A nanomedicine transports a peptide caspase-3 inhibitor across the blood-brain barrier and provides neuroprotection

Hulya Karatas; Yesim Aktas; Yasemin Gursoy-Ozdemir; Ebru Bodur; Muge Yemisci; Secil Caban; Atay Vural; Onur Pinarbasli; Yilmaz Capan; Eduardo Fernandez-Megia; Ramon Novoa-Carballal; Ricardo Riguera; Karine Andrieux; Patrick Couvreur; Turgay Dalkara

doi:10.1523/JNEUROSCI.4246-09.2009

A nanomedicine transports a peptide caspase-3 inhibitor across the blood-brain barrier and provides neuroprotection

Hulya Karatas
, Yesim Aktas
, Yasemin Gursoy-Ozdemir
, Ebru Bodur
, Muge Yemisci
, Secil Caban
, Atay Vural
, Onur Pinarbasli
, Yilmaz Capan
, Eduardo Fernandez-Megia
, Ramon Novoa-Carballal
, Ricardo Riguera
, Karine Andrieux
, Patrick Couvreur
, Turgay Dalkara

Research output: Contribution to journal › Article › peer-review

187 Citations (Scopus)

Abstract

Caspases play an important role as mediators of cell death in acute and chronic neurological disorders. Although peptide inhibitors of caspases provide neuroprotection, they have to be administered intracerebroventricularly because they cannot cross the blood-brain barrier (BBB). Herein, we present a nanocarrier system that can transfer chitosan nanospheres loaded with N-benzyloxycarbonyl-Asp(OMe)-Glu(OMe)-Val-Asp(OMe)-fluoromethyl ketone (Z-DEVD-FMK), a relatively specific caspase-3 inhibitor, across BBB. Caspase-3 was chosen as a pharmacological target because of its central role in cell death. Polyethylene glycol-coated nanospheres were conjugated to an anti-mouse transferrin receptor monoclonal antibody (TfRMAb) that selectively recognizes the TfR type 1 on the cerebral vasculature. We demonstrate with intravital microscopy that this nanomedicine is rapidly transported across the BBB without being measurably taken up by liver and spleen. Pre-or post-treatment (2 h) with intravenously injected Z-DEVD-FMK-loaded nanospheres dose dependently decreased the infarct volume, neurological deficit, and ischemia-induced caspase-3 activity in mice subjected to 2 h of MCA occlusion and 24 h of reperfusion, suggesting that they released an amount of peptide sufficient to inhibit caspase activity. Similarly, nanospheres inhibited physiological caspase-3 activity during development in the neonatal mouse cerebellum on postnatal day 17 after closure of the BBB. Neither nanospheres functionalized with TfRMAb but not loaded withZ-DEVD-FMKnor nanospheres lacking TfRMAb but loaded with Z-DEVD-FMK had any effect on either paradigm, suggesting that inhibition of caspase activity and subsequent neuroprotection were due to efficient penetration of the peptide into brain. Thus, chitosan nanospheres open new and exciting opportunities for brain delivery of biologically active peptides that are useful for the treatment of CNS disorders.

Original language	English
Pages (from-to)	13761-13769
Number of pages	9
Journal	Journal of Neuroscience
Volume	29
Issue number	44
DOIs	https://doi.org/10.1523/JNEUROSCI.4246-09.2009
Publication status	Published - 4 Nov 2009

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Karatas, H., Aktas, Y., Gursoy-Ozdemir, Y., Bodur, E., Yemisci, M., Caban, S., Vural, A., Pinarbasli, O., Capan, Y., Fernandez-Megia, E., Novoa-Carballal, R., Riguera, R., Andrieux, K., Couvreur, P., & Dalkara, T. (2009). A nanomedicine transports a peptide caspase-3 inhibitor across the blood-brain barrier and provides neuroprotection. Journal of Neuroscience, 29(44), 13761-13769. https://doi.org/10.1523/JNEUROSCI.4246-09.2009

@article{2ced06b7984c4fa7938e060be4789fc3,

title = "A nanomedicine transports a peptide caspase-3 inhibitor across the blood-brain barrier and provides neuroprotection",

abstract = "Caspases play an important role as mediators of cell death in acute and chronic neurological disorders. Although peptide inhibitors of caspases provide neuroprotection, they have to be administered intracerebroventricularly because they cannot cross the blood-brain barrier (BBB). Herein, we present a nanocarrier system that can transfer chitosan nanospheres loaded with N-benzyloxycarbonyl-Asp(OMe)-Glu(OMe)-Val-Asp(OMe)-fluoromethyl ketone (Z-DEVD-FMK), a relatively specific caspase-3 inhibitor, across BBB. Caspase-3 was chosen as a pharmacological target because of its central role in cell death. Polyethylene glycol-coated nanospheres were conjugated to an anti-mouse transferrin receptor monoclonal antibody (TfRMAb) that selectively recognizes the TfR type 1 on the cerebral vasculature. We demonstrate with intravital microscopy that this nanomedicine is rapidly transported across the BBB without being measurably taken up by liver and spleen. Pre-or post-treatment (2 h) with intravenously injected Z-DEVD-FMK-loaded nanospheres dose dependently decreased the infarct volume, neurological deficit, and ischemia-induced caspase-3 activity in mice subjected to 2 h of MCA occlusion and 24 h of reperfusion, suggesting that they released an amount of peptide sufficient to inhibit caspase activity. Similarly, nanospheres inhibited physiological caspase-3 activity during development in the neonatal mouse cerebellum on postnatal day 17 after closure of the BBB. Neither nanospheres functionalized with TfRMAb but not loaded withZ-DEVD-FMKnor nanospheres lacking TfRMAb but loaded with Z-DEVD-FMK had any effect on either paradigm, suggesting that inhibition of caspase activity and subsequent neuroprotection were due to efficient penetration of the peptide into brain. Thus, chitosan nanospheres open new and exciting opportunities for brain delivery of biologically active peptides that are useful for the treatment of CNS disorders.",

author = "Hulya Karatas and Yesim Aktas and Yasemin Gursoy-Ozdemir and Ebru Bodur and Muge Yemisci and Secil Caban and Atay Vural and Onur Pinarbasli and Yilmaz Capan and Eduardo Fernandez-Megia and Ramon Novoa-Carballal and Ricardo Riguera and Karine Andrieux and Patrick Couvreur and Turgay Dalkara",

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doi = "10.1523/JNEUROSCI.4246-09.2009",

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Karatas, H, Aktas, Y, Gursoy-Ozdemir, Y, Bodur, E , Yemisci, M, Caban, S, Vural, A, Pinarbasli, O, Capan, Y, Fernandez-Megia, E, Novoa-Carballal, R, Riguera, R, Andrieux, K, Couvreur, P & Dalkara, T 2009, 'A nanomedicine transports a peptide caspase-3 inhibitor across the blood-brain barrier and provides neuroprotection', Journal of Neuroscience, vol. 29, no. 44, pp. 13761-13769. https://doi.org/10.1523/JNEUROSCI.4246-09.2009

TY - JOUR

T1 - A nanomedicine transports a peptide caspase-3 inhibitor across the blood-brain barrier and provides neuroprotection

AU - Karatas, Hulya

AU - Aktas, Yesim

AU - Gursoy-Ozdemir, Yasemin

AU - Bodur, Ebru

AU - Yemisci, Muge

AU - Caban, Secil

AU - Vural, Atay

AU - Pinarbasli, Onur

AU - Capan, Yilmaz

AU - Fernandez-Megia, Eduardo

AU - Novoa-Carballal, Ramon

AU - Riguera, Ricardo

AU - Andrieux, Karine

AU - Couvreur, Patrick

AU - Dalkara, Turgay

PY - 2009/11/4

Y1 - 2009/11/4

N2 - Caspases play an important role as mediators of cell death in acute and chronic neurological disorders. Although peptide inhibitors of caspases provide neuroprotection, they have to be administered intracerebroventricularly because they cannot cross the blood-brain barrier (BBB). Herein, we present a nanocarrier system that can transfer chitosan nanospheres loaded with N-benzyloxycarbonyl-Asp(OMe)-Glu(OMe)-Val-Asp(OMe)-fluoromethyl ketone (Z-DEVD-FMK), a relatively specific caspase-3 inhibitor, across BBB. Caspase-3 was chosen as a pharmacological target because of its central role in cell death. Polyethylene glycol-coated nanospheres were conjugated to an anti-mouse transferrin receptor monoclonal antibody (TfRMAb) that selectively recognizes the TfR type 1 on the cerebral vasculature. We demonstrate with intravital microscopy that this nanomedicine is rapidly transported across the BBB without being measurably taken up by liver and spleen. Pre-or post-treatment (2 h) with intravenously injected Z-DEVD-FMK-loaded nanospheres dose dependently decreased the infarct volume, neurological deficit, and ischemia-induced caspase-3 activity in mice subjected to 2 h of MCA occlusion and 24 h of reperfusion, suggesting that they released an amount of peptide sufficient to inhibit caspase activity. Similarly, nanospheres inhibited physiological caspase-3 activity during development in the neonatal mouse cerebellum on postnatal day 17 after closure of the BBB. Neither nanospheres functionalized with TfRMAb but not loaded withZ-DEVD-FMKnor nanospheres lacking TfRMAb but loaded with Z-DEVD-FMK had any effect on either paradigm, suggesting that inhibition of caspase activity and subsequent neuroprotection were due to efficient penetration of the peptide into brain. Thus, chitosan nanospheres open new and exciting opportunities for brain delivery of biologically active peptides that are useful for the treatment of CNS disorders.

AB - Caspases play an important role as mediators of cell death in acute and chronic neurological disorders. Although peptide inhibitors of caspases provide neuroprotection, they have to be administered intracerebroventricularly because they cannot cross the blood-brain barrier (BBB). Herein, we present a nanocarrier system that can transfer chitosan nanospheres loaded with N-benzyloxycarbonyl-Asp(OMe)-Glu(OMe)-Val-Asp(OMe)-fluoromethyl ketone (Z-DEVD-FMK), a relatively specific caspase-3 inhibitor, across BBB. Caspase-3 was chosen as a pharmacological target because of its central role in cell death. Polyethylene glycol-coated nanospheres were conjugated to an anti-mouse transferrin receptor monoclonal antibody (TfRMAb) that selectively recognizes the TfR type 1 on the cerebral vasculature. We demonstrate with intravital microscopy that this nanomedicine is rapidly transported across the BBB without being measurably taken up by liver and spleen. Pre-or post-treatment (2 h) with intravenously injected Z-DEVD-FMK-loaded nanospheres dose dependently decreased the infarct volume, neurological deficit, and ischemia-induced caspase-3 activity in mice subjected to 2 h of MCA occlusion and 24 h of reperfusion, suggesting that they released an amount of peptide sufficient to inhibit caspase activity. Similarly, nanospheres inhibited physiological caspase-3 activity during development in the neonatal mouse cerebellum on postnatal day 17 after closure of the BBB. Neither nanospheres functionalized with TfRMAb but not loaded withZ-DEVD-FMKnor nanospheres lacking TfRMAb but loaded with Z-DEVD-FMK had any effect on either paradigm, suggesting that inhibition of caspase activity and subsequent neuroprotection were due to efficient penetration of the peptide into brain. Thus, chitosan nanospheres open new and exciting opportunities for brain delivery of biologically active peptides that are useful for the treatment of CNS disorders.

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DO - 10.1523/JNEUROSCI.4246-09.2009

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JO - Journal of Neuroscience

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A nanomedicine transports a peptide caspase-3 inhibitor across the blood-brain barrier and provides neuroprotection

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