on selected patients. We previously demonstrated that radioiodinated heteroarylcarboxamide ([ 131 I]ICF01012) induced a strong anti-tumoural effect by inhibiting both primary tumour growth and dissemination process in a B16BL6 melanoma model. In our study, we show that a single injection of [ 131 I]ICF01012 (ranging from 14.8 to 22.2 MBq) was effective and associated with low and transient haematological toxicity. Concerning pigmented organs, cutaneous melanocytes and skin were undamaged. In 30% of treated animals, no histological alteration of retina was observed, and in the remaining 70%, damages were restricted to the optic nerve area. Using the Medical Internal Radiation Dose methodology, we determined that the absorbed dose in major organs is very low (<4 Gy) and that a delivery of 30 Gy to the tumour is sufficient for an effective anti-tumoural response. Molecular analyses of treated tumours showed a strong radiobiological effect with a decrease in proliferation, survival and pro-angiogenic-related markers and an increase in tumour suppressor gene expression, melanogenesis and anti-angiogenic markers. All these features are in accordance with a tumour cell death mechanism that mainly occurs by mitotic catastrophe and provide a better understanding of in vivo anti-tumoural effects of Metastatic melanoma has a poor prognosis with an estimated death rate ranging from 1.8 to 3.5 per 100,000 cases worldwide. 1,2 As with other cancers, chemotherapy (dacarbazine) remained the conventional treatment with poor benefit for over half a century. Two strategies have improved melanoma treatment, one using the tumour immune response by blocking cytotoxic T-lymphocyte activation (antibody anti-CTL4) 3 and the other targeting BRAF. 4 A recent multicentre phase 1 clinical trial testing a mutated BRAF (V600E) inhibitor showed complete or partial tumour regression in the majority of patients. 5 However, BRAF mutations are detected in only 60% of melanoma cases, and the therapy involves selection of patients with tumours that carry the V600E BRAF mutation. 5,6 Furthermore, most treated patients acquire resistance to this inhibitor after initial clinical response. 7 Metastatic melanoma is always described as a refractory disease, and new observations suggest that combined therapies will have a greater impact on melanoma residual activity. As the mechanisms of resistance to treatment rely on tumour adaptation by somatic mutations, 8 other non-protein targets such as melanin could be considered for future therapies.Melanin pigment is detected in more than 90% of primary melanoma cases, and thus, a strategy targeting this pigment

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Presence of specific platelet-activating factor binding sites in the rat retina

Thierry

Doly

Braquet³

et al. 1989

European Journal of Pharmacology

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Light-induced variations of retinal sensitivity in rats

Ranchon

Gorrand

Cluzel

et al. 1998

Current Eye Research

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Jacques Cluzel

In vivo efficacy of melanoma internal radionuclide therapy with a ¹³¹I‐labelled melanin‐targeting heteroarylcarboxamide molecule

Presence of specific platelet-activating factor binding sites in the rat retina

Light-induced variations of retinal sensitivity in rats

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Jacques Cluzel

In vivo efficacy of melanoma internal radionuclide therapy with a 131I‐labelled melanin‐targeting heteroarylcarboxamide molecule

Presence of specific platelet-activating factor binding sites in the rat retina

Light-induced variations of retinal sensitivity in rats

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In vivo efficacy of melanoma internal radionuclide therapy with a ¹³¹I‐labelled melanin‐targeting heteroarylcarboxamide molecule