T heory predicts 1-4 that, with an ultrashort and extremely bright coherent X-ray pulse, a single diffraction pattern may be recorded from a large macromolecule, a virus or a cell before the sample explodes and turns into a plasma. Here we report the first experimental demonstration of this principle using the FLASH soft-X-ray free-electron laser. An intense 25 fs, 4 × 10 13 W cm −2 pulse, containing 10 12 photons at 32 nm wavelength, produced a coherent diffraction pattern from a nanostructured non-periodic object, before destroying it at 60,000 K. A novel X-ray camera assured single-photon detection sensitivity by filtering out parasitic scattering and plasma radiation. The reconstructed image, obtained directly from the coherent pattern by phase retrieval through oversampling 5-9 , shows no measurable damage, and is reconstructed at the diffraction-limited resolution. A three-dimensional data set may be assembled from such images when copies of a reproducible sample are exposed to the beam one by one 10 .X-ray free-electron lasers (FELs) are expected to permit diffractive imaging at high resolutions of nanometre-to micrometre-sized objects without the need for crystalline periodicity in the sample [1][2][3][4] . Structural studies within this size domain are particularly important in materials science, biology and medicine. Radiation-induced damage and sample movement prevent the accumulation of high-resolution scattering signals for such samples in conventional experiments 11,12 . Damage is caused by energy deposited into the sample by the very probes used for imaging, for example photons, electrons or neutrons. At X-ray frequencies, inner-shell processes dominate the ionization of the sample; photoemission is followed by Auger or fluorescence emission and shake excitations. The energies of the ejected photoelectrons, Auger electrons and shake electrons differ from each other, and these electrons are released at different times, but within about ten femtoseconds, following photoabsorption 1,13 . Thermalization of the ejected electrons through collisional electron cascades is completed within 10-100 fs (refs 14,15). Heat transport, diffusion and radical reactions take place over some picoseconds to milliseconds.The effect of X-ray-induced sample damage on the recorded image or diffraction pattern could be substantially reduced, if we could collect diffraction data faster than the relevant damage processes 1,16 . This approach requires very short and very bright X-ray pulses, such as those expected from a short-wavelength FEL. However, the large amount of energy deposited into the sample by a focused FEL pulse will ultimately turn the sample into a plasma. The question is when exactly would this happen. There are no experiments with X-rays in the relevant time and intensity nature physics VOL 2 DECEMBER 2006 www.nature.com/naturephysics
We present results obtained with a novel mass spectrometer capable of determining the mass of multiply charged electrospray ions generated from samples of macromolecules in the megadalton (MDa) size range. The instrument utilizes a sensitive amplifier which can detect the charge on a single ion as it passes through a tube detector. A velocity measurement of an ion with known electrostatic energy provides the ion's mass-to-charge ratio. Simultaneous detection of the ion charge permits a mass assignment to be made for each ion. Electrospray ions of DNA and polymer molecules with masses greater than 1 x 10(6) Da and charge numbers (z) in excess of 425 e(-) are readily detected in this mass spectrometer. The weights of small particles were also measured. The on-axis single-ion detection configuration provides a duty cycle of nearly 100% and extends the practical application of electrospray mass spectrometry to the analysis of very large molecules with relatively inexpensive instrumentation.
In nanotechnology, strategies for the creation and manipulation of nanoparticles in the gas phase are critically important for surface modification and substrate-free characterization. Recent coherent diffractive imaging with intense femtosecond X-ray pulses has verified the capability of single-shot imaging of nanoscale objects at suboptical resolutions beyond the radiation-induced damage threshold. By intercepting electrospray-generated particles with a single 15 femtosecond soft-X-ray pulse, we demonstrate diffractive imaging of a nanoscale specimen in free flight for the first time, an important step toward imaging uncrystallized biomolecules.
The design and operation of a new type of electrostatic ion trap provides simultaneous measurements of mass, charge, and velocity of large electrospray ions. The trap consists of a detector tube mounted between two sets of center-bored trapping plates. Voltages applied to the trapping plates define symmetrically-opposing potential valleys which guide axially-injected ions to cycle back and forth through the charge-detection tube. A low noise charge-sensitive amplifier, connected to the tube, reproduces the image charge of individual ions as they pass through the detector tube. Ion mass is calculated from measurement of ion charge and velocity following each passage through the detector.The device does not use magnetic or radio frequency fields but relies on gating the entrance set of electrodes. Voltages on the entrance plates are initially at ground while voltages on the exit plates maintain a potential gradient appropriate for reflecting the ions. When a highly charged electrospray ion enters the detector tube, its image charge triggers a circuit which enables the entrance plates, thus closing the electrostatic gate to the trap. Individual ions carrying more than 250 charges at an energy of 200 e V /charge have been trapped for 10 ms corresponding to 500 cycles through the detector tube. At this level of trapping time, a theoretical precision for charge measurement as small as 2 electrons RMS can be achieved. The operation of the system is demonstrated by trapping 2.88 megadalton ions of DNA.
BACKGROUND: Current methods for measuring the concentrations of lipoprotein particles and their distributions in particle subpopulations are not standardized. We describe here and validate a new gas-phase differential electrophoretic macromolecular mobility-based method (ion mobility, or IM) for direct quantification of lipoprotein particles, from small, dense HDL to large, buoyant, very-low-density lipoprotein (VLDL).
We present results from experiments at the Linac Coherent Light Source (LCLS) demonstrating that serial femtosecond crystallography (SFX) can be performed to high resolution (~2.5 Å) using protein microcrystals deposited on an ultra-thin silicon nitride membrane and embedded in a preservation medium at room temperature. Data can be acquired at a high acquisition rate using x-ray free electron laser sources to overcome radiation damage, while sample consumption is dramatically reduced compared to flowing jet methods. We achieved a peak data acquisition rate of 10 Hz with a hit rate of ~38%, indicating that a complete data set could be acquired in about one 12-hour LCLS shift using the setup described here, or in even less time using hardware optimized for fixed target SFX. This demonstration opens the door to ultra low sample consumption SFX using the technique of diffraction-before-destruction on proteins that exist in only small quantities and/or do not produce the copious quantities of microcrystals required for flowing jet methods.
The morphology of micrometre−size particulate matter is of critical importance in fields ranging from toxicology to climate science, yet these properties are surprisingly difficult to measure in the particles' native environment. Electron microscopy requires collection of particles on a substrate; visible light scattering provides insufficient resolution; and X−ray synchrotron studies have been limited to ensembles of particles. Here we demonstrate an in situ method for imaging individual sub−micrometre particles to nanometre resolution in their native environment, using intense, coherent X−ray pulses from the Linac Coherent Light Source free−electron laser. We introduced individual aerosol particles into the pulsed X−ray beam, which is sufficiently intense that diffraction from individual particles can be measured for morphological analysis. At the same time, ion fragments ejected from the beam were analysed using mass spectrometry, to determine the composition of single aerosol particles. Our results show the extent of internal dilation symmetry of individual soot particles subject to non−equilibrium aggregation, and the surprisingly large variability in their fractal dimensions. More broadly, our methods can be extended to resolve both static and dynamic morphology of general ensembles of disordered particles. Such general morphology has implications in topics such as solvent accessibilities in proteins, vibrational energy transfer by the hydrodynamic interaction of amino acids, and large−scale production of nanoscale structures by flame synthesi
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