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NMR studies of excluded volume interactions in peptide dendrimers. | LitMetric

AI Article Synopsis

  • - Peptide dendrimers are promising for biomedical uses because they are biocompatible and have low toxicity, making them suitable for drug and gene delivery as well as nanoparticle synthesis.
  • - This study tests two theories regarding dendrimers: that NMR relaxations are unaffected by excluded volume effects and that the mobility of side and terminal segments is similar.
  • - Results show that temperature-related NMR relaxations of inner groups in two types of dendrimers are nearly the same, supporting the first theory, while terminal groups also show similar behavior, backing the second theory.

Article Abstract

Peptide dendrimers are good candidates for diverse biomedical applications due to their biocompatibility and low toxicity. The local orientational mobility of groups with different radial localization inside dendrimers is important characteristic for drug and gene delivery, synthesis of nanoparticles, and other specific purposes. In this paper we focus on the validation of two theoretical assumptions for dendrimers: (i) independence of NMR relaxations on excluded volume effects and (ii) similarity of mobilities of side and terminal segments of dendrimers. For this purpose we study H NMR spin-lattice relaxation time, T, of two similar peptide dendrimers of the second generation, with and without side fragments in their inner segments. Temperature dependences of 1/T in the temperature range from 283 to 343 K were measured for inner and terminal groups of the dendrimers dissolved in deuterated water. We have shown that the 1/T temperature dependences of inner groups for both dendrimers (with and without side fragments) practically coincide despite different densities of atoms inside these dendrimers. This result confirms the first theoretical assumption. The second assumption is confirmed by the 1/T temperature dependences of terminal groups which are similar for both dendrimers.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC5995971PMC
http://dx.doi.org/10.1038/s41598-018-27063-3DOI Listing

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