Annual Reports on NMR Spectroscopy (eBook)
318 Seiten
Elsevier Science (Verlag)
978-0-08-045816-8 (ISBN)
* Includes comprehensive review articles on NMR Spectroscopy
* NMR is used in all branches of science
* No other technique has grown to such importance as NMR Spectroscopy in recent years
Nuclear magnetic resonance (NMR) is an analytical tool used by chemists and physicists to study the structure and dynamics of molecules. In recent years, no other technique has grown to such importance as NMR spectroscopy. It is used in all branches of science where precise structural determination is required and where the nature of interactions and reactions in solution is being studied. Annual Reports on NMR has established itself as a premier means for the specialist and nonspecialist alike to become familiar with new techniques and applications of NMR spectroscopy.* Includes comprehensive review articles on NMR Spectroscopy* NMR is used in all branches of science* No other technique has grown to such importance as NMR Spectroscopy in recent years
Cover 1
Annual Reports on NMR Spectroscopy 4
List of Contributors 6
Contents 10
Small-Volume and High-Sensitivity NMR Probes 12
Introduction 13
Small-Volume Conventional NMR Probes 14
The 3mm micro-NMR probes 14
The 1.7mm submicro- or SMIDGTM NMR probes 19
The 1mm gradient inverse triple resonance probes 23
Magic Angle Sideways Spinning Liquid Probes 27
µCoil NMR Probes 31
Cryogenic NMR Probes 32
Applications of Small-Volume High-Sensitivity and Cryogenic NMR Probes 42
The 3 and 2.5mm NMR probe applications 42
The 1.7 and 1.0mm NMR probe applications 78
Nano-probeTM applications 82
The µCoil NMR probe applications 88
Cryogenic NMR probe applications 89
Conclusions 98
References 99
Continuous-Wave NMR Imaging in the Solid State 108
Introduction 109
Line-Broadening Mechanisms 111
The dipole–dipole interaction 111
The chemical-shift interaction 113
The quadrupole interaction 113
Magnetic susceptibility effects 114
Overview of Solid Imaging Techniques 115
Strafi 115
Imaging with oscillating gradients 116
Single point imaging (SPI) 117
Multiple quantum (MQ) imaging 119
Magic angle spinning (MAS) imaging 120
Magic angle rotating frame (MARF) imaging 120
Imaging with multi-pulse line narrowing 121
Magic-echo imaging 123
CW-NMRI 124
CW-NMRI 125
CW-NMR spectroscopy 125
Magnetic field modulation 126
Spatial localisation 130
System hardware 132
Overview 132
Coil assembly 133
Resonators 134
Automatic frequency controller 135
Detector 136
Support frame 137
Applications 138
Imaging of cementitious materials 138
Water penetration 139
Brine penetration 142
Imaging of solid27 Al in cement 143
Diffusion of water in clay minerals 144
Imaging of a rigid polymer 147
Concluding remarks 148
Acknowledgements 148
References 149
Solution- and Solid-State NMR Studies of Eight- and Nine-Membered Medium Ring Cis-Cycloalkene Stereochemistry 152
Introduction 154
Methods 160
NMR experiments 160
Computational techniques 162
Representative Examples of NMR Studies on 2,5-Benzoxazocine Medium Ring Stereochemistry 163
(1RS,5RS)- and (1RS,5SR)-5-methyl-1-phenyl-3,4,5,6,-tetrahydro-1H-2,5-benzoxazocine hydrochloride [nefopam hydrochloride equatorial and axial N-methyl diastereomers] (15) and (18), respectively 163
5,5-Dimethyl-1-phenyl-3,4,5,6-tetrahydro-1H-2,5-benzoxazocinium halide [nefopam methohalide] (methiodide, 19) (methobromide, 21) and (methochloride, 22) 170
1-Phenyl-3,4,5,6-tetrahydro-1H-2,5-benzoxazocine hydrochloride [N-desmethyl-nefopam hydrochloride] (23) 176
(1RS,3RS,5RS)- and (1RS,3RS,5SR)-3,5-dimethyl-1-phenyl-3,4,5,6-tetrahydro-1H-2,5-benzoxazocine hydrochloride [(1RS,3RS,5RS)- and (1RS,3RS,5SR)-3-methyl-nefopam hydrochloride equatorial and axial N-methyl diastereomers] (24) and (25), respectively 179
(1RS,3SR,5SR)- and (1RS,3SR,5RS)-3,5-dimethyl-1-phenyl-3,4,5,6-tetrahydro-1H-2,5-benzoxazocine hydrochloride [(1RS,3SR,5SR)- and (1RS,3SR,5RS)-3-methyl-nefopam hydrochloride equatorial and axial N-methyl diastereomers] (26) and (27), respectively 183
4-Methyl-6-phenyl-3,4-dihydro-2H,6H-1,5,4-benzodioxazocine (28) 187
1-Phenyl-3,4,5,6-tetrahydro-1H-2,5-benzoxazocine-5-carbonitrile (30) 190
1-Phenyl-3,4,5,6-tetrahydro-1H-2,5-benzothiazocine-5-carbonitrile (31,32) 192
(1RS,3SR)-1-phenyl-3,4,5,6-tetrahydro-3,5,5-trimethyl-1H-2,5-benzoxazocinium chloride [(1RS,3SR)-3-methyl-nefopam methochloride] (33) 195
(1RS,3RS)-3-Methyl-1-phenyl-3,4,5,6-tetrahydro-1H-2,5-benzoxazocine-5-carbonitrile (35) 199
Representative Examples of NMR Studies on 2,6-Benzoxazonine Medium Ring Stereochemistry 200
1-Phenyl-1,3,4,5,6,7-hexahydro-2,6-benzoxazonine hydrochloride [N-desmethyl-2,6-homonefopam hydrochloride] (36) 200
(1RS,3SR)-3-Methyl-1-phenyl-1,3,4,5,6,7-hexahydro-2,6-benzoxazonine hydrobromide [(1RS,3SR)-N-desmethyl-3-methyl-2,6-homonefopam hydrobromide] (37) 204
(1RS,5RS)-6-Methyl-1-phenyl-1,3,4,5,6,7-hexahydro-2,6-benzoxazonine hydrogenfumarate [(1RS,5RS)-2,6-homonefopam hydrogenfumarate] (38a) and mesylate [(1RS,5RS)-2,6-homonefopam mesylate] (38b) 207
6,6-Dimethyl-1-phenyl-1,3,4,5,6,7-hexahydro-2,6-benzoxazonium iodide [2,6-homonefopam methiodide] (39) 208
(1RS,3RS)-3-Methyl-1-phenyl-1,3,4,5,6,7-hexahydro-2,6-benzoxazonine-6-carbonitrile (41) 213
1-Phenyl-1,3,4,5,6,7-hexahydro-2,6-benzoxazonine-6-carbonitrile (42) 214
(1RS,3SR)-3-Methyl-1-phenyl-1,3,4,5,6,7-hexahydro-2,6-benzoxazonine-6-carbonitrile (43) 218
Conclusions 220
Acknowledgments 221
References 221
Methods and Applications of Quantitative MRI 224
Introduction 224
Definition of a Model for the Data 225
True response 225
Noise 226
Estimation of noise variance 228
Design of the Quantitative Experiment 230
Lower bounds of the estimation variance 230
Strategies for the optimization of the measurement protocol 233
Reconstruction of Parametric Maps 235
Preprocessing 235
Estimation of the parameters q 237
Discussion/Conclusion 238
References 238
Secondary Relaxation Processes in Molecular Glasses Studied by Nuclear Magnetic Resonance Spectroscopy 242
Introduction 242
The Glass Transition Phenomenon 245
Major experimental findings 245
NMR studies of the main relaxation and NMR time windows 251
NMR Studies of Secondary Relaxation Processes 259
Probing highly hindered motion by 2H NMR: theoretical background and random walk simulations 259
Theoretical background 259
Technique of random walk simulations 261
RW simulations of 2H NMR data 262
Secondary relaxation processes of neat molecular glasses 266
2H NMR solid-echo spectra: ß-process in the glass (T< Tg)
2H NMR stimulated-echo experiments: ß-process in the glass (T< Tg)
The ß-process of TOL: a model based on 2H NMR data 273
Spin– lattice relaxation in the glass (T< Tg)
Indication of small-angle motion above Tg 282
Secondary relaxation processes of polymers 284
Multi-component glasses 286
Glass transition of binary molecular glasses 287
The secondary relaxation in binary molecular glass formers 290
Glassy-ion conductors 293
Some Comments on Theoretical Approaches to the Glass Transition Phenomenon 299
Conclusions and Outlook 302
Acknowledgement 304
References 305
Index 312
Small-Volume and High-Sensitivity NMR Probes
Gary E. Martin Pfizer Global Research and Development, Michigan Structure Elucidation Group, Kalamazoo, MI 49001-0199, USA
Abstract
Aside from efforts to develop capillary nuclear magnetic resonance (NMR) probes during the 1970s, most NMR samples were traditionally examined using 5 mm probes. Due to low gyromagnetic ratio and/or natural abundance, some larger format NMR probes were developed, these including 8 and 12 mm, and large volume probes of 18 and 22 mm. Large format probes addressed the difficulties of acquiring NMR data for insensitive nuclides when an investigator was not sample limited or dealing with highly insoluble materials. In contrast, for the characterization of scarce samples of natural products, impurities or degradants of pharmaceuticals, metabolites, forensic samples, and other severely sample-limited applications, even conventional 5 mm probes were not well suited to the task of acquiring data for such samples. These considerations led to the development of the first of the 3 mm NMR probes in the early 1990s followed by a succession of progressively smaller format NMR probes down to the 1 mm tube format probes currently available. In parallel, μCoil probes were also developed allowing the use of still smaller sample volumes, albeit in a flow cell rather than a “tube” format, as were magic angle sideways spinning liquids probes such as the Varian Nano-probe™. In the late 1990s, the first examples of cryogenic NMR probe technology became available, and these extremely high-sensitivity NMR probes are now becoming more readily available to investigators faced with undertaking the structural characterization of scarce samples. The development of small-volume and high-sensitivity NMR probes is described in this contribution and examples of the application of these probe technologies are reviewed.
1 INTRODUCTION
Nuclear magnetic resonance (NMR) methods are capable of providing a wealth of atom-to-atom connectivity information that has served to make NMR the cornerstone of modern structure elucidation. Unfortunately, NMR is also an inherently insensitive technique. Considerable effort has been expended on the part of thousands of scientists to enhance NMR sensitivity. Efforts have been focused in three primary directions. Magnet technology has been one very major focus. Magnets have progressed from predominantly 60 MHz permanent magnets in use when this author's career in NMR began to the first superconducting NMR magnets at 220 and 300 MHz with voracious appetites for liquid helium, and now to huge 900 MHz magnets that are intended for biomolecular NMR studies and essentially require a gymnasium-sized room to house them. At the same time, the field strength of magnets on instruments for more routine applications have also steadily climbed to the point that most instruments intended for walk-up usage by chemists in the pharmaceutical industry are now 400 or 500 MHz instruments. A second primary area of focus has been in the development of more sophisticated NMR pulse sequences to achieve higher sensitivity. Heteronuclear shift correlation experiments progressed from the fledgling heteronucleus-detected experiments in the early 1980s to the proton- or inverse-detected heteronuclear shift correlation experiments now in widespread usage for chemical structure characterization. The third major area of focus has been on the development of higher-sensitivity NMR probes. Historically, NMR probes have typically been based around an rf coil designed to accommodate a 5 mm NMR tube. With the advent of commercial Fourier transform NMR instruments in the late 1970s, probes evolved from simple 5 mm proton observe capabilities to heteronuclear probes with the heteronuclear or X-coil inboard surrounded by a larger proton-decoupling coil. These designs were quite serviceable through the late 1970s and early 1980s, but with the development of the first proton-detected heteronuclear shift correlation experiments by Müller,1 Bodenhausen and Ruben,2 and Bax et al.3 it became obvious that conventional heteronuclear NMR probe designs would be supplanted by what were originally termed “reverse-geometry” NMR probe designs. These are probes with the proton coil closest to the sample for improved proton sensitivity since 1H is the detected nuclide. More recently, “inverse-detection” terminology has come into common usage, the terminology again based on the exchange of the rf coils in the probe design. Modification of NMR probe coil geometry afforded better sensitivity than conventional designs, but sample requirements were still relatively high for investigators working in severely sample constrained areas of investigation such as the characterization of impurities and degradants of pharmaceuticals, metabolites, etc. This brief history sets the stage for the development of small-volume high-sensitivity conventional NMR probes that occurred through much of the 1990s, which has been followed more recently by the development and commercial availability of cryogenically cooled NMR probes with still higher sensitivity.
2 SMALL-VOLUME CONVENTIONAL NMR PROBES
Small-volume conventional NMR probes encompass the development of 3 mm micro-probes, followed very closely by a 2.5 mm variant. Nearly 6 years after the introduction of 3 mm probes, a 1.7 mm submicro- or SMIDG™ probe was introduced followed, most recently, by the development of a 1.0 mm probe. Given sample handling considerations, it is unlikely that smaller conventional (those using tubes) NMR probes will be developed. This section does not include the development of either magic angle sideways spinning liquids (Nano-probes™) or what are now generally referred to as μCoil NMR probes. These types of high-sensitivity probe technology are discussed in later sections of this contribution.
2.1 The 3 mm micro-NMR probes
Historically, small-volume NMR probes date back to the 1966 Report of Odelblad, which employed a solenoidal microcoil to study human cervical mucosal secretions.4 By the early 1970s, Shoolery had begun exploring the use of 1.7 mm capillary NMR probes for the acquisition of 13C data.5 These early reports essentially set the stage for the start of the development of 3 mm or micro-NMR probes that began in 1991 through a collaboration by the author and his colleagues, then at Burroughs Wellcome, Co., in North Carolina with staff at the Nalorac Corporation. The first experimental results obtained with a 3 mm inverse-detection micro-NMR probe were reported in 1992. Using the simple indoloquinoline alkaloid cryptolepine (1) as a model compound for the study, Crouch and Martin6 were able to demonstrate the acquisition of a heteronuclear multiple-quantum correlation (HMQC) spectrum recorded on 12 μg (0.05 μmol) of the alkaloid dissolved in 145 μL of d6-dimethyl sulfoxide (d6-DMSO) in 16 h (Fig. 1). Long-range heteronuclear shift correlation data in the form of a heteronuclear multiple-bond correlation (HMBC) experiment, which is substantially less sensitive than the HMQC experiment, were recorded on a 35 μg (0.15 μmol) sample of the alkaloid in the same volume of deuterated solvent in 21 h. These preliminary results heralded a significant advance in the characterization of small samples by heteronuclear two-dimensional (2D) NMR shift correlation methods. Later in 1992, Crouch and Martin7 reported a direct comparison of 3 and 5 mm NMR probe performance at 500 MHz. Using a sample of 167 μg (1 μmol; samples were prepared by serial dilution) of the simple alkaloid harmane (2) dissolved in either 160 or 600 μL of d6-DMSO for 3 or 5 mm NMR sample tubes, respectively, the authors found that it took four times as long to achieve the same signal-to-noise ratio (s/n ratio) in the 5 mm probe as for the 3 mm probe, based on the s/n ratio of a projection through the F2 frequency domain when identically parameterized HMQC spectra were run. Unfortunately, data were not recorded for the 3 mm sample run coaxially in the 5 mm probe.
Following the initial 1992 reports describing the capabilities of 3 mm micro-NMR probe technology, a 3 mm dual probe was developed with the X-coil inboard for the acquisition of 13C spectra. This 3 mm probe variant made it possible to acquire a 13C-NMR spectrum for submilligram samples overnight at a 13C observation frequency of 100 or 125 MHz. As NMR console designs continued to evolve incorporating pulsed field gradient capabilities, 3 mm micro-probes with gradient capabilities were also developed. Interestingly, based on work done in the laboratories of the...
Erscheint lt. Verlag | 21.9.2005 |
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Sprache | englisch |
Themenwelt | Schulbuch / Wörterbuch ► Lexikon / Chroniken |
Naturwissenschaften ► Chemie ► Analytische Chemie | |
Naturwissenschaften ► Chemie ► Physikalische Chemie | |
Naturwissenschaften ► Physik / Astronomie ► Elektrodynamik | |
Technik | |
ISBN-10 | 0-08-045816-5 / 0080458165 |
ISBN-13 | 978-0-08-045816-8 / 9780080458168 |
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