Here is a paper that delves into biophotonic communication and presents a fascinating view of human physiology. A must-read for all who are interested.
Biofield Physiology: A Framework for an Emerging Discipline - link
Biofield Physiology: A Framework for an Emerging Discipline - link
Abstract
Biofield physiology is proposed as an overarching descriptor for the electromagnetic, biophotonic, and other types of spatially-distributed fields that living systems generate and respond to as integral aspects of cellular, tissue, and whole organism self-regulation and organization. Medical physiology, cell biology, and biophysics provide the framework within which evidence for biofields, their proposed receptors, and functions is presented. As such, biofields can be viewed as affecting physiological regulatory systems in a manner that complements the more familiar molecular-based mechanisms. Examples of clinically relevant biofields are the electrical and magnetic fields generated by arrays of heart cells and neurons that are detected, respectively, as electrocardiograms (ECGs) or magnetocardiograms (MCGs) and electroencephalograms (EEGs) or magnetoencephalograms (MEGs). At a basic physiology level, electromagnetic activity of neural assemblies appears to modulate neuronal synchronization and circadian rhythmicity. Numerous nonneural electrical fields have been detected and analyzed, including those arising from patterns of resting membrane potentials that guide development and regeneration, and from slowly-varying transepithelial direct current fields that initiate cellular responses to tissue damage. Another biofield phenomenon is the coherent, ultraweak photon emissions (UPE), detected from cell cultures and from the body surface. A physiological role for biophotons is consistent with observations that fluctuations in UPE correlate with cerebral blood flow, cerebral energy metabolism, and EEG activity. Biofield receptors are reviewed in 3 categories: molecular-level receptors, charge flux sites, and endogenously generated electric or electromagnetic fields. In summary, sufficient evidence has accrued to consider biofield physiology as a viable scientific discipline. Directions for future research are proposed.
INTRODUCTION AND OVERVIEW
The impetus to frame a new area of physiology often arises at the interface of existing fields of inquiry. As prime examples, neuroendocrinology emerged when nerve endings in the hypothalamus, near the base of the brain, were observed to release hormones that cue the anterior pituitary to regulate an array of endocrine tissues; psychoneuroimmunology emerged when the phenomenon of conditioned immunosuppression was observed and when nerve endings were discovered adjacent to lymphocytes in secondary lymphoid tissue; cognitive neuroscience came into its own when correlates of mental processes began to be identified by means of increasingly sensitive brain imaging techniques. We suggest that biofield physiology, with its initial focus on the characterization of endogenous electrical and magnetic fields as indices of health and illness—eg, via electroencephalography or magnetoencephalography (EEG and MEG) or electrocardiography and magnetocardiography (ECG and MCG)—represents another such confluence of disciplines, integrating concepts and information from cell biology, biophysics, and medical physiology.
Biologically-generated fields (biofields) are a spatially distributed set of forces and physical properties that have the capacity to encode information and exert instructive influences on cells and tissues capable of perceiving and being modified by them. As such, complement molecular processes as key contributors to what biophysicist Mae-Wan Ho, PhD, describes as global coherence—the multilevel integration of diverse biological activities across time and scale. In her view, global coherence—the defining quality of living organisms—accounts for their most salient properties such as long-range order and coordination, rapid and efficient energy transfer, and extreme sensitivity to specific signals.
Although we focus in this paper on fields generated by living systems, there is substantive scientific literature demonstrating that physiological regulatory systems in humans and animals are also affected by and even synchronized to environmentally generated fields, eg, of geomagnetic and solar origin. Of additional interest, disruptions in these fields have been observed to create adverse effects on health and behavior. A companion paper in this supplement reviews evidence for the therapeutic use of externally applied electrical and magnetic fields (see Muehsam, et al, this issue). For example, a recent Cochrane review concludes that pulsing electromagnetic field therapy “may offer some benefit in the treatment of delayed union and non-union of long bone fractures,” a finding supportive of the US Food and Drug Administration approval of such therapeutic usage.
Given that electrical and magnetic fields, as well as biophotons in the full range from ultraviolet to infrared are detected during normal physiological activity, the question often arises whether such endogenous phenomena are merely epiphenomena of metabolic events or are incompletely understood biological signaling systems. The present paper explores the evidence for the latter view. We suggest physiological regulatory systems are affected by biofields in a manner that complements the more familiar molecular-based mechanisms, by which regulatory systems respond to endogenous biochemical signals and exogenous pharmacological agents.
We begin our article by describing known and postulated biofields, including how they are generated and which physiological systems may be affected. Next, we consider receptor systems that may detect, integrate, and trigger responses to both biofields and environmental fields. We conclude by identifying areas for future research aimed at clarifying form and function of biofields. Overall, a case will be made that sufficient evidence has accrued to consider biofield physiology as a viable, if nascent-stage, scientific discipline that is likely to expand the current biomedical model of health and disease.
BIOFIELDS: FORM AND FUNCTION
Every region of the body, however superficial or deep, is crisscrossed with well-studied communication and regulatory systems, including neural pathways, blood-borne hormones and exosomes (cell-derived vesicles), and immune surveillance. Yet the existence of fluctuating endogenously generated electromagnetic and other fields, which also suffuse all our cells and comprise an additional rich source of biological information and regulation, remains an underappreciated aspect of physiology.
Electrical activity, in the form of charge separation, is a fundamental feature of every living cell. As single cell and multicellular organisms evolved in a primordial sea, the ability to maintain a low-sodium/high-potassium intracellular milieu, in the face of the high-sodium/low-potassium concentrations in sea water, served as a source of energy to enable uptake of metabolites and discharge of waste products across the cell surface. Proteins, evolved to serve as specific ion channels and pumps, maintain this ionic gradient (the “resting potential”) between inside and outside of each cell.
But evolution found greater promise for the resting potential than merely as an energy source for ion pumps and crossmembrane transport of molecules. As multicellular organisms evolved, patterns of resting potentials of cells throughout the body became designated as instructive scaffolding to guide pattern formation and stem cell behavior during embryogenesis and organ regeneration. For example, endogenous arrays of bioelectric potentials are now known to instruct left-right patterning, eye induction, size regulation, and patterning during complex organ regeneration. New tools allow these bioelectric gradients to be directly observed noninvasively in vivo and to be specifically altered to assess effects on intercellular communication and tissue-level or organ-level outcomes. Importantly, the molecular mechanisms that couple changes in bioelectric gradient distribution to downstream transcriptional and epigenetic targets are also being characterized.
Further, as the advent of multicellular organisms led to increased cellular specialization, muscle and nervous tissue developed mechanisms to turn their resting potentials into high-speed action potentials, propagating along the cell surface with frequencies and other characteristics that encode information. Passage of this information from cell to cell via chemical and electrical synapses expanded the effective area of these electrical fields. Transmembrane currents in neurons also produce local electric fields that induce “ephaptic coupling” (nonsynaptic electrical coupling) between adjacent axons, which influences the synchronization and timing of action potential firing in neurons. As further examples, various types of electrical fields—created by either mechanical stress (piezoelectricity) or streaming potentials—in bone, tendons, skin, and fascia are thought to regulate the functioning of osteocytes and fibroblasts to adjust the density of supporting tissues in response to loads. Also, electric fields generated by the intracellular network of microtubules, centrosomes, and chromosomes appear to play fundamental roles in regulating the dynamics of mitosis, meiosis, and a variety of other cellular activities.
In addition to the high-speed electrical signals conducted along nerve axons, a second communication network, based in ubiquitous epithelial cells, conducts information as slowly varying direct currents. The DC fields generated by this system, which spread across considerable distances, play key roles in recognizing damage and guiding cell migration necessary for wound healing (especially in skin, heart, and cornea) as well as in regulating the migration of neuronal path-finding. Recent research has identified numerous molecular signaling pathways that mediate the interactions of these bioelectric fields, first described decades ago with the plasma membrane and cytoskeletal mechanisms to facilitate tissue repair.
Although the transepithelial DC fields and the gradients of resting membrane potentials (Vmem) share functional similarities, the DC fields are produced only by epithelial layers in a relatively standardized form, while Vmem are generated by all cells in a wide variety of patterns. A further difference lies in the transduction mechanisms of these systems. The Vmem patterns are sensed by a different set of membrane proteins from those that respond to the DC fields. Cells use both systems during morphogenesis: the DC fields set directionality of growth and positional information and the Vmem gradients control differentiation and proliferation and establish anatomical identity of whole regions.
Since electric charge in motion, whether along a wire or a nerve axon, produces a magnetic field in the surrounding space, this phenomenon represents a further type of biofield. Magnetic fields emanating from the body, although extremely weak relative to the geo-magnetic field of the earth, are readily detected by superconducting quantum interference device (SQUID)–based magnetometers. Evidence has recently been summarized that nonthermal electromagnetic fields of amplitude similar to the cardiac field can affect a wide variety of biological functions, including gene expression, particularly in stem cells.
The strongest rhythmic electrical and magnetic fields in the body are produced by synchronous activity of heart muscle cells. While the ECG is readily detected via surface electrodes, the heart's magnetic field can be recorded up to several feet from the body surface as an MCG. Magnetic fields produced by the heart appear to carry information that can also be detected by other persons or animals. An example of the informational potential (bioeffectiveness) of these heart fields is cardiac-induced entrainment, or frequency locking, detected when the R-waves of one subject's ECG become precisely synchronized with the onset of EEG alpha waves of another subject at a distance of up to 5 feet. Heart fields may also encode psychoemotional information, as indicated by the 75% accuracy rate in detecting discrete emotional states from patterns of heart rate variability.
The electrical and magnetic fields generated by the composite activity of thousands of brain cells are detected as an EEG and MEG, respectively. At a functional level, the electromagnetic activity of neural assemblies has been proposed to modulate neuron synchronization71 and circadian rhythmicity72 and to underlie the computational and cognitive processes of the brain. More specifically, weak sinusoidal electric fields appear to enhance and entrain physiological neocortical network activity. Thus, in a feedback loop, the local fields help to synchronize the neural network that generates them.
Another type of biofield phenomenon is the coherent, ultraweak photon emissions (UPE), detected from cell cultures and from the body surface. Since the initial observations of UPE or biophotons were detected from inflammation-producing reactive oxygen species, the level of these emissions has been explored as a noninvasive marker of “metabolic stress” and a measure of overall health. More broadly, such UPE, instead of being considered as metabolic epiphenomena, may serve important physiological roles.
A role for ultraweak light signaling in normal physiological regulation is suggested by evidence of intercellular communication under chemically separated but optically coupled in vitro conditions, eg, through a thin glass film. These studies have identified infrared as a primitive source of “cellular vision” to guide migration and other behaviors. More recently, a role for biophotons in neural activity was based on observations that fluctuations in UPE correlate with cerebral blood flow and cerebral energy metabolism as well as with EEG activity. Moreover, photonic stimulation at one end of a nerve appears to elicit increased UPE at the other end. As a means of information transfer, biophotons have the advantages of extremely high speed and the ability to penetrate into and through cell membranes and organs that present barriers to the diffusion of molecular signals. Nonconventional means of UPE-mediated biosignaling include wave propagation within longitudinally-oriented neuronal microtubules and passage through membrane-spanning regions of proteins that may serve as “light pipes.”
Considerations of physiological activity of biofields also include resonance signaling, ie, the modulation of cell function by specific electromagnetic frequencies. Involvement of nonclassical and quantum forms of energy (eg, A-fields and scalar waves) has not been explored to the same level of rigorous detail as the bioelectric gradients and fields discussed above, and physiological roles for such phenomena have not yet been demonstrated. (See the article “Biofield Science: Current Physics Perspectives” in this Supplement for a more extensive discussion of non-classical and quantum forms of energy.)
BIOFIELD RECEPTOR SYSTEMS
A further challenge for framing a physiology of biofields is to identify endogenous receptor systems that detect electromagnetic or other types of fields and trigger responses to these nonmolecular stimuli. While the concept of receptor brings to mind the conformational matching invoked to characterize receptor-mediated responses to hormones and drugs, biofield reception may be better described by phenomena from physics, such as resonance and impedance matching, based on tuning to signal frequencies. As previously proposed, overlapping categories of biofield receptors can be considered: molecular-level receptors, charge flux sites, and endogenously generated electric or electromagnetic fields.
An important series of studies on cultured cells identified examples of the first type of receptor sites—deoxyribonucleic acid (DNA) and the cell membrane—at which exogenous electromagnetic signals exert specific biological effects. Just as steroid hormones upregulate transcription of particular genes by binding to hormone response elements of DNA, so do low-frequency (<300 Hz) electromagnetic fields appear to increase transcription of select genes by acting at upstream regions of DNA designated as electromagnetic response elements (EMRE). Deletion of the EMRE eliminates the ability of the applied electromagnetic field to regulate the target genes, while other genes can be converted from electromagnetic nonresponders to responders by inserting the EMRE at upstream regions. Similar electromagnetic fields, as demonstrated by the same researchers, appear to increase the activity of several membrane-bound enzymes.
Charge flux sites, the second type of receptor as exemplified by the perturbation of transmembrane calcium fluxes, have been proposed as a generic mechanism by which weak electromagnetic fields affect biological systems. If voltage sensitivity of calcium ion (Ca2+) channels facilitates the targeting of these sites by electromagnetic fields, voltage-modulated channels for other ions should also be tested as potential target sites. Low-frequency electromagnetic fields have also been proposed to interact with DNA by accelerating the movement of electrons within the helical arrays of base pairs. Changes in charge separation in small DNA regions occur during aggregation, so that interactions may be more pronounced in specific active segments of DNA.
While ion channels and ion pumps have major roles in establishing the resting potential of an individual cell, it is gap junctions, the specialized electrical connections between adjacent cells, that allow voltage and current-mediated signals to be propagated across groups of cells. In this manner, spatiotemporal patterns of resting potentials arise to provide bioelectrical guidance during tissue development, regeneration, and cancer suppression. Although it is not yet apparent that applied weak electromagnetic fields can alter resting potentials, let alone affect multicellular patterns of membrane voltage, applied weak electrical currents do appear to induce regeneration of adult frog limbs. These exogenously applied currents are comparable in direction and density to the outward electrical currents detected from regenerating amphibian limbs, and it is possible that some of the reported effects of applied electromagnetic fields are due to modification of endogenous bioelectric gradients.
A final candidate for a receptor system for endogenous and exogenous biofields is a body-wide network that appears to exhibit all 3 types of potential receptor sites: molecular, charge flux, and endogenous field. Unspecialized ‘‘loose'' connective tissue, often referred to as fascia, forms a continuous head to toe network surrounding and permeating all tissues and organs. As an extracellular matrix, structured mainly by collagen fibers, fascia provides a supportive and regulatory framework for all organs of the body as it coordinates cellular perception and interpretation of mechanical forces. This extracellular system reaches into the interior of cells via transmembrane bridging molecules known as integrins, which allow information from the fascia to modify cell metabolism and genetic activity. Speculation on the nature of such collagen-signaling focuses on water molecules hydrogen-bonded along the outer shell of the collagen triple helix, oriented in a manner that supports the rapid jump conduction of protons along the length of the collagen fibers. Since collagen structures both conduct and modify photon pulses emitted from biological sources, it is conceivable that signaling along collagen fibers serves as a surveillance system of endogenous biofield emission to complement the immune and nervous systems in monitoring tissue health.
Further speculation based on the water-protein relationship along collagen fibers invokes quantum coherence, a state that can occur when all water molecules in a particular domain or region are spinning synchronously, emitting spin or torsion waves. Such spin coherence and quantum coherence enable the collagen matrix to be ultrasensitive to electromagnetic fields in a manner that can be frequency selective due to a quantum phenomenon known as the Larmor Precession. This effect, resulting from the torque of an external magnetic field exerted on the spin of subatomic particles, is the basis of magnetic resonance imaging (MRI).107
Known sensitivities of organisms to extremely small environmental cues, including visible light and electromagnetic fields, merit consideration in this overview of biofield receptors. These sensitivities—which evolved, for example, to locate prey, avoid predators, navigate, and sense changing weather patterns—often operate at or near limits set by physics. An exemplar is the ability of the retina to detect a single photon of light, which occurs via calcium channel–mediated signal amplification and allows thousands of calcium ions enter a retinal rod in response to an individual photon. The public health debate concerning potentially harmful effects of electromagnetic fields was influenced for decades by the conventional physics doctrine that living systems could only be affected by energy strong enough to cause ionization or heating of tissues. In contrast, evidence that very weak, nonionizing electromagnetic fields exert biological effects is well documented, and the history of the shift away from the thermal model has been chronicled. Finally, German researchers have demonstrated that individual molecules can act as transmitting and receiving antennae in the mediation of efficient inter-molecular communication via single photons.
CONCLUSIONS
Sufficient evidence has accrued to consider biofield physiology as a viable scientific discipline, based on nonlocal, integrated, information-conveying phenomena as well as on emerging molecular details of localized biophysical interactions. Endogenously generated pulses of ultraweak photons, electromagnetic fields directly related to cardiac activity, and patterns of distributed membrane voltage are varied forms of physiological activity designated as biofields, each with established properties and proposed biological functions. Several receptor systems have been identified that mediate responses to these biofields. By analogy with the hormones, receptors, and regulatory functions that comprise endocrinology, components of the biofield physiology framework are in place.
In seeking to define biofield physiology as an area of research, it is helpful to distinguish it from the existing discipline of bioelectromagnetics and to consider the 2 approaches as different phases of a continuum. If bioelectromagnetics is more about defining mechanisms of local interactions, then biofield physiology is more about understanding the integrated, longer-range functions within the whole organism: the former more reductive, the latter more integrative.
Biofield physiology is still at an early stage of formation. While it is incontrovertible that biological systems emit and react to a wide range of energetic influences, we have not achieved a detailed understanding or mathematical modeling of the essential field aspect of such interactions (a prerequisite for exploiting their long-range organizing properties). Moreover, many of the experimental findings are preliminary, while the biofields studied are varied in form and cannot yet be considered as interrelated representatives of a clearly defined system of biological self-regulation. Further, much of the research appears guided by existing paradigms of biochemistry and physiology. As one example, evidence of DNA response elements that respond to specific electromagnetic frequencies, analogous to DNA regions responsive to specific hormones, is an important finding. However, biofields may also act in a more dispersive, nonspecific manner to activate self-regulatory systems that, in turn, stimulate surveillance to detect the source of tissue imbalance or disease. As future research is likely to reveal, such imbalances may be understood via models based on either molecular-level or biofield-level dysfunction, a perspective that will further expand diagnostics, treatment options, and our concepts of physiology.
