Myopia (near-sightedness) is the most common refractive vision disorder in children. It is characterized by blurring of objects viewed at a distance, and is commonly the result of abnormal elongation of the eyeball – which causes the refractive image formed by the cornea and the lens to fall in front of the photoreceptors of the retina (Fig. 1).
The underlying biological cause of myopia is unknown, and there is no widely accepted means of prevention or cure. The optical error of myopia can be corrected only by using spectacle or contact lenses or corneal surgery. If left untreated, moderate myopia is one of the leading causes of visual impairment worldwide. The greater the degree of myopia, the greater the risk of complications such as macular degeneration, retinal detachment, cataracts, and glaucoma ; the risk is especially great when the negative refractive error is more negative than -6.00 D (diopters), a condition called ‘high myopia’. The prevalence of myopia varies greatly, depending on ethnicity, geographical location, and socioeconomic status, but is rising rapidly in most populations studied  (Fig. 2). Myopia is a centuries-old problem, and although we have made great progress in scientific investigation of its underlying cause, we have been unsuccessful in preventing it from becoming named by the World Health Organization as an ever-increasing global health concern .
Clinical Aspects & Health Care Burden
There are two clinical designations for myopia: pathological degenerative myopia, and spontaneous-onset or school age myopia. Pathological myopia is characterized by rapid, extreme axial elongation of the globe, leading to a high refractive error (typically far more negative than -6.00D). This extreme stretching puts stress on the ocular structures (retina, choroid, and sclera), which can then result in degenerative changes in the eye (Fig. 3), and irreversible vision loss. Fortunately, pathological myopia is relatively rare, affecting 0.9-3.1% of the population .
The most common form of myopia is school-age myopia; this is the form that will be discussed in this chapter, and it will be called simply “myopia” from this point on. It progresses slowly, and usually stabilizes by the age of 20. The retina looks normal. Recently, is has been projected that 2.5 billion people (1/3 of the world’s population) will have some degree of myopia by 2030 .
2. Genes may play a role in development of Myopia
Myopia prevalence varies greatly in different ethnic and geographical populations . Recent studies of American preschool children (aged 6–72 months) revealed a prevalence of 1.2% in non-Hispanic whites, 3.7% in Hispanics, 3.98% in Asians, and 6.6% in African Americans [5-6]. Among older children, the difference between Asian and Caucasian populations is obvious; a study of Australian adolescents reported prevalence of 42.7% in 12 yr old and 59.1% in 17 yr old children of East Asian ethnicity, compared to 8.3% in 12 yr old and 17.7% in 17 yr old children of European Caucasian descent .
There have been attempts to identify genes that may be important in myopia development. “Genome-wide association studies” (GWAS), which examine genetic variations between individuals to determine whether certain variants are associated with a specific trait (in this case myopia), have identified correlations between variations in certain genes and an increased risk of myopia. The recently published Consortium for Refractive Error And Myopia (CREAM) study is the largest international genome-wide meta-analysis on myopia and refractive error ever conducted. It is based on data from 32 studies encompassing Europe, the United States, Australia and Asia . Twenty-four genomic variations were associated with up to a 10x increase in risk of myopia. These genetic variations are involved in many apparently unrelated ocular functions, instead of a single underlying system or structure. Thus, the CREAM study provided significant evidence that the risk of developing myopia may be affected by many unrelated genetic abnormalities, instead of a single underlying cause (Fig. 4).
Twin studies and parental myopia studies have also been conducted to try to assess the role of genetics in development of myopia (review9). Twin studies have reported that the correlation of prevalence of myopia was significantly higher in identical twins than fraternal twins [9-11]. Age and the methods used to gather and analyze the data are important, however, as myopia correlations determined by such studies can range from r = 0.11 (low correlation) to r = 0.94 (high correlation) . There is strong evidence to suggest that increased risk of myopia is highly correlated with the number of myopic parents [12-16], and that this risk is independent of environmental factors [12,13]. One problem with twin and familial studies, however, is that few of them bothered to control for environmental factors that would be likely be shared among family members – for example, the likelihood that identical twins engage in the same activities in a much higher frequency than fraternal twins or non-twin siblings.
It is reasonable to assume that genes play a part in myopia risk, but they alone cannot account for the rapid changes in myopia prevalence that are being observed all over the world, nor for the dramatic differences in myopia prevalence within the same ethnic populations – in urban vs. rural environments, for example [2,17]. Thus, the underlying cause of spontaneous-onset myopia is most likely to be a combination of genes and environmental triggers. Most of the identified risk factors for myopia are correlated with environmental influences, such as an increased socioeconomic status, residing in an urban environment, higher education and IQ, increased time spent performing near work, and increased time spent indoors [1,18]. These risk factors are based on observations of human populations over many decades, but they do not provide a mechanistic explanation as to why they are associated with an increased risk of myopia.
To understand the roles of environmental risk factors for the cause of myopia (which are difficult to study in human subjects under stringently controlled conditions), scientists have turned to animal models. The results have demonstrated clearly that, while genetics may determine myopia susceptibility (e.g.: age of onset, rate of progression, ultimate refractive error), environmental factors are powerful modifiers of eye growth, and they may override genetic predispositions. For a comprehensive review on the biological basis and mechanisms of the eye’s self-regulation of growth see, “Homeostasis of eye growth and the question of myopia”, by Wallman & Winawer .
3. Animal models of myopia: What we see conrols how the eye grows
The first reported case of myopia in experimental animals was observed serendipitously in non-human primates, during investigations into the cortical effects of monocular visual deprivation in young macaques. In these animals, sewing the eyelids shut for many months resulted in high levels of myopia20; the longer the period of visual deprivation, the greater the resultant refractive error21. The establishment of this “form-deprivation” model of myopia in primates led to parallel studies of experimentally-induced myopia in young tree shrews  and chickens . Instead of sewing the eyelids shut, scientists now use frosted plastic goggles to induce deprivation myopia, or lenses with a strong negative power to cause “lens-induced myopia”  (Fig. 5). Today, the most commonly-used myopia model animals are chicks and guinea pigs, but tree shrews, non-human primates, and mice are also studied .
That we can experimentally-induce myopia in young, rapidly growing animals tells us that the visual environment plays an important role in regulation of eye growth. Applying goggles over the eye works even when the optic nerve has been cut, which tells us that the eye alone – or more specifically, a specialized sensorineural tissue in the eye called the retina – can discriminate whether the image is well focussed or not, and act locally to mediate optically-induced changes in eye growth [19,26,27]. Affixing a frosted goggle or negative lens over the eye causes excessive axial elongation of the eye, and myopia, but affixing a positive lens over the eye causes inhibition of axial elongation, and far-sightedness (hyperopia) (Fig. 6). The complementary effects of positive and negative defocus reveal that the eye – most probably the retina itself – can discriminate between positive and negative defocus, as well as between unfocussed blur (form-deprivation) and blur due to negative lens treatment, even though the static images produces by the two different treatments appear very similar (Fig. 5, b vs. c). We do not know whether eye growth is controlled by two different signals, one “start” and one “stop”, operating in push-pull fashion (like turning the steering of an automobile to left or right) – or by a single signal that increases elongation (“grow” or “on”) or decreases it (“stop” or “off”) (like increasing or decreasing pressure on the accelerator pedal of an automobile). We also do not know the identities of these hypothetical “start” or “stop” growth signals, but a number of signalling substances have been identified that are very strong candidates for “eye growth regulators” (discussed in greater detail below).
Myopia-inducing stimuli require prolonged exposures (days-weeks) for a significant effect. In the chick, however, it takes only ≥2 hrs per day of unobstructed viewing of a richly textured visual environment to completely block the development of form-deprivation myopia , and positive-lens wear for only 2 min, four times per day, is enough to block lens-induced myopia . In addition, the eye can “recover” from experimentally induced myopia and return to an emmetropic refractive state, if the animal (or human) is young enough. Once an organism has reached adulthood, however, there is no known way to decrease the size of the globe, without surgical intervention.
4. Inhibiting accomodation des not prevent myopia
Perhaps you are familiar with the old wives’ tale, “Don’t sit too close to the TV, or you’ll ruin your eyes!”. This is likely because the most common and longstanding hypothesis about the cause of myopia development was that excessive near work results in accommodative fatigue, which then causes myopia. Accommodative fatigue occurs when the ciliary muscle weakens due to overexertion – as arm or leg muscles would – in response to an entire day of heavy lifting. Weakening of the ciliary muscle would result in loss of the focussing power of the lens, leading to hyperopic defocus when objects are viewed up close (Fig. 7). As discussed previously in the section about animal models of myopia, hyperopic defocus (pushing the plane of focus behind the photoreceptors) can be a stimulus for eye growth.
To investigate whether reducing the need for accommodation in children would be preventative against myopia, scientists have utilized progressive-addition lenses (PALs). In principle, the use of PALs should allow accommodation (contraction of the ciliary muscle) to relax, while keeping a blur-free image on the retina  (Fig. 8).
“The Correction Of Myopia Evaluation Trial” (COMET) was the largest and most significant human clinical trial ever conducted to test whether relaxation of accommodation through the use of PALs could help to inhibit the progression of myopia in children. It was a multicenter, randomized, double-masked, controlled clinical trial that took place over a period of three years (n = 469 children). At the end of the study, a statistically significant 3-year mean difference was found in children who wore PALs versus single vision lenses (SVL) (refractive error progression: PAL: −1.28 ± 0.06 D vs. SVL: −1.48 ± 0.06 D, p = 0.004; axial length elongation: PAL: 0.64 ± 0.02 mm vs. SVL: 0.75 ± 0.02 mm, p = 0.0002). These data supported the hypothesis that changes in accommodation can affect myopia progression. Unfortunately, this effect was too small to be considered clinically significant, although one subset of children – those who had high accommodative lag – seemed to benefit significantly from PAL wear (Fig. 9). Subsequent studies have confirmed these findings , reporting a statistically significant, but small, reduction in myopia progression in children wearing PALs versus SVLs; these effects were not dependent on accommodative lag, as high-lag children had similar results as others. The accumulation of experimental evidence from animal models and further human trials, however, does not support a significant role of accommodation in myopia development . It remains possible that most PAL-wearers in the COMET study did not use the lenses properly, but tolerated the blur that resulted from accommodative fatigue and continued near-work without adjusting viewing angle for better focus.
A second hypothesis is that accelerated eye growth can occur because of over-correction of myopic refractive error (similar to lens-induced myopia). To test this hypothesis, children were under-corrected by +0.5 to +0.75 D. This trial therapy was largely unsuccessful; myopia progressed more rapidly in under-corrected children than in fully-corrected controls [33-34]. Interestingly, a recently published study  reported that myopia and axial elongation progressed more rapidly in fully under-corrected than in fully corrected myopic children. This held true even when controls were applied for other risk variables, such as baseline refractive error and axial length, number of myopic parents, age at myopia onset, and time spent doing near work and outdoors . Thus, there is still no consensus on whether under-correction may be an effective anti-myopia therapy.
5. Intense outdoor light protects against myopia
n recent years, spending time outdoors has been reported to reduce the risk of developing myopia, and this effect does not seem to be dependent on the amount of physical activity [36-37]. We do not yet know the mechanisms through which outdoor light might protect against myopia, but some ideas are that it might (a) stimulate intensity- or wavelength-dependent anti-myopia systems in the retina, (b) cause sustained pupillary constriction via the melanopsin system – thus improving retinal image quality by reducing longitudinal aberrations, (c) increase the production of vitamin D in the skin, (d) increase the average viewing distance of objects outdoors compared to indoors, thereby reducing accommodative fatigue, or (e) increase the activation of spatiotemporal image-response mechanisms in the retina, which inhibit myopia development. For a recent review on the roles each of these factors may play in myopia, please refer to “The role of luminance and chromatic cues in emmetropization” by Frances Rucker . For more information about the melanopsin system, refer to the Webvision chapter “Melanopsin-expressing, Intrinsically Photosensitive Retinal Ganglion Cells (ipRGCs)” by Dustin M. Graham and Kwoon Y. Wong.
When Rose et al. studied the effects of time spent outdoors on the development of myopia in Australian children, they found that children who spent more time outdoors had lower associated myopic refractive errors than children who spent most of their time indoors, even after adjusting for near-work, parental myopia, and ethnicity . Exercise versus leisure did not affect associated levels of myopia (Fig. 10).
Therefore, it was proposed that the higher mean illuminance (light intensity) outdoors – which can be as much as 100,000 lux in Sydney AU, compared to typical indoor values of 350-500 lux – was responsible for the protective effect of outdoor activity against myopia progression. Human pilot studies to test this hypothesis have been successful in inhibiting myopia, in a small cohort of Chinese schoolchildren  and in a larger cohort of Australian schoolchildren . High-intensity light is also protective against experimentally-induced myopia in monkeys [41-42] and chicks [43-44]. The mechanism through which intense light may prevent myopia is unknown, but we can use animal models to investigate the signalling molecules that may be involved. There are substantial links to the up-regulation of neuromodulators such as dopamine  and nitric oxide . These neurotransmitters are strongly correlated with myopia-inhibition on their own [47-48], and they may also work together in the same myopia-inhibiting pathway .
During emmetropization, the eye needs some sort of visual cue to determine the direction of blur , and chromatic aberrations have been suggested as a possible cue . The most common chromatic aberration is longitudinal chromatic aberration (LCA), in which different wavelengths of light are focussed at different distances along the same axis (Fig. 11).
In humans, the fovea is most densely populated with medium- and long-wavelength-sensitive cones. One idea is that the eye should be guided to grow to a size at which middle wavelengths in the visible spectrum (yellow-green, 550-570nm) will be the most sharply focussed, with the highest contrast, to attain the highest possible spatial acuity. If this were the case, the in-focus image of an eye that is too small will be blue-shifted, with high contrast at short-wavelengths (450-470 nm), whereas the in-focus image of an eye that is too large will be red-shifted with high contrast at long-wavelengths (610-630 nm) (Fig. 12).
The results of research on the effects of LCA on emmetropization in the eye show that it is sufficient to detect the direction of retinal blur , but it does not seem to be necessary for emmetropization [52-54]. Despite this, many studies have demonstrated clearly that the chromaticity (spectral composition) of light can be an important modulator of eye growth, although its effects do not seem to be the same in all animal models. In chickens raised without goggles or lenses, short-wavelength (blue) light retards eye growth, whereas long-wavelength (red) light promotes it; white light (which contains all spectral wavelengths) has no effect . In chicks wearing monocular diffusers, long-wavelength illumination (achieved using filters) is myopia-promoting, while short-wavelength illumination is myopia-inhibiting (Ghodsi & Stell , and Nguyen & Stell, unpublished studies; Fig. 13). Form-deprivation myopia in guinea pigs also responds to narrow-band long- or short-wavelength exposure in the same way as chicks [57-59]. In contrast, long-wavelength light is growth-inhibiting and short-wavelength light is growth-promoting in rhesus monkey  and tree shrew (Gawne et. al. ). Thus, further investigations are needed to explore the effects of light spectrum on myopia development and to identify the underlying retinal mechanisms, in various animal models.
Retinal circuitry and ocular pathways of myopia
Emmetropization is an active-feedback process, guided by visual cues. It aims to match the axial length and resting focal power of the eye in such a way that images of objects viewed at any distance, can be focussed onto the retinal photoreceptors by accommodation .
Past studies indicate that the retina is the primary source of signals that regulate eye growth19, while pathways involving transmission between retina and brain, via the optic nerve, may play roles in focal refinement of the visual image . The retina is a highly specialized neural tissue that lies at the back of the eye (Fig. 14).
Although evidence suggests that the retina is the source of ocular growth-regulating signals19, we do not know the specific cell types involved in emmetropization. There is no evidence for the direct involvement of horizontal cells, but destruction of photoreceptors (PRs) and/or amacrine cells (ACs) in the chick retina has been associated with increased axial growth of the eye [63-64]. Given the broad-spectrum action of toxins on retinal neurons, the relative roles of PRs and ACs in myopia-control in these types of studies are not well-defined, and molecular tools which would disrupt function of retinal cell types more specifically than toxins, are not widely-researched or available in chicks, the most common myopia model organism. Animals in which molecular tools are currently available – such as mice – are less suitable for studies of eye growth because their eyes are extremely small. This makes it very difficult to measure accurately any changes in axial growth or refractive error. This drawback of the chick model may change with a new genome-editing technology called CRISPR [65-66], which is an exciting development in the myopia-research field. Delivery of gene-silencing agents to cells in the retina of hatched chicks presents challenges that we have still not overcome (Waldner D, et al. IOVS 2017; : ARVO E-Abstract 5905).
That is not to say that myopia experiments in mice have not been performed. Genetic “knockout” mice models – in which their genome has been edited to “remove” certain retinal cell types or visual processing mechanisms by causing mutations – were used to determine the contributions of rods, cones, and retinal ON-pathways (some bipolar cells) to emmetropization . Eyes of mice with mutations causing severe degeneration of rods and cones (rd1-/- & rd10-/-) were more susceptible to form-deprivation myopia than those of their wild-type (unmanipulated) counterparts  (Fig. 15), while the eyes of rod-specific knockout Gnat1-/- mice, which exhibit little retinal damage, were unresponsive to form-deprivation . Eyes of mice with a mutation in nyctalopin (Nyxnob/nob) – a protein important in ON-bipolar cell signalling – exhibited an increased susceptibility to form-deprivation myopia .
This led the authors to conclude that perhaps rod-mediated signalling in the retina is more important for emmetropization than cone-mediated signalling. This revolutionary concept is supported further by the fact that rod photoreceptors signal primarily through ON-bipolar cells, which likely mediate the effects of the injected glutamate analog, L-APB, on eye growth in chicks . Furthermore, rods vastly outnumber cones in most mammalian retinas, including those of mice and humans; and vision with high spatial resolution, which is not mediated by rods, is not necessarily required for the retina to successfully detect blur [19-72]. It is possible that the transgenic ablation of rod-ON-BCs could have damaged the inner-retinal circuitry that produces myopia-STOP signals, and the ability of mice with intact rods, but no cones, to develop FDM has not yet been investigated. Thus, we would hope to see further evidence in support of this counter-intuitive hypothesis.
Ganglion cells, and therefore cortical visual pathways, do not seem to contribute significantly to homeostatic eye growth, even though ganglion cell axons make up the optic nerve. Disconnection of the optic nerve – either by surgery or toxins – has little effect on emmetropization and/or compensation to induced defocus26, [73-75], and eyes will still respond to deprivation myopia . Retinal efferent (centrifugal) fibres also run through the optic nerve, in birds and other animals. Unilateral lesioning of this system, while leaving retinal ganglion cell axons intact, results in hyperopia in the eye contralateral to the disrupted fibre tract. By 21 days after surgery, however, the eyes return to an emmetropic state  – suggesting, perhaps, that the initial hyperopic shift was due to short-term release of neuroactive substance(s) such as NO from the retinal axon terminals of the damaged cells, or retrograde signalling within the retina by axotomized RGCs. There is a precedent for a process such as this in the induction of rod-precursor proliferation in goldfish, which can be elicited by sectioning of the optic nerve and ablation of olfactory bulb/tract – the source of efferent fibres in fish . Many studies do not report intra-ocular effects of treatment, even though direct retino-retinal connections have been shown to exist in rats and mice [78-79].
Amacrine cells are the visual processing powerhouses of the retina, and the most likely source of retina-derived eye growth-regulating molecules . There are as many as 30 different confirmed subtypes of amacrine cells, and it is likely that more remain to be discovered [80-81]. The majority of amacrine cells provide inhibitory feedback to bipolar cells via GABA- and glycine-mediated signalling; but they can also contact and provide feedback to other amacrine cells and ganglion cells [81-82], as well as release neuromodulatory substances that modify properties such as excitability, gain, synaptic transmission, and cell-cell coupling of many retinal neurons and circuits, through non-synaptic mechanisms. They are responsible for higher-level processes in the retina such as detecting environmental changes in movement , contrast, and blur . For more information on amacrine cell function, see the Webvision chapter “Roles of Amacrine Cells” by Helga Kolb.
Many studies have shown that various signalling molecules found in amacrine cells can affect myopia onset and inhibition [47,85-89], such as dopamine , nitric oxide , and neuropeptides (VIP, glucagon, somatostatin, and neurotensin) . Destruction of subpopulations of amacrine cells by toxins has significant effects on normal eye growth and induction of form-deprivation myopia [63,64,90-92]. The functions of most amacrine cells identified remain to be discovered, but the contribution of specific amacrine cell-derived signalling molecules to emmetropization and myopia inhibition will be discussed in more detail below. Most likely, signalling molecules originating from the retina do not control eye growth directly; instead, they are assumed to act via a signalling cascade that relays eye growth-regulating signals through the RPE and choroid, which may then release different signalling molecules that directly affect scleral growth  (Fig. 16).
6. Muscarinic acetylcholine receptors, dopaine, and nitric oxide are strongly implicated in regulation of eye growth
Muscarinic Acetylcholine Receptors (mAChRs)
Muscarinic receptors in the eye mediate contraction of the pupillary constrictor muscle, as well as the ciliary muscle, which controls accommodation. As discussed previously, it was long thought that myopia inhibition could be achieved by blockade of accommodative fatigue. However, the failure of clinical trials such as COMET (discussed above), plus experimental evidence from animal models, does not supported the hypothesis that mAChR antagonists (blockers) inhibit myopia via paralysis of the ciliary muscle alone32. Chicks can develop experimentally-induced myopia and/or respond to treatment with drugs such as atropine or pirenzepine – which block muscarinic receptors [93-94] – even though their ciliary muscles are controlled by nicotinic receptors, which atropine and pirenzepine do not target. Pirenzepine inhibits the progression of myopia in humans [95-97] and a wide range of animal species  including monkey [98-99], tree shrew [100-102], and chick [94,103-105], even though it has little effect on iris and ciliary musculature [99,102,103,106,107]. Finally, lesioning of the ciliary nerve does not impair development of either form-deprivation or lens-induced myopia; chicks with damaged ciliary nerves develop similar amounts of myopia as intact controls .
These data have largely ruled out accommodative activity or the ciliary muscle as an important eye-growth-regulator; thus, we have turned to the retina, choroid, or sclera as possible target sites for myopia-inhibition by mAChR antagonists. Muscarinic receptors are present in the retina, RPE, choroid, and sclera . Fischer et al. localized chick mAChR orthologues (cM2, cM3, cM4) in chick eye tissues and showed that immunoreactive sites are present in the inner retina (cholinergic amacrine cells and ganglion cells), retinal pigment epithelium (RPE), and choroid, as well as the ciliary body . Expression patterns in the tree shrew , and rabbit  are similar to those reported for the chick (Fig. 17). However, even though there is evidence for mAChRs in the ocular tissues, it remains uncertain exactly which ocular tissues, cells, or receptors mediate the anti-myopia effects of mAChR antagonists. The theorized mechanism of action of myopia-inhibition by these drugs is heavily dependent on the assumption that they block signalling through mAChRs, but this has never been proven conclusively.
In fact, substantial evidence argues for a non-retinal or non-muscarinic mode of action . For example, only some muscarinic antagonists inhibit myopia in humans [95,96,115-117] and animals [101,104,118], while the vast majority have no effect ; high concentrations of these drugs are required for a significant effect. Protein and mRNA expression studies utilizing radioligand binding and real-time PCR techniques have found no change in receptor density or receptor gene expression for any mAChR subtypes in the retina or choroid of chick  or tree shrew , even when there is significant myopia development. This is strange, as it would be expected that significant changes in eye growth should cause changes in the expression of target receptors. Interestingly, amacrine cells that make the neurotransmitter required for action by mAChRs (acetylcholine) do not seem to be required for emmetropization, development of experimentally-induced myopia, or atropine-mediated suppression of form-deprivation myopia . This is again very strange, because ‘orthosteric’ mAChR antagonists such as atropine should have no action by themselves; they simply block access of the signalling neurotransmitter to the target receptor. Thus, if myopia inhibition by atropine is mediated by mAChRs, atropine should not inhibit myopia if the source of acetylcholine has been destroyed.
These data support a few possible theories: The first is that the cells responsible for myopia inhibition by mAChR antagonists are not in the retina, but instead in the RPE, choroid, or sclera. When muscarinic antagonists are administered by injection into whole, intact eyes, this is a possibility. For a drug to have a significant effect on a system, it must be present in a certain concentration at the receptor for binding and activation to occur. The inverse of this effective concentration is called ‘potency’. Atropine is a very potent drug; thus, it requires an extremely low concentration to block mAChR signalling (1-10 nM). If it were working at a target far away from the intravitreal injection site (i.e., the choroid or sclera), the requirement for a large concentration of drug could be justified; it is possible that only a small amount of atropine might reach its target, through loss by diffusion through the vitreous, and/or blockade by the RPE and blood-retinal barrier. If the target tissues (retina, choroid, sclera) are isolated, however, the requirement for large concentrations of drug should be eliminated, because these barriers have been removed. One study examining the effects of mAChR agonists (stimulators) and antagonists on eye cups consisting of the RPE/choroid/sclera (in vitro; retina removed) demonstrated that stimulation of mAChRs by carbachol, oxotremorine, arecadinine, and pilocarpine resulted in choroidal thinning, and that pirenzepine caused choroidal thickening; atropine was not tested, and oxyphenonium had no effect . Another study on the effects of atropine on isolated scleral cells found that it can slow proliferation, which would be expected if atropine inhibited myopia by directly affecting scleral growth. Unfortunately, however, because the concentrations of drugs used in these isolated tissues were very high (0.6-5 mM), neither study conclusively indicates a non-retinal origin for mAChR-control of eye growth control.
A second possibility is that high concentrations of mAChR antagonists are required for myopia inhibition because these drugs are not acting at mAChRs, but instead at some other, unknown receptor. All drugs are “dirty”, or promiscuous, meaning they can, and will, bind to unintended receptors; the risk of this “off-target” or “non-specific” binding increases as the concentration of drug increases. In the case of myopia-inhibition, extremely high concentrations – up to one-million times greater than those required for binding (1 mM used vs. 1 nM required; see above) – are used routinely. Thus, it’s no great stretch of the imagination to speculate that when drugs are used at concentrations such as these, they will act in ways we cannot accurately predict. To determine whether “off-target” binding of mAChR antagonists is possible, we conducted in vitro experiments using isolated human mAChR M4 receptor (M4), chicken mAChR M4 receptor (cM4), and human alpha2A-adrenoceptor (hADRA2A). Our hypothesis was that myopia-inhibiting mAChR antagonists would bind to hADRA2A – an “off-target” receptor – when applied at high concentrations. We found that myopia-inhibiting mAChR antagonists bind to hADRA2A when applied at concentrations similar to those expected to be present when these drugs are used to treat myopia in the chick model (0.001-1 mM)104, while mAChR antagonists that do not inhibit myopia did not bind to this receptor with any significant activity, or at all. Interestingly, the correlations between the ability of mAChR antagonists to bind to M4/cM4 receptors and their reported ability to inhibit myopia in chick  were very poor, whereas correlations between mAChR antagonist binding at hADRA2A and myopia inhibition in chick were significantly better (Fig. 18).
Of additional importance were our findings regarding the experimental anti-myopia ligand, MT3, a polypeptide isolated from venom of the green mamba snake. Recently, it has been reported that MT3 inhibits myopia in chicks at concentrations significantly lower than those required for atropine (2.5-10 μM vs. 1-100 mM, respectively) [122,124]. MT3 is known to be selective for mammalian mAChR M4 over all other mAChR subtypes . Thus, the authors of these studies claimed that because MT3 inhibits myopia at a much lower concentration than atropine, mAChR M4 must be the “myopia-controlling” receptor. However, in our studies, we found that MT3 is the least potent antagonist of all tested at the chicken (cM4) receptor – 56x less potent than at human M4 (Fig. 19). This disconnect between MT3-potency at cM4 and its rank as the most potent anti-myopia ligand in the chick – and the fact that MT3 binds with high potency, not only to mAChR M4, but also to alpha1A-, alpha1D-, and alpha2A-adrenoceptors [126,127] – casts further doubt on the theory that M4/cM4 are the target receptors that mediate inhibition of myopia by muscarinic antagonists.
These data are preliminary, however, and should be interpreted with caution. They do not prove a role for alpha2A-adrenoceptors in control of eye growth. Rather, they disprove M4/cM4 as a likely target, and offer alpha2A-adrenoceptors as one possible alternative out of many – including other subtypes of mAChRs. There is some evidence for a role of alpha-adrenoceptors and their neurotransmitters, norepinephrine (NE) and epinephrine (E), in the eye. NE and E are the primary neurotransmitters in the sympathetic nervous system, from which the superior cervical ganglion originates. This ganglion projects to the eye and controls processes such as pupil dilation via the iris dilator papillae, reduction of ocular blood flow via vasoconstriction, and regulation of intraocular pressure via control of aqueous humor outflow . A few studies have localized alpha-adrenoceptors in these ocular tissues, which is not surprising, but these receptors also seem to be present in the retina [129,130]. One hypothesized role of alpha2-adrenoceptors in the retina is that they might be involved in regulation of dopamine synthesis [131-133]. There is strong evidence that dopamine is a very important molecule in myopia-inhibition and regulation of eye growth (see below). Confirming these studies, and expanding upon them, may help to refine whether there is alpha2-adrenoceptor-mediated signalling in the retina, whether it can affect retinal dopamine regulation, and possibly identify cell types that might be involved. Confoundingly, although there is evidence for the presence of alpha2-adrenoceptors and the enzyme phenylethanolamine N-methyltransferase (PMNT) – which converts NE into E – in the retina, there is no significant evidence that either NE or E act as a retinal neurotransmitter . For now, the function and activating transmitters of the alpha-adrenoceptors in the retina remains largely unknown. Significant further investigation will be required to determine whether these receptors are a worthy target for anti-myopia therapies.
Dopamine is perhaps one of the most-studied neurotransmitters in regards to regulation of eye growth. For an in-depth review of the studies investigating the effects of dopamine and dopaminergic systems on myopia, please see “An updated view on the role of dopamine in myopia” by Feldkaemper and Schaeffel  and “Dopamine signaling and myopia development: What are the key challenges” by Zhou et al. .
Dopamine is a catecholamine neurotransmitter/neuromodulator that acts as a light-adaptive signalling molecule in the retina . It is synthesized in and released from tyrosine hydroxylase-containing amacrine cells. Intravitreal injection of dopamine agonists is strongly correlated with inhibition of eye growth [47,88,136-144] (Fig. 20), while injection of dopamine antagonists before unrestricted vision prevents myopia rescue .
In addition to a direct role of dopamine agonism on inhibition of myopia in chicks, retinal dopamine levels and subsequent effects on myopia are sensitive to modulation by other drugs. Myopia-prevention by the cholinomimetic agent diisopropylfluorophosphate  and mamba toxin-3 in chick , and mamba toxin-7 (MT7) in tree shrew , can be blocked by dopamine antagonism. Interestingly, intravitreal injection of atropine or in vitro application of atropine to the chick retina causes increased levels of dopamine metabolite DOPAC and retinal dopamine release , and like atropine , myopia-inhibition by dopamine is blocked by simultaneous injection of nitric oxide synthase inhibitors [49,149]. Interestingly, the effects of dopamine agonists and muscarinic antagonists are not additive . This led the authors to suggest that acetylcholine and dopamine may act at different points of a common pathway to prevent myopia; further investigation into this hypothesis has not been undertaken.
Nitric oxide (NO) is a small-molecule gas that can act as a non-conventional neurotransmitter and neuromodulator in the retina. It is difficult to image NO directly, because it is volatile and chemically unstable. Consequently, past studies utilized histochemical activity of the enzyme NADPH-diaphorase  and antibody-labelling of NO-synthesizing enzymes (nitric oxide synthase, NOS) to determine the localization of NO action in tissues. NADPH-diaphorase activity and immunoreactive neuronal NOS (nNOS, NOS-1) are found in subpopulations of all major cell types in the chick retina and choroid, and at least 15 types of identified retinal neurons [151,152]. Direct imaging of NO has been accomplished by means of an indicator molecule that fluoresces after reacting with NO , which has been used to refine further the localization of various NOS isoforms, and where NO may act in the retina [154,155].
The investigation of the role of NO as a regulator of eye growth is still in its early stages, but preliminary results are promising. Non-specific inhibitors of NO synthesis, L-NAME  and L-NMMA , cause transient thinning of the choroid – a change correlated with myopiagenesis. Blockade of NO synthesis with L-NAME abolishes the rescue effect of unoccluded vision , and experiments in mice have verified that pharmacological blockade of NO synthesis increases myopia susceptibility ; this further implicates NO as a possible “stop” signal for eye growth. Finally, intravitreal injection of drugs that cause increased levels of NO in chick retina and RPE, dose-dependently inhibited the development of form-deprivation myopia (Fig. 21).
The mechanism of NO-mediated prevention of myopia remains to be elucidated. Increased retinal NO acts as a signal for light-adaptation [160-163], and retinal NO synthesis is increased under intense illumination . NO donors in dark-adapted chicks mimic the adaptational effects of increased illumination , while NOS inhibitors mimic the effects of decreased illumination in light-adapted chicks . Thus, increased NO may be a possible mechanism by which high-intensity environmental illumination protects against myopia. In addition, NO inhibits cell-cell coupling via gap junctions in the retina , and uncoupling of gap junctions containing connexin-35/36 (Cx35 in chicks) – which sharpens spatial tuning of retinal function – has also been implicated in myopia-inhibition  (Teves et al. .
Although we do not know the receptors through which atropine may act, we do know that myopia-prevention by atropine is also dependent on induction of nitric oxide (NO). Simultaneous injection of atropine with nitric oxide synthase inhibitors – which blocks the ability of cells to make NO – completely abolishes all protective effects of atropine in chicks  (Fig. 22).
7. Many other molecules can affect eye growth
Adenosine Receptors and 7-methylzanthine (7-MX)
7-MX is a caffeine derivative, which has some affinity to adenosine receptors. Recent clinical trials of 7-MX have provided evidence that it may be useful in combatting axial myopia . Children with a fast base-line rate of myopia progression, fed daily tablets containing 400mg 7-MX for >2 years, experienced slowing of axial elongation and myopia progression compared to placebo controls. This myopia-inhibiting effect halted as soon as 7-MX treatment was discontinued. The mechanism through which 7-MX may prevent myopia is currently unknown, but there are two working hypotheses: (i) that it causes stiffening of the sclera, which prevents axial elongation [169,170]; or (ii) that it blocks adenosine receptors in the retina and/or ciliary muscle, and consequently causes changes in acetylcholine and dopamine neurotransmitter release .
Recent studies have shown that alpha2-adrenoceptor agonists can inhibit form-deprivation myopia in the chick . Intravitreal injection of high concentration clonidine (200 nmoles) or guanfacine (20-200 nmoles) significantly inhibited changes in refractive error and axial elongation (Fig. 23). These studies are appealing, because the alpha2-adrenoceptor agonist brimonidine is already approved for use in humans, as a glaucoma treatment . Thus, it would be much easier to translate these findings into a clinical trial than it would for experimental ligands such as mamba toxin-3. These data are very preliminary, but could yield new pharmaceutical targets for anti-myopia therapies lacking the negative side-effects of atropine treatment.
Gamma-aminobutyric Acid (GABA)
Gamma (γ)-aminobutyric acid (GABA) is the primary mediator of inhibitory synaptic transmission in the central nervous system (CNS). For more detailed reviews of the localization and function of the GABA in the retina, please see previous Webvision chapters, “Neurotransmitters in the Retina” by Helga Kolb, and “GABAC Receptors in the Vertebrate Retina” by Haohua Qian.
There is significant evidence that GABA receptors are involved in the regulation of eye growth. Daily intravitreal injections of a wide variety of GABA receptor antagonists into form-deprived eyes resulted in reduction of eye growth (mostly in the equatorial dimension) . One of the most effective anti-myopia GABAergic drugs is the GABAAOr/C antagonist (1,2,5,6-Tetrahydropyridin-4-yl)methylphosphinic acid (TPMPA), which has been shown to significantly inhibit goggle-induced myopic refractive error, vitreal chamber depth, and equatorial diameter in the chick  and guinea pig [175,176]. Novel GABAAOr/C drugs cis- and trans-3-ACPBPA also inhibit lens-induced myopia in chicks, the cis form being much more potent . How GABAAOr/C antagonists may inhibit myopia is not known, and GABA can be expected to play a role in practically every visual processing mechanism in the retina; but there is some evidence of interaction with retinal dopaminergic systems, in the particular , as well as possible effects on scleral glycosaminoglycans .
Growth Factors: TGF-β and bFGF
Transforming growth factor-beta (TGF-β) and basic fibroblast growth factor (bFGF) seem to operate in a push-pull manner to regulate scleral growth during experimentally-induced myopia. Intravitreal injection of bFGF in chicks is protective against myopia, and co-administration of TGF-β with bFGF blocks this effect . In the guinea pig, Chen et al. confirmed that bFGF prevents experimentally-induced myopia. They also reported that bFGF protein expression was decreased, while TGF-β expression was increased, in scleral tissues of eyes that had undergone light induced myopia for extended periods of time (15-30 days) . The mechanism of bFGF-mediated myopia inhibition has not been elucidated. Attempts were made to link bFGF with the dopaminergic system, because bFGF protein content is upregulated during light and it is co-localized with tyrosine-hydroxylase – the cell marker for dopaminergic amacrine cells . However, other studies revealed that the two pathways are likely not related .
Peptide Hormones: Glucagon and Insulin
Glucagon is a pancreatic peptide hormone whose best-known role in mammals is to raise the concentration of glucose in the blood; insulin, another pancreatic peptide hormone, plays the opposite role – to lower blood sugar levels. However, many (perhaps all) gut peptides and their receptors are also expressed by neurons in the central and peripheral nervous systems, where they presumably play neuromodulatory roles. Glucagon-positive cells in the retina consist of a subset of amacrine cells in the inner retina of birds and reptiles, about 40% of which are also GABAergic [182,183]. The activity of glucagon amacrine cells in the chick retina changes dramatically in response to defocus, as revealed by changes in these cells’ content of an activity-inducible transcription factor, early growth response protein 1 (EGR-1 or ZENK). Positive-lens defocus, or removal of the diffuser after inducing form-deprivation myopia, causes stronger and more widespread labeling of EGR-1, whereas negative-lens defocus or form-deprivation results in little or no labeling . The activity-dependent induction of Egr-1 is best interpreted as an indicator of cell depolarization, and therefore is an indicator of increased transmitter release. Egr-1 is likely to upregulate the transcription of genes whose products are important in functional compensation for prolonged increases in cell activity, rather than directly to affect downstream actions of the activated cell such as those involved in myopia-inhibition.
In the chick, injection of a glucagon agonist into form-deprived eyes inhibits myopia development , and injection of a glucagon antagonist blocks myopia recovery from clear vision . Intravitreal injection of insulin has the opposite effect, acting as a powerful myopiagenic agent . Glucagon inhibits the development of myopia in chicks, even after most amacrine cells have been ablated by neurotoxins, suggesting that (in chicks at least) glucagon amacrine cells could be the final or near-final output of “stop” signals acting on the RPE (Beloukhina N, et al. IOVS 2005; 46: ARVO E-Abstract 3337).
The relevance of these interesting findings in the chick model to the control of refractive development in mammalian eyes remains uncertain. A comparable role of glucagon in the retina of mammals remains elusive. To date, glucagon has not been identified or localized in any mammalian retina; and although many other members of the glucagon polypeptide family are present, their expression is not changed upon treatment of the eyes with form-deprivation stimuli. However, other kinds of amacrine cells, which have been labelled by similar focus- and defocus-dependent induction of Egr-1 in macaque monkey [188,189] and tree shrew (Stell WK, et al. IOVS 2004; 45: ARVO E-Abstract 1159) are plausible candidates for playing similar roles in the control of eye growth.
Retinoic acid (RA) is member of the retinoid family of compounds, which also includes Vitamin A. Retinoic acid stands out among other candidate regulators in the control of eye growth, because its levels are bi-directionally modulated in response to opposing defocus stimuli [190-193]. In the chick, retinal and choroidal RA levels and mRNA expression of its synthesizing enzyme, aldehyde dehydrogenase-2 (AHD2), are predictably changed in response to defocus stimuli; increasing in response to negative defocus and decreasing in response to positive defocus [192-194]. Treatment of form-deprived chicks with a blocker of RA synthesis, disulfiram, caused myopia inhibition, but this effect was not carried over in response to lens-induced myopia . RA might act as a regulator of eye growth by inducing changes in scleral extracellular matrix  or modulating cell-cell coupling [196,197].
7. Choroidal changes correspond to changes in eye growth
Although the origin of homeostatic growth-regulating signals is most likely the retina, experimental and therapeutic treatments may affect any target within other ocular tissues – the retinal pigment epithelium (RPE), choroid, and/or sclera most likely. It is unlikely that a single kind of molecule is responsible for transmission of growth-regulating signals, because of difficulties in crossing the occluding junctions of the RPE (a major component of the blood-retina-barrier), and drug loss due to protein binding and dilution of the drug during en route transport into cells. More likely, a cascade of molecules may relay signals from retina-to-RPE, RPE-to-choroid, and then choroid-to-sclera (Fig. 16).
Interestingly, the choroid responds to induced defocus in a compensatory fashion  – thickening in response to myopic defocus (positive lenses, removal of myopia-inducing goggles) and myopia-inhibiting treatments [121,156-158,199], and thinning in response to diffusers or hyperopic defocus (negative lenses) (Fig. 24). Whether the directional changes in the choroid are responsible for scleral changes in eye growth – or just an initial compensatory step/by-product of other mechanisms that are themselves the primary regulators – remains to be determined, although the authors of a recent study have reported that changes in choroidal thickness are not predictive of changes in eye growth in eyes with experimentally-induced myopia200. Nevertheless, it may be assumed that the choroid should play some role in the regulation of ocular refraction and/or the cause(s) and prevention of myopia , and that it may be the source of growth-regulating signals that act on the sclera .
8. Human Therapies and Recommendations for Myopia Prevention
Pharmaceutical Interventions: Atropine
Although many neurotransmitter/neuromodulator agonists and antagonists have been investigated for their ability to control eye growth, very few laboratory discoveries have been translated into clinical therapies. The most widely used pharmaceutical agent, atropine, was championed almost 40 years ago by Bedrossian  and subsequently became the subject of numerous clinical trials and scientific scrutiny. In 2006, Chua et al. published the results of the Atropine in the Treatment Of Myopia (ATOM) study . This was a two-year, comprehensive, randomized, placebo-controlled, double-blind trial of 346 Asian children to determine the effectiveness and safety of daily 1% atropine eye drops for the prevention of myopia progression. ATOM was significant in that it was one of the first clinical trials with double-blind and placebo-controlled groups, which provided a much more objective measurement of the effects of atropine for human myopia. The outcomes revealed that atropine significantly reduced the mean progression of myopic refractive error: 84% of placebo-treated children experienced myopic progression of -0.5 D or more, while only 34% of atropine-treated children experienced the same (Fig. 25). No serious adverse effects were reported, but the common side-effects – photophobia, glare, allergic reaction, and headaches caused by blurred vision – caused some children to drop out. In addition, a subset of children experienced a “rebound effect”, in which myopia returned and progressed much more rapidly after atropine-treatment had ceased . Chia et al.  repeated the ATOM study (ATOM2), using lower concentrations of atropine (0.5%, 0.1%, and 0.01%) for two years, and found that the drug retained most of its efficacy at these lower concentrations. Minimal side effects were reported, but many children continued to suffer from blurred vision, conjunctivitis, and eyelid dermatitis at the higher concentrations. The “rebound effect” was also still present in the higher-concentration treatment groups (0.5% and 0.1%) .
In an attempt to address the rebound effect, the study was repeated, but with a different treatment schedule . Children were treated with 0.5%, 0.1%, or 0.01% atropine for two years, and then treatment was discontinued for one year to see whether rebound would occur. Treatment was restarted only in children who experienced myopic progression of -0.50 diopters or more in at least one eye, and then continued for another two years. It was found that there was an inverse dose-related increase in myopia by the end of phase 2 (period with no treatment – ‘wash-out’) caused by rebound, resulting in the greatest effect of the 0.01% treatment group. Children requiring a second round of atropine-treatment were 24%, 59%, and 68% for the 0.01%, 0.1%, and 0.5% groups, respectively. Results from the second round of treatment confirmed that the most effective concentration of atropine was 0.01%; children treated with 0.01% atropine had the least rebound during the wash-out period, but still experienced significant inhibition of myopia-progression during treatment (Fig. 26). Side-effects for the 0.01%-treatment group were mild – only minimal pupillary dilation, minimal loss of accommodation, and no significant loss of near-vision – compared with those at the higher concentrations.
Corneal-Reshaping Lenses: Orthokeratology
Orthokeratology (Ortho-K, Overnight Vision Correction, Corneal Refractive Therapy) uses gas-permeable contact lenses, worn and night and removed during the day, to temporarily reduce refractive errors. The lenses reshape the cornea while the user is sleeping, are removed in the morning, and refractive correction is maintained well throughout the day. Not only does Ortho-K correct myopia without drugs or surgery, but clinical trials of Ortho-K have demonstrated a strong correlation between Orth-K treatment and inhibition of myopia progression . The Longitudinal Orthokeratology Research in Children (LORIC) study, in Hong Kong, was a non-randomized two-year pilot study that investigated the ability of overnight Ortho-K lens wear (i) to correct myopic vision, and (ii) to slow the progression of myopia (n=35) . Positive results from this small pilot study led to the first larger-scale, single-masked, randomized clinical trial named the Retardation Of Myopia In Orthokeratology (ROMIO) study , in which 78 children (37 Ortho-K, 41 controls) took part for two years. The children wearing Ortho-K lenses experienced significantly slower axial elongation during the study than those wearing single-vision lenses, and at the end of the treatment period had significantly shorter eyes (Fig. 27). Some children (5) did drop out of the study for ocular health reasons related to lens-wear, but their vision was not permanently affected once Ortho-K treatment was stopped. The mechanism by which orthokeratology inhibited myopia progression remains unclear, but studies have suggested that Ortho-K lenses may induce relative peripheral myopia, as well as increases in spherical aberration and amplitude of accommodation210. However, alternative mechanisms – such as neurally mediated reflex control of ocular elongation or corneal curvature – have not yet been ruled out.
Alternative Strategies: High Environmental Illuminance
Human trials investigating the effects of high-intensity outdoor light on myopia prevention have so far been very promising [37,39,40] (Fig. 10). Sending children outdoors is by far the least invasive treatment-option currently available. In countries where the intensity of outdoor light is generally lower, because of air pollution or short duration of natural daylight – such as Canada or Scandinavia in the winter, or Beijing year-around – sunlight therapy could be supplemented in the form of SAD lights (approved and used for Seasonal Affective Disorder), which have an output of ~2,000-10,000 lux and are sold to combat depressive symptoms brought on by seasonal affective disorder. This alternative will become even more attractive, when the spectral region responsible for myopia-prevention in primates has been identified.
9. Where do we go from here?
The world is experiencing a “myopia boom” , and viable treatment options are becoming more crucial than ever before. Atropine is considered to be the best pharmaceutical treatment we have. It is the only one currently available, and is rather widely accepted and used, despite remaining off-label for the purpose of treating myopia. Advocates of atropine use would claim that the occurrence of unwanted side-effects and its unknown mechanism of action are not serious enough drawbacks to warrant discontinuation of therapy. Unlike atropine, single-vision lenses do not prevent continued myopia progression, which can lead to blindness-inducing vision problems later in life; and overall, topical atropine-treatment in children has been proven to be effective and quite safe. Parents should be aware of the most common side effects: possible photophobia due to pupil dilation, impairment of near-vision due to paralysis of the ciliary muscle, allergic reactions, and rebound after cessation of treatment. It should also be noted, that not all children will respond to atropine-treatment .
It is imperative to determine the mechanism through which atropine inhibits myopia, because a better agent might be found. Ideally, an agent as effective topically as atropine, but completely lacking the unacceptable side-effects of even 0.01% atropine eye-drops – mild photophobia, blur, and allergies. There is evidence that mAChRs may not be the receptors that mediate myopia-inhibition , and learning the true targets could effectively eliminate atropine’s three most common side-effects. Lowering the required concentrations or treatment frequency could mitigate the allergic reactions caused by daily atropine use, and using a non-mAChR-specific drug would eliminate both photophobia and loss of accommodation, which are mediated by known target receptors of atropine (mAChRs).
Retrospective reviews have been performed to determine the safety and efficacy of Ortho-K lens-wear; however, although gas-permeable Ortho-K lenses have been determined to be quite safe [207,212], caution is still advised. Long-term use of these lenses may be required, which can increase the risk of microbial keratitis, and discontinuation of use has resulted in a rebound effect similar to that seen in pharmacological treatments of myopia [204,205,210]. Recently, a study was performed that combined the anti-myopia effects of atropine (0.01%) and Ortho-K. The authors reported that combining the two therapies resulted in a significantly greater effect than Ortho-K treatment alone . Long-term studies on the safety and efficacy of cornea-reshaping lenses are vital; whether overall eye health can be maintained while using lenses that change eye shape by applying a significant amount of physical pressure to corneal cells for many hours every day remains to be determined.
Outdoor-light therapy may offer the ideal treatment for myopia. Not only does encouraging children to play outside and combat other major health concerns – such as childhood obesity, juvenile diabetes, and depression – but also, light therapy presents little to no serious health concerns or side-effects compared to those of other available myopia-treatments. Exposure to potentially-harmful UV radiation can be avoided by wearing UVA/UVB-blocking sunglasses and sunscreen. Alternative light sources such as commercially available SAD lights do not contain UV-radiation, and have been shown to be nearly equally effective in myopia-prevention in animal models. This approach seems to be particularly promising, if further testing of non-human primates, followed by clinical trials, confirms that long (rather than short) wavelengths of visible light are the ones that can protect humans against myopia, as blue-light can be potentially harmful to the retina .
Although we have made significant progress in determining possible treatments for myopia, much still needs to be done before we understand fully the homeostatic mechanisms responsible for regulation of eye growth. New discoveries about the way visual feedback regulates eye size may lead to new treatment options for myopia, and further our understanding of a fundamental mechanism of human eye development and emmetropization, a poorly understood, but highly important function of visual processing in the retina.
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About the authors
Brittany Carr graduated with Honours from the Bachelor of Health Sciences program at the University of Calgary in 2011, and earned her PhD in Neuroscience at the Cumming School of Medicine at the University of Calgary, Alberta, Canada, in April 2017. Mentored by Dr. William K. Stell and Dr. Morley D. Hollenberg, her doctorate research was concerned with investigating the signalling mechanisms involved in atropine-mediated inhibition of myopia. By investigating the pharmacological behavior of atropine and other myopia-inhibiting muscarinic acetylcholine receptor (mAChR) antagonists, she successfully demonstrated that myopia inhibition by atropine may not be controlled by mAChRs, but instead some other unknown target receptor(s) or pathway(s), possibly involving alpha2A-adrenoceptors. She is currently a postdoctoral fellow, studying retinal degeneration at the University of British Columbia Centre for Macular Research (Vancouver, BC, Canada).
Bill Stell has been Professor of Cell Biology and Anatomy in the Cumming School of Medicine, University of Calgary, since 1980. He graduated from Swarthmore College with High Honors in Zoology in 1961, and received his Ph.D. in Anatomy in 1966 and M.D. in 1967, both from the University of Chicago. Subsequently he was at the NINDS, NIH, in the laboratories of Drs. Thomas G. Smith, Jr., K.C. Richardson, Henry G. Wagner, and M.G.F. Fuortes. In 1972 he joined the faculty of the Jules Stein Eye Institute, UCLA for 8 years, and finally found a home in Neuroscience at the University of Calgary, Alberta. Originally known for pioneering studies in EM of Golgi-impregnated neurons in fish retina, more recently Bill became interested in the retinal origins of myopia. Since then, he – with outstanding PhD. Students such as Dr. Carr – has made many and varied contributions to understanding the role(s) of the retina in causing and preventing myopia.