Application Notes

TD-NMR vs NMR spectroscopy and other complementary methods

Author: Kevin Nott

Published: 12 Jun 2026 · Last updated: 18 Jun 2026

Time-domain nuclear magnetic resonance (TD-NMR) is a low-field NMR technique that is commonly used in quality assurance and quality control (QA/QC) across food, agriculture, petroleum, polymer and other industries. It enables fast and robust measurements of oil, water, solid, and hydrogen/fluorine content, as well as various physical properties such as crystallinity.

Beyond routine QA/QC, TD-NMR is increasingly used in academic and industrial research for a broad range of measurements to characterise food, pharmaceuticals, cement, and other porous media.

This article outlines the characteristics and specific advantages of TD-NMR and compares it with other established analytical techniques such as NMR spectroscopy or other physiochemical methods.

TD-NMR vs NMR spectroscopy

Despite being based on the same principles, there are various practical differences between TD-NMR and NMR spectroscopy:

Sample size and robustness: TD-NMR enables measurements of larger samples and is less sensitive to sample type. Informative data can, for example, be acquired from samples contained in glass vials, including those equipped with aluminium caps such as vaccine vials. Measurements inside metal containers are not possible, as ferrous and conductive materials interfere with the magnetic field.
Magnetic field strength and nuclei: Measuring larger samples typically results in a reduced magnetic field strength, which affects sensitivity. As a consequence, TD-NMR is practically limited to nuclei with high natural abundance, most commonly 1H to 19F.
Spectral information vs relaxometry: Measuring large samples reduces magnetic field homogeneity across the sample, which prevents the acquisition of chemical spectra. Instead, TD-NMR exploits relaxometry to obtain information on molecular mobility and microstructure, in addition to enabling quantitative measurements of hydrogen and fluorine, oil, water, and solid contents.
Sample state: TD-NMR enables data acquisition in and on non-metallic materials, whether solid, liquid, or a mixture of both. In contrast, benchtop NMR spectroscopy is usually limited to liquids or solutions.
Diffusion measurements: Benchtop TD-NMR systems typically operate with higher magnetic field gradients (commonly > 3 T/m) than benchtop NMR spectroscopy systems (~0.5 T/m), which in principle allows the measurement of slower diffusion processes. While TD-NMR cannot resolve diffusion of individual chemical species, it is often used to measure water diffusion in a variety of samples and to determine droplet size in emulsions based on restricted diffusion.

	Benchtop NMR Spectroscopy	Time Domain NMR*
Instrument(s)	X-Pulse 60/90	MQC+23, MQC-R, MQC+5
Field strength	>1.45 Tesla	< 0.55 Tesla
¹H frequency	60 MHz	< 23 MHz
Nuclei	¹H, ¹⁹F, ¹³C, ³¹P (¹¹B, ⁷Li, ²³Na, ²⁹Si …)	¹H and ¹⁹F
Sample diameter	4-5 mm	10-26 mm (MQC+23, MQC-R) 40-51 mm (MQC+5)
Line width (homogeneity)	ppb	ppm
NMR spectra acquisition	Yes	No
Sample state	Liquid/Solution	Solid/Liquid/Paste
	Structural elucidation (of simple low mass compounds); Quantitative analysis (using peak areas); Qualitative analysis (spectral fingerprinting); Reaction monitoring (variable temperature 0-65°C, flow); Diffusion and imaging	Hydrogen/Fluorine content; Oil/Fat & Moisture content; Solid Fat Content (SFC); Amorphous/Crystalline content MQC-R only: Mobility and structure (e.g. pore size), diffusion, droplet size and imaging

*Also known as TD-NMR, low-resolution and low-field NMR. The term “low-field NMR” is sometimes used for Benchtop NMR Spectroscopy.

TD-NMR relaxometry experiments can provide information complimentary to that obtained from solid-state high-field NMR experiments, typically performed on a superconducting magnet. Key advantages include simpler experimental protocols and reduced sample preparation.

Since relaxation times depend on magnetic field strength, TD-NMR is sensitive to slower molecular motions that are not accessible at high field. In addition, low-field TD-NMR is less affected by spectral line broadening in heterogeneous or susceptibility-varied samples such as food, biological tissues and porous media (e.g. concrete). As a result, clean relaxation data can be obtained without the need to acquire and interpret NMR spectra.

TD-NMR vs chemical and other physical techniques

Most TD-NMR methods used in QA/QC are intended to replace wet chemical methods, which are time-consuming, labour-intensive, and require skilled operators. In addition to routine applications, TD-NMR offers a range of capabilities for research that complement, and in some cases replace, established material characterisation techniques.

Measurement	Alternative techniques	Advantages of NMR
Composition	Solvent extraction, drying	Measurement without sample alteration, no chemicals needed
Phase transitions	Thermal (e.g. Differential Scanning Calorimetry)	Non-invasive; non-destructive
Pore size distribution	X-Ray CT, N₂adsorption, BET and mercury-porosimetry	Faster, easier and safer; no consumables needed
Mass transport (diffusion, ingress and separation)	UV/visible spectroscopy (of dye), Optical (fluorescent molecules), Electrochemical (in solution)	Applicable to solids and liquids; Direct detection of water (hydration/drying) and other ¹H (or ¹⁹F) containing liquids

Composition

TD-NMR is a suitable alternative to solvent extraction and drying methods for compositional analysis. While conventional chemical techniques often require hazardous reagents and permanently alter the sample, TD-NMR characterises and quantifies 1H and 19F- containing components directly and non-invasively.

Phase transitions

Thermal methods are widely used to measure phase transitions but are restricted in the type of information they provide and typically destroy the sample. In contrast, TD-NMR is non-destructive and is routinely applied to measure phase transitions in food (e.g. fat melting, water freezing), pharmaceuticals (amorphous/crystalline transition), polymers (glass transition), and more.

TD-NMR offers unique advantages for samples containing water, as water acts as the signal source and not as an interference. This enables direct monitoring of hydration and dehydration processes in a variety of different samples, such as agriculture-food products, pharmaceuticals, and building materials.

Pore size distribution

TD-NMR also uses water as a probe molecule to measure pore size distributions in cementitious materials and rocks. It can resolve pore size, surface-to-volume ratio and connectivity under real world conditions, it however requires saturation with water or another solvent. TD-NMR provides additional insights into bound and interlayer water, which makes it a suitable method for linking structure, chemistry, and dynamics at solid-liquid interfaces.

The information obtained with TD-NMR is complementary to that from other techniques. X-ray computerised tomography (CT) visualises solid structure rather than porosity. N2 adsorption measures pore size distribution in the micro- and meso-pore regime, while BET (Brunauer–Emmett–Teller) analysis derives specific surface area from the same data. Mercury porosimetry measures pore size distribution in the meso- and macro-pore regime along with other related parameters but requires high pressure and toxic mercury.

Mass transport

Mass transport analysis often relies on tracers, for example UV/visible or fluorescence spectroscopy using dyes. These approaches probe transport indirectly and are often limited to transparent, liquid systems or to conductive samples in electrochemical methods.

TD-NMR provides the unique capability to directly measure diffusion and mass transport without using tracers, particularly for water, fat or fluorine-containing species in solids, liquids and heterogeneous materials. By measuring restricted diffusion, TD-NMR links molecular mobility to structural length scales, enabling for example the easy assessment of water and fat droplet sizes in emulsions.

Summary

TD‑NMR directly measures hydrogen and fluorine nuclei. This provides several unique capabilities that are difficult to achieve with other chemical, thermal, or optical techniques:

Direct, quantitative water, fat and fluorine measurement

Total water, fat and fluorine content analysis
Differentiation between bound and free water
Assessment of water mobility and confinement

Non‑destructive and non‑invasive

No drying, freezing, vacuum, or sample alteration needed, unless intended
Minimised risk of sample contamination

Applicable to opaque and heterogeneous materials

Polymers, cement, food, biological tissues, rocks, soils

Sensitive to phase changes involving water

Freezing and melting
Hydration and dehydration
Glass transitions (assessed via molecular mobility changes)

Direct measurement of mass transport and diffusion

For ¹H and ¹⁹F - containing species
Including water, oil and fat in a wide range of systems

Fast measurements and minimal sample preparation

Rapid data acquisition and immediate results
Simple and robust experimental setup
Analysis of bulk samples, pastes, gels, and composites

Together, these features make TD‑NMR uniquely well suited to both research and routine quality control applications across a wide range of materials, where many other techniques struggle or introduce artefacts.

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