Research output: Contribution to journal › Article › peer-review
Journal | Chemistry : A European Journal |
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Date | Accepted/In press - 10 Sep 2017 |
Date | E-pub ahead of print (current) - 1 Dec 2017 |
Issue number | 67 |
Volume | 23 |
Number of pages | 8 |
Pages (from-to) | 16990-16997 |
Early online date | 1/12/17 |
Original language | English |
Despite the successful use of isoniazid, rifampicin, pyrazinamide and ethambutol in the treatment of tuberculosis (TB), it is a disease of growing global concern. We illustrate here a series of methods that will dramatically improve the magnetic resonance imaging (MRI) detectability of nineteen TB-relevant agents. We note that the future probing of their uptake and distribution in vivo would be expected to significantly enhance their efficacy in disease treatment. This improvement in detectability is achieved by use of the parahydrogen based SABRE protocol in conjunction with the 2H-labelling of key sites within their molecular structures and the 2H-labelling of the magnetization transfer catalyst. The T1 relaxation times and polarization levels of these agents are quantified under test conditions to produce a protocol to identify structurally optimized motifs for future detection. For example, deuteration of the 6-position of a pyrazinamide analogue leads to a structural form that exhibits T1 values of 144.5 s for 5-H with up to 20 % polarization. This represents a >7-fold extension in relaxation time and almost 10-fold improvement in polarization level when compared to its unoptimized structure.
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Project: Research project (funded) › Research
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