Exploiting Bacterial Pathways for BBB Crossing with PLGA Nanoparticles Modified with a Mutated Form of Diphtheria Toxin (CRM197): <i>In Vivo</i> Experiments G. Tosi A. Vilella P. Veratti D. Belletti F. Pederzoli B. Ruozi M. A. Vandelli M. Zoli F. Forni 10.1021/acs.molpharmaceut.5b00446.s002 https://acs.figshare.com/articles/journal_contribution/Exploiting_Bacterial_Pathways_for_BBB_Crossing_with_PLGA_Nanoparticles_Modified_with_a_Mutated_Form_of_Diphtheria_Toxin_CRM197_i_In_Vivo_i_Experiments/2125807 Drugs can be targeted to the brain using polymeric nanoparticles (NPs) engineered on their surface with ligands able to allow crossing of the blood–brain barrier (BBB). This article aims to investigate the BBB crossing efficiency of polymeric poly lactide-<i>co</i>-glycolide (PLGA) NPs modified with a mutated form of diphtheria toxin (CRM197) in comparison with the results previously obtained using PLGA NPs modified with a glycopeptide (g7-NPs). Different kinds of NPs, covalently coupled PLGA with different fluorescent probes (DY405, rhodamine-B base and DY675) and different ligands (g7 and CRM197) were tested <i>in vivo</i> to assess their behavior and trafficking. The results highlighted the possibility to distinguish the different kinds of simultaneously administered NPs and to emphasize that CRM-197 modified NPs and g7-NPs can cross the BBB at a similar extent. The analysis of BBB crossing and of the neuronal tropism of CRM197 modified NPs, along with their BBB crossing pathways were also developed. <i>In vivo</i> pharmacological studies performed on CRM197 engineered NPs, loaded with loperamide, underlined their ability as drug carriers to the CNS. 2015-10-05 00:00:00 CNS NP CRM 197 PLGA Nanoparticles Modified BBB DY