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Surface functionality affects the biodistribution and microglia-targeting of intra-amniotically delivered dendrimers.


ABSTRACT: Cerebral Palsy (CP) is a chronic childhood disorder with limited therapeutic options. Maternal intrauterine inflammation/infection is a major risk factor in the pathogenesis of CP. In pre-clinical models, dendrimer-based therapies are viable in postnatal period, attenuating inflammation and improving motor function in vivo. However, treatment to the mother, in the prenatal period, may provide the possibility of preventing/resolving inflammation at early stages. Towards this goal, we used a maternal intrauterine inflammation-induced rabbit model of CP to study fetal-maternal transport and neuroinflammation targeting of intra-amniotically administrated dendrimers with neutral/anionic surface functionality. Our study suggested both hydroxyl-terminated 'neutral' (D-OH) and carboxyl-terminated 'anionic' (D-COOH) Polyamidoamine (PAMAM) dendrimers were absorbed by fetuses and demonstrated bi-directional transport between fetuses and mother. D-OH was more effective in crossing the fetal blood-brain barrier, and targeting activated microglia. The cell-specific targeting was associated with the extent of microglia activation. This study demonstrated intra-amniotically administered hydroxyl PAMAM dendrimers could be an effective drug delivery vehicle for targeting fetal inflammation and preventing subsequent neurologic injury associated with chorioamnionitis.

SUBMITTER: Zhang F 

PROVIDER: S-EPMC5380001 | biostudies-literature | 2016 Sep

REPOSITORIES: biostudies-literature

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Surface functionality affects the biodistribution and microglia-targeting of intra-amniotically delivered dendrimers.

Zhang Fan F   Nance Elizabeth E   Zhang Zhi Z   Jasty Venkatasai V   Kambhampati Siva P SP   Mishra Manoj K MK   Burd Irina I   Romero Roberto R   Kannan Sujatha S   Kannan Rangaramanujam M RM  

Journal of controlled release : official journal of the Controlled Release Society 20160701


Cerebral Palsy (CP) is a chronic childhood disorder with limited therapeutic options. Maternal intrauterine inflammation/infection is a major risk factor in the pathogenesis of CP. In pre-clinical models, dendrimer-based therapies are viable in postnatal period, attenuating inflammation and improving motor function in vivo. However, treatment to the mother, in the prenatal period, may provide the possibility of preventing/resolving inflammation at early stages. Towards this goal, we used a mater  ...[more]

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