Significance: Cerebral tissue oximetry is imprecise and confounded by an uncertain and variable arteriovenous volume ratio. Venous saturation is better grounded in physiology. The superior sagittal sinus (SSS) is relatively large and placed under the open fontanel on the top of the head in newborn infants. Aim: To enable the development of a dedicated near-infrared-spectroscopy-based cerebral oximeter with sufficient claims on accuracy to be tested for benefit of clinical use. Approach: To set up a research agenda based on the combination of dedicated, high-fidelity digital and physical phantoms. Results: A seven-step path is outlined to identify an optode geometry with high sensitivity to variation in hemoglobin-oxygen saturation in the SSS, with little confounding by changes in the optical properties of the skin and scalp or brain tissue, or in the width of the subarachnoidal space, and that is robust to variations in the placement of the optode. Conclusion: If an oximeter that is designed after exploration of digital phantoms can produce measurements in physical phantoms with good agreement with predictions, it will contribute credibility that cannot be achieved by direct gold-standard validation in newborn human infants. |
1.IntroductionTissue oximetry by near-infrared light applied to the head has a special opportunity when applied to newborn and small infants. Due to their thin scalp and skull, a particularly high proportion of the signal will come from the brain.1 Thus, this can really be called cerebral oximetry. Furthermore, in the clinical field of neonatology, there is a great need for minimally invasive methods of oximetry.2 First, sampling of blood must be minimized due to the small circulating blood volume of the infants. Second, the placement of catheters in blood vessels is difficult due to their small size and risky due to their poor defenses against infection. Third, cardiopulmonary support and intensive care are often required during the transition from intra- to extrauterine life. A large literature describes the clinical research application of cerebral oximetry to elucidate the physiology and pathophysiology of cerebral blood flow and oxygen metabolism in newborn infants. Several oximeters are approved for clinical use in this patient group and two large-scale randomized trials are currently testing the clinical benefits and harms of the combination of monitoring of cerebral oxygenation and a guideline with suggestions of what to do if the cerebral oxygenation drops below a hypoxic threshold.3,4 2.Methodological ProblemsThe precision of transcranial cerebral oximetry is relatively poor. If the optode is lifted off and replaced at a slightly different position on the head, the average difference in reading will be about 5%.5,6 This is high compared to the interindividual standard deviation of cerebral oxygenation in normal newborn infants of 8%,7 or compared to the requirement of an absolute root mean square accuracy of better than 3% for pulse oximetry, another optics-based clinical monitoring technology.8 Tissue oxygenation is not a well-defined concept. The measured value is a weighted average of the hemoglobin saturation in all blood vessels in the optical field. Since driving pressures on the venous side of the circulation is much lower than those on the arterial side, veins need to be larger than arteries and the arterial-to-venous ratio has been estimated to 1:29,10 and to 1:3 and variable.11 This leads to three problems. First, the question of accuracy is not simple, since there is no physiological reference comparable to that of pulse oximetry, where co-oximetry on arterial blood can be considered the gold standard. Calibration and validation of cerebral oximeters therefore typically use desaturation studies in healthy adult volunteers and are based on an assumed, fixed arterial-to-venous ratio.12 Perhaps this is one reason why different devices give widely different values in dynamic blood lipid phantoms13 and during spontaneous deoxygenation in preterm infants.14 Second, if the arterial-to-venous ratio changes during the clinical course, this may be misinterpreted as a change in cerebral oxygenation.11 Third, it reduces the sensitivity of tissue oxygenation to decrease in cerebrovenous oxygenation due low blood flow, e.g., due to hyperventilation, or due to increased oxygen needs, e.g., during seizures, due to “dilution” of the signal with arterial blood of normal oxygenation. Several attempts have been made to measure cerebrovenous oxygen saturation in newborn infants by near-infrared spectroscopy. Tilting the head down or occlusion of the jugular veins on the neck for a few seconds to induce pooling of blood in the cerebral veins has been used to measure the relative increases in oxy- and deoxyhemoglobin by continuous wave spectroscopy.15 Average values in healthy term newborn infants were 65%,16 close to the average normal values in healthy adults. These methods, however, do involve manipulation of potentially sick and vulnerable newborn infants and are not always successful. Analysis of signal changes induced by positive pressure ventilation is also possible and has given similar values17 but has not been explored further, and the analysis of signal changes induced by spontaneous ventilation is often not possible.18 3.OpportunityIn newborn and small infants, the bones of the skull are not yet fused, and the anterior fontanelle on the top of the head is patent for the first year of life. Just below the anterior fontanelle, the two layers of falx cerebri (the fibrous sheath that separates the two brain hemispheres) split into two before it fuses with the periosteum (the fibrous sheath that covers the inside of the bone). The triangular space constitutes a sinus that is filled with venous blood flowing from the superior parts of the hemispheres (Figs. 1 and 2). This sinus can be interrogated at the level of the anterior fontanel, thus avoiding interposing bone and red bone marrow, or more posteriorly through bone, as is usually done for cerebral oximetry. The short distances, the large amount of venous blood, and the well-defined anatomy should make it possible to obtain a nearly purely venous oxygenation and thereby to circumvent the three problems delineated above. This approach, however, has not yet been tried. 4.Limitations of In-Vivo Calibration and ValidationIt is not ethically permissible to sample blood from the superior sagittal sinus (SSS) in newborn infants although this was routinely done at the outset of modern neonatology. Even cannulation of the internal jugular vein cannot be done for a research purpose, and catheterization of veins on the neck is rarely done for clinical purposes in newborn infants, so opportunistic blood sampling cannot be planned on a large enough scale to obtain statistically firm estimates of accuracy. The brains of experimental animals, such as piglet or lambs, are considerably smaller than the brain of human infants, and although the anatomy of the SSS is similar, the differences in size will subtract significantly from the value of validation in these animals. 5.Definitive Role for PhantomsHigh-resolution imaging is possible by ultrasound as well as MR, therefore precise three-dimensional anatomy can be defined and used for building physical phantoms as well as in-silico models of photon propagation (digital phantoms). Only short source–detector distances need to be examined, so the overall size of the phantoms can be small. Comparison of results from physical and digital phantoms and exploring and possibly resolving any significant differences may enhance the trust in the validity of the results. 6.Challenge of Anatomical VariabilityOne challenge for the translation of results from phantom work to the application of an instrument on patients or research subjects is the anatomical variability. A digital phantom study of the reliability of frequency-domain NIRS across the age span from birth to adult age used MR images to model the “superficial layer” (i.e., skin-scalp-bone + subarachnoidal space), subarachnoidal space, and brain tissue.1 Compared with children below 1 year of age, with a thin scalp and skull, a very attenuated response to changes in the absorption coefficient () in brain tissue was demonstrated in adults and larger children. By chance, perhaps, one of the MR images of a young child used for this study displayed an open sylvian fissure (a space of subarachnoidal fluid in the parietotemporal region), just under the row of detectors. The Monte-Carlo simulations demonstrated how this space attenuated the sensitivity to changes of in brain tissue. The variability of the development of gyration of the brain and closure of the Sylvian fissure is well known. Although there is less variation at the top of the hemispheres, near the SSS, the width of the subarachnoidal space does differ among infants.20 The width increases with growth and development of preterm infants, and furthermore, infants born very preterm when 4 to 8 weeks old have wider subarachnoidal space compared to infants with the same biological age, but born more recently. The average width in the first scan was 1.5 mm, with an upper limit of the “normal range” of 4 mm, while in the latest follow-up scans the mean value was 3 mm and the upper limit of the normal range was 6 mm. The head circumference ranged from 220 to 340 mm. Similarly, the thickness of skin, bone, and the subarachnoidal space has been studied over the temporoparietal region. The thickness of skin varied from 1 to 3 mm and bone from 1 to 5 mm.21 Digital phantom work has previously demonstrated that superficial layers with a thickness up to 6 mm do not significantly affect the measurement of brain oxygenation.22 7.Phantom Research AgendaAn agenda for developing a device to measure oxygen saturation in the SSS in newborn and small infants could include the following.
8.Next StepsGold-standard verification in human infants is impossible, but alternative in-vivo methods are available. One option is to compare with the results of the methods based on brief obstruction of venous outflow from the brain, as described above. Many years ago, two different methods of measuring cerebral blood volume by continuous wave near-infrared spectroscopy revealed significant differences.24 Another way is to examine the “construct validity,” i.e., to compare measured responses to expected responses to stimuli for which there already is good evidence for the magnitude. For instance, the validity can be examined by comparing the absolute changes between this measure of cerebrovenous saturation (in %) and arterial blood saturation (in %) as monitored by pulse oximetry during spontaneous variations in oxygenation, which are common in preterm infant due to periodic breathing or frank apnea.25 When arterial oxygen saturation stays within the normal range, compensatory changes in cerebral blood flow or cerebral metabolism of oxygen are not expected26 and arterial and venous saturation is expected to occur in parallel. This has been used to measure cerebral blood volume and flow in newborn infants using “oxygen as a tracer.”15 Also, robustness against changes in venous pressure can be examined. Spontaneous changes in intrathoracic pressures happen during ventilatory support, and these are expected to cause passive dilatation of cerebral veins, but not to affect cerebrovenous saturation. These comparisons, however, will all be far from ideal, and thus the validation obtained by phantom studies will be of great value, and can potentially contribute significantly to the trust in a venous oximeter. 9.ConclusionGood agreement between the performance of an “SSS oximeter” as predicted from digital phantom evidence and actual performance on a series of physical phantoms with realistic variations in anatomic features and in optical properties could contribute significantly to the credibility of the accuracy of such an oximeter. DisclosuresThe author has provided advice to manufacturers of cerebral oximeters but has not received any fees and does not hold any patents or shares in medical device industry beyond what may be included in his bonds portfolio at any time. The author is employed at a public hospital and as such wants clinically valuable medical devices available to patients at affordable prices. The author is the coordinating investigator of the SafeBoosC-project that is testing the clinical value of commercial cerebral oximeters in newborn infants. ReferencesM. Dehaes et al.,
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BiographyGorm Greisen is a professor and consultant neonatologist. His research has focused on causes of brain injury in preterm infants, cerebral blood flow and cerebral oxygenation, systematic follow-up studies to evaluate outcomes later in life and interventions in the newborn period to improve health later in life. He is currently engaged in an attempt to test the clinical value of monitoring cerebral oxygenation in newborn infants with a group of neonatologists in 18 European countries. |