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Published April 2009 | public
Journal Article

PASADENA hyperpolarization of ^(13)C biomolecules: equipment design and installation

Abstract

Object The PASADENA method has achieved hyperpolarization of 16–20% (exceeding 40,000-fold signal enhancement at 4.7 T), in liquid samples of biological molecules relevant to in vivo MRI and MRS. However, there exists no commercial apparatus to perform this experiment conveniently and reproducibly on the routine basis necessary for translation of PASADENA to questions of biomedical importance. The present paper describes equipment designed for rapid production of six to eight liquid samples per hour with high reproducibility of hyperpolarization. Materials and methods Drawing on an earlier, but unpublished, prototype, we provide diagrams of a delivery circuit, a laminar-flow reaction chamber within a low field NMR contained in a compact, movable housing. Assembly instructions are provided from which a computer driven, semi-automated PASADENA polarizer can be constructed. Results Together with an available parahydrogen generator, the polarizer, which can be operated by a single investigator, completes one cycle of hyperpolarization each 52 s. Evidence of efficacy is presented. In contrast to competing, commercially available devices for dynamic nuclear polarization which characteristically require 90 min per cycle, PASADENA provides a low-cost alternative for high throughput. Conclusions This equipment is suited to investigators who have an established small animal NMR and wish to explore the potential of heteronuclear (^(13)C and^(15)N) MRI, MRS, which harnesses the enormous sensitivity gain offered by hyperpolarization

Additional Information

© 2009 Springer. Received 28 November 2007 Revised: 24 October 2008 Accepted: 5 November 2008 Published online: 6 December 2008. Rudi Schulte Research Institute of Santa Barbara generously funded construction and supported research with PASADENA. We also thank the following for generous funding: NIH 1R21 CA118509 (PB), NCI 5R01CA122513 (BDR), NIH 1R01NS048589 (JBH, BDR), Rudi Schulte Research Institute (RSRI) (EYC, JBH), James G. Boswell Fellowship (PB, EYC), American Heart Association (PB), American Brain Tumor Association (PB), Tobacco Related Disease Research Program (PB), NARSAD (KH), Cancer Research and Prevention Foundation (EYC). We thank Dr. Daniel P. Weitekamp, Valerie A. Norton and Raymond A. Weitekamp for assistance with instrumentation.We also thank Dr.William Opel for support of PASADENA program at HMRI, Dr. Scott Ross for providing convenient access to high resolution solution NMR facility at Caltech. JBH thanks Drs. Peter Bachert and Wolfhard Semmler (German Cancer Research Center, DKFZ, Heidelberg, Germany) for PhD supervision. PB and BDR thank Drs. Oskar Axelsson, Haukur Johannesson and Magnus Karlsson for advice and training with the parahydrogen polarizer, in Malmö and provided for this work under loan agreement between HMRI and GE Healthcare, established by Dr. Klaes Golman.

Additional details

Created:
August 21, 2023
Modified:
October 19, 2023