Abstract
Excessive screen exposure has become a significant health concern. This study investigates the impact of screen time on aging in middle-aged and elderly populations. Healthy working adults over 45 years old in Shanghai, China, underwent general and ocular examinations. Questionnaires collected demographics, medical history, and screen exposure details. Aging was assessed using the retinal age gap, defined as the difference between the retinal age predicted by deep learning algorithms based on fundus images and chronological age. Pathway analysis tested the mediation effect of sleep duration and onset time on the relationship between screen usage and retinal age gap. The retinal age gap increased with longer screen exposure, from 0.49 ± 3.51 years in the lowest tertile to 5.13 ± 4.96 years in the highest tertile (Jonckheere-Terpstra test, p < 0.001). Each additional hour of screen exposure accelerated the retinal age gap by 0.087 years (95% CI, 0.027, 0.148, p = 0.005) in the fully adjusted linear model. Sleep onset time mediated the impact of screen usage on the retinal age gap (indirect effect, β = 0.11; 95% CI 0.04–0.24). The impact of screen usage in a light-off environment on the retinal age gap was fully mediated by sleep onset time (indirect effect, β = 0.22; 95% CI 0.07–0.38), with the proportion being 100%. Our study identified a correlation between excessive screen time and a wider retinal age gap in middle-aged and elderly individuals, likely due to delayed sleep onset. To mitigate the adverse effects on the retina and aging, it is important to limit screen usage and avoid screens before bedtime.
Similar content being viewed by others
Avoid common mistakes on your manuscript.
Background
Excessive exposure to screen devices, including smart phones, computer, and television, which are frequently equipped with light-emitting diodes (LED), becomes a pervasive global health concern in recent decades. Mounting evidence indicates that prolonged screen time was associated with ocular diseases, such as myopia, dry eye, and digital eye strain [1,2,3]. Additionally, extended screen time was also reported to have negative impact on other health problems, such as increased risk of obesity, mental health, disrupted circadian rhythm, cardiovascular diseases, and stroke [4,5,6,7,8]. It is now well recognized the adverse effect of excessive screen time on both physiological and psychological health in children and adolescents [5, 9]; however, studies on the effect of screen time and health problems in middle-aged and elderly population are limited [8].
Among the various health effects of screen exposure, it is worth noting its impact on sleep and circadian rhythms [6, 10]. The luminescence spectrum of screen devices is mainly concentrated in the short-wavelength blue light band around 450 nm, which is generally more effective than long-wavelength light in inhibiting melatonin levels, altering circadian rhythms, increasing alertness, and decreasing subsequent sleep quality [11]. The existing literature suggested that long-time exposure to screen can lead to shorter sleep duration, delayed sleep onset time, deteriorated sleep quality, and other manifestations of circadian rhythm disorder [6, 10, 12, 13]. Sleep and aging are closely related [14]. Normal aging is accompanied by a reduced capacity to initiate and maintain sleep [14]. Circadian and sleep dysfunction could be early signs of various neurodegenerative diseases, and be involved in driving the process of brain aging [15, 16]. Moreover, sleep and circadian disorders are also associated with accelerated epigenetic aging, shorter telomere length, and other hallmarks of biological aging [17,18,19].
The fundus is the only part of the human body where nerves and blood vessels are visible without invasive methods [20]. The morphological changes in retinal structures such as the optic disc and blood vessels not only represent the occurrence and development of ocular diseases, but also are indicators for general health. For example, changes in the diameter of retinal vessels are considered to be associated with systemic diseases such as hypertension, arteriosclerosis [21], chronic kidney diseases [22], and stroke. Recently, retinal age, developed using deep learn technology based the fundus images, has been verified as a novel biomarker for aging [23]. The retinal age gap was calculated as the predicted age derived from the fundus image minus the chronological age, which has been shown to be associated with the risk of mortality [23], Parkinson’s disease [24], cardiovascular diseases [25, 26], metabolic syndrome [27], diabetic retinopathy, and kidney failure [28, 29]. To the best of our knowledge, there is no study reporting the association between screen exposure and retinal age gap.
Therefore, we speculate that excessive screen exposure may lead to accelerated aging by disrupting circadian rhythm such as shorter sleep duration and delayed sleep onset. We intend to verify this hypothesis through investigating the relationship between screen time, sleep duration and onset and retinal age gap in a middle-aged and elderly population.
Methods
Study design and population
This is a cross-sectional study in 2023 in Shanghai, China. We randomly selected one community in Shanghai Songjiang District. We recruit healthy working people over the age of 45 years. Exclusion criteria were as follows: (1) those with severe systemic diseases, such as tumor, autoimmune diseases, history of myocardial or cerebral infarction, kidney or hepatic dysfunction; (2) those with severe ocular diseases, such as glaucoma, age-related macular degeneration, pathologic myopia, and grade 3 or higher cataract based on Emery classification; (3) those cannot cooperate with the examinations or questionnaires; and (4) those with incomplete examination results; (5) those who work outdoors or in strong light.
General and ocular examinations
All participants underwent general examinations and ocular examinations. General examinations included height, weight, hip circumference, heart rate, blood pressure, and fasting blood tests. Blood tests contained fasting blood glucose, triglyceride, total cholesterol, high-density lipoprotein, low-density lipoprotein, and serum creatinine. Blood pressure was defined as the mean of two repeated measures with at least a 1-min interval taken with a HEM-7015IT electronic blood pressure monitor (Omron Healthcare, the Netherlands) in a seated position.
Ocular examinations included visual acuity, refraction, and fundus photography. The fundus photography was carried out using standardized methods and a unified parameter setting. For each participant, after 5 min of dark adaptation, the optic disc and macula of both eyes were photographed in a darkened room using a 50° 3.78-megapixel digital nonmydriatic camera (Kestrel-3100 m, SYSEYE, Chongqing, China). Since the correlation between the right and the left eye was high [30], to ensure the independency of the observation, optic disc-centered photos of the right eye were used for analyses, and if lacking or not qualified, the photos from the left eye were used instead.
Questionnaires and measurement of screen exposure time
Variables on demographics, lifestyle, and medical history were obtained through questionnaires. Basic information such as birth date, gender, job, education level, and marriage status were collected. Medical history, including hypertension, hyperlipidemia, diabetes, and other systemic and ocular diseases were also collected. Average outdoor activity duration and usual sleep time in the most recent month were recorded. We requested the participants to provide precise timings (at what time and minutes, e.g., 10:30 p.m.) of their usual sleep onset and wake-up times during the day and at night for the past 1 month.
Additionally, detailed information about the type of screen exposure and the corresponding duration in the light-on or the light-off environment in the most recent month was recorded. The type of screen exposure included mobile phone, computer, television, projector, and others. Participants were required to specify the exact duration of time spent using each type of electronic device, separately for usage in the light-on environment and in the light-off environment. For instance, regarding mobile phone usage, participants were asked to record the length of time spent using the phone in light-on and light-off environment, respectively. The participants were also asked to choose the content of the screen exposure, such as social communication, reading books, watching short videos, watching movies or TV series, and playing games.
Fundus images, deep learning model for age prediction, and calculation of retinal age gap
We formerly had developed a deep learning (DL) model based on color fundus images for age prediction (Supplementary material 1). Upon completion of the model training, predictions were made on an additional 664 images, and the retinal age gap was calculated. The retinal age gap is defined as the difference between the retinal age predicted by the DL model and the actual age. A positive retinal age gap indicates a retina that may be aging faster than normal, while a negative retinal age gap suggests the opposite. The average age of the population from which this set of images was sourced is 55.96, with a standard deviation of 4.72, a maximum age of 62, and a minimum age of 45.
Statistical analysis
The baseline features were summarized through descriptive statistics. Continuous variables were expressed as mean ± standard deviation or median (interquartile range), while categorical variables were presented as counts (percentages). Weight (in kilograms) divided by squared height (in meters) was used to calculate BMI. Mean arterial pressure was calculated as (systolic pressure + 2×diastolic pressure)/3. Total screen exposure time was the sum of all the screen usage types and their corresponding duration. The total duration of screen exposure time was also separately calculated for both light-on and light-off environments. The variable “sleep onset time” was designated to represent the time of sleep onset at night. Using 0:00 as a starting point, we calculated how many hours have passed since the time of sleep onset from 0:00. For example, if sleep onset at 10:30 p.m., we would record it as 22.5 h; if sleep onset at 0:15 a.m. of the next day, we would record it as 24.25 h. The interval between sleep onset time and wake-up time, including both during the day and at night, is designated as the variable “sleep duration.”
The continuous variables were in the form of mean (standard deviation) and were statistically tested by one-way ANOVA for comparing three groups and by Student’s t-test for comparing two groups; the categorical variables were in the form of No. (%), and were analyzed using chi-squared test. To test the trend of the three groups, Jonckheere-Terpstra test was used for continuous variables and Cochran-Mantel–Haenszel test was used for ordinal variables. Multiple linear regression was used for assessing the associations of screen usage duration with retinal age gap. Model 1 was adjusted for age, gender, and education. Model 2 was further adjusted for time outdoors, sleep duration, sleep onset time, fasting blood glucose, BMI, hip circumference, total cholesterol, and mean arterial pressure. Pathway analysis was used to test the mediation effect of sleep duration (or sleep onset time) between screen usage and retinal age gap. Bootstrap confidence intervals were performed [31]. Subgroup analysis was performed by age group. SAS version 9.4 (SAS Institute, Cary, NC) was used to conduct all the analyses. Two-sided P-values of 0.05 were deemed significant if not otherwise indicated.
Results
Basic characteristics of the study population
A total of 690 residents were initially recruited, among which 5 residents who work outdoors under intense light, 8 residents with severe eye diseases, 22 residents who could not cooperate with the examinations or questionnaire surveys, and 89 residents without complete examination results or questionnaire information were excluded (Fig. 1). As a result, 566 residents were included, comprising 194 males (34.28%) and 372 females (65.72%), with an overall mean age of 55.42 ± 4.78 years. The average total daily screen exposure time was 4.55 ± 2.16 h, with 4.46 ± 2.11 h in the light-on environment and 0.09 ± 0.3 h in the light-off environment.
Table 1 shows the basic characteristics of the study population stratified by the tertiles of the total screen exposure time. Retinal age gap, chronological age, gender, education level, sleep duration, sleep onset time, and outdoor time were statistically different among the three groups. The groups with higher screen exposure time were younger (ANOVA, p < 0.001; Jonckheere-Terpstra, p < 0.001), received higher educational level (p < 0.001; Cochran-Mantel–Haenszel, p < 0.001), shorter outdoor time (ANOVA, p < 0.001; Jonckheere-Terpstra, p < 0.001), shorter total sleep duration (ANOVA, p = 0.040; Jonckheere-Terpstra, p = 0.008), especially for the night-time sleep (ANOVA, p = 0.005; Jonckheere-Terpstra, p < 0.001), and later sleep onset (ANOVA, p < 0.001; Jonckheere-Terpstra, p < 0.001).
Table 2 shows the basic characteristics of the study population stratified by median of retinal age gap. Screen exposure time, chronological age, education level, outdoor time, sleep duration, sleep onset time, and hip circumference were statistically different among the two groups. The group with larger retinal age gap was younger (p < 0.001), received higher educational level (p < 0.001), shorter outdoor time (p < 0.001), shorter total sleep duration (p < 0.001), especially for the night-time sleep (p < 0.001), later sleep onset (p < 0.001), and smaller hip circumference (p = 0.005).
Screen time exposure and retinal age gap
As shown in Table 1, the retinal age gap increased as the screen exposure time extended, from 0.49 ± 3.51 years in the lowest tertile to 5.13 ± 4.96 years in the highest tertile (ANOVA, p < 0.001; Jonckheere-Terpstra, p < 0.001). The group with larger retinal age gap also had significantly longer screen exposure (5.29 ± 2.2 h) compared with the group with smaller retinal age gap (3.8 ± 1.84 h, p < 0.001), no matter under bright environment or dark environment (Table 2).
Table 3 demonstrates the linear regression analyses for the relationship between retinal age gap and total screen exposure time. The screen exposure was linearly associated with the retinal age gap both in Model 1 and Model 2. For every 1 h increase in the total screen exposure time, the retinal age gap accelerated by 0.087 (95%CI, 0.027, 0.148, p = 0.005) years, adjusting for chronological age, gender, education, time outdoors, sleep duration, sleep onset time, fasting blood glucose, BMI, hip circumference, total cholesterol, and mean arterial pressure.
Mediation analyses based on the sleep traits
Screen exposure time shortened sleep duration and accelerated aging (Table 4). However, sleep duration is not an intermediate variable between screen exposure time and retinal age gap. In the pathway analyses (Table 4), we observed that sleep onset time mediated the impact of screen usage on retinal age gap (indirect effect, β = 0.11; 95% CI 0.04 ~ 0.24), while sleep duration did not (indirect effect, β = 0; 95% CI − 0.03 to approximately 0.02). In detail, longer screen use may delay sleep onset time (β = 0.20, 95% CI 0.13 ~ 0.27), increasing the retinal age gap (β = 0.57, 95% CI 0.21 ~ 0.93) (Fig. 2). The proportion of indirect effect was 10.1%.
Further, we explored the impacts of screen usage in a light-on environment and in a light-off environment, respectively. We observed that sleep onset time mediated the impact of screen usage in a light-on environment (indirect effect, β = 0.42; 95% CI 0.27 ~ 0.57) on retinal age gap, and the proportion of indirect effect was 20.5%. In addition, sleep onset time fully mediated the impact of screen usage in a light-off environment (indirect effect, β = 0.22; 95% CI 0.07 ~ 0.38) on retinal age gap (Supplementary material 2-Table 1).
Subgroup analyses for mediation analyses
Among the residents aged below 60-year-old, for every 1-h increase in the total screen exposure time, the retinal age gap accelerated by 0.088 (95% CI, 0.020, 0.156, p = 0.011) years; while among the residents aged over 60-year-old, the impact of the total screen exposure time on the retinal age gap was not significant (p = 0.081) (Supplementary material 2-Table 2).
In addition, the pathway analysis confirmed the results above. Among the residents aged below 60 years old, sleep onset time mediated the impact of screen usage on retinal age gap, and the proportion of indirect effect was 23.7%. However, among the residents aged over 60 years old, the increase in the total screen exposure time did not delay the residents’ sleep onset time (Supplementary material 2-Table 3).
Discussion
Our study found that in the middle-aged and elderly population, excessive time spent in screen devices was associated with larger retinal age gap, which might be mediated by the delayed sleep onset time. This phenomenon was pronounced in residents younger than 60 years of age and might not be applicable to residents over 60 years of age. Although screen exposure time shortened sleep duration and accelerated aging, sleep duration is not an intermediate variable between screen exposure time and retinal age gap.
To the best of our knowledge, there is no study on excessive screen exposure and accelerated retinal aging. Normal use of LED light devices is not deleterious to human retina [32]. However, the potential toxicity of long-term cumulative exposure to the LED light devices is not determined in human eyes due to the difficulty to accurately measure the exposure [33]. Blue light which was enriched in LED devices could induce and accelerate cellular damage and photochemical reactions through the generation of ROS, resulting in lipid peroxidation, the loss of photoreceptors, and retinal pigment epithelium (RPE) cell dysfunction or apoptosis [34, 35]. These processes are similar to those observed in age-related macular degeneration (AMD), a senile disease with increasing prevalence with age, in which the photoreceptors degenerate while the RPE cells accumulate phototoxic components [36]. These were also coincided with the aging retina where the RPE cells were manifested by the accumulation of lipofuscin and formation of drusen, and the number of photoreceptor cells were decreased [37]. Moreover, with age, the antioxidant defenses are weakened making them incapable of neutralizing the oxidative stress produced by excessive exposure to blue light, which, in turn, could also expedite the damage of blue light to the human retina [38]. Therefore, theoretically, long-term exposure to screen could lead to retinal aging.
Study on screen exposure and biological aging is also scarce. The retinal age gap represents the accelerated process of aging and is related to a number of senile diseases [24, 26,27,28,29]. The present study found that prolonged screen exposure could speed up aging through the delay of sleep onset, which could be an indicator of delayed circadian clock. Existing literatures have suggested that excessive screen exposure, especially at night, could lead to changes in circadian rhythm, such as delayed sleep onset, reduced next-morning alertness, and decreased melatonin secretion [6, 10, 12, 13]. It has also been proven that blue light, which is abundant in screen devices, can disrupt the circadian rhythm [32, 39]. Meanwhile, changes in circadian rhythms could lead to the acceleration of aging and the shortened lifespan both in animals and human beings [17,18,19, 40,41,42]. In addition, in the process of aging, the damage of the retina caused by the blue light could lead to a decline in neuronal excitability and synaptic transmission [39]. It was reported that excessive screen time could alter gray matter and white volumes in the brain, undermine acquisition of memories and learning, and increase the risk of mental disorders and dementia [43]. All these evidence support the findings in the present study.
According to mediation analyses, it was indicated that sleep duration did not serve as a mediator between screen exposure and the retinal age gap; however, sleep onset time did. One possible explanation for the absence of a correlation in the mediation effect is that the relationship between sleep duration and aging could be nonlinear. In other words, both excessive and insufficient sleep duration may lead to accelerated aging [16, 44, 45], thus negating a mediating role. Conversely, a delayed sleep onset suggests a lag in the release of melatonin and disturbances in the circadian rhythm, which are closely associated with the acceleration of aging [17,18,19, 40,41,42]. Further analyses showed that the impact of screen usage in the light-off environment on the retinal age gap was fully mediated by sleep onset time, while the proportion of indirect effect of sleep onset time in the light-on environment was only 20.5% (Supplementary material 2-Table 1). This also suggested that circadian rhythm disruption may mediate the relationship between screen exposure and aging.
The phenomenon was observed in subgroup of residents younger than 60 years old, but not in the residents older than 60 years. Given that 60 is the retirement age in our country, individuals below this age are typically engaged in work. Consequently, their screen time tends to be more concentrated in the evenings, after work, which subsequently increases the likelihood of delayed sleep onset. Conversely, those who have reached or exceeded the age of 60 years, being rehired after retirement and often engaging in some leisure jobs, could have adequate time to use screens during the day, resulting in a lower likelihood of experiencing delayed sleep onset among this elderly population. Furthermore, as one ages, the crystalline lens of the eye becomes increasingly dense, thereby allowing less blue light to penetrate into the retina [33, 46]. Consequently, this reduced exposure to blue light decreases the likelihood of disrupting the circadian rhythm, ultimately contributing to the aging process.
The strength of this study lies in its comprehensive design, encompassing general and ophthalmological examinations, as well as questionnaires conducted among the community population. Rigorous statistical analyses were employed to arrive at the present conclusions. However, there are limitations to be noted. Firstly, the study is cross-sectional, lacking longitudinal follow-up, thus preventing the establishment of a causal relationship, and merely suggesting a correlation. Secondly, aging was assessed through the calculation of the retinal age gap from fundus photographs, lacking additional indicators for a more comprehensive evaluation of aging. Thirdly, sleep time, sleep onset time, and screen exposure time were all obtained via questionnaires, introducing the potential for recall bias. Future studies should aim to incorporate more objective measures for these variables, incorporate additional aging indicators for validation, and include longitudinal follow-up to establish causal relationships.
Conclusions
Our study revealed that, among middle-aged and elderly individuals, excessive screen time was linked to a wider retinal age gap. This may be partly explained by delayed sleep onset time. Notably, this trend was more evident among those below 60 years of age and may not extend to those over 60. Therefore, for working population, it is necessary to control screen time and avoid using screens before bedtime to reduce the impact of screen on the retina and systemic aging.
Data availability
The data that support the findings of this study are not openly available due to reasons of sensitivity and are available from the corresponding author upon reasonable request. Data are in controlled access data storage at Shanghai Eye Disease Prevention and Treatment Center.
Abbreviations
- LED:
-
Light-emitting diodes
- DL:
-
Deep learning
- RPE:
-
Retinal pigment epithelium
- AMD:
-
Age-related macular degeneration
References
Lanca C, Saw SM. The association between digital screen time and myopia: a systematic review. Ophthalmic Physiol Opt. 2020;40(2):216–29.
Kamøy B, Magno M, Nøland ST, et al. Video display terminal use and dry eye: preventive measures and future perspectives. Acta Ophthalmol. 2022;100(7):723–39.
Kaur K, Gurnani B, Nayak S, et al. Digital eye strain- a comprehensive review. Ophthalmol Ther. 2022;11(5):1655–80.
Paudel S, Del Pozo CB, Inan-Eroglu E, Ahmadi M, Stamatakis E. Associations of changes in physical activity and discretionary screen time with incident obesity and adiposity changes: longitudinal findings from the UK Biobank. Int J Obes (Lond). 2022;46(3):597–604.
Baattaiah BA, Alharbi MD, Babteen NM, Al-Maqbool HM, Babgi FA, Albatati AA. The relationship between fatigue, sleep quality, resilience, and the risk of postpartum depression: an emphasis on maternal mental health. BMC Psychol. 2023;11(1):10.
Cajochen C, Frey S, Anders D, et al. Evening exposure to a light-emitting diodes (LED)-backlit computer screen affects circadian physiology and cognitive performance. J Appl Physiol (1985). 2011;110(5):1432–8.
Qiu Z, Jia X, Fu Y, Yang Y. Screen time in the development of cardiovascular diseases: a two-sample Mendelian randomization study. Nutr Metab Cardiovasc Dis. 2024;34(3):706–17.
Ren Y, Sun K, Rong Y, et al. Association between daily screen time and risk of stroke among middle-aged and elderly people: research based on China health and nutrition survey. Front Sports Act Living. 2023;5:1307930.
Lissak G. Adverse physiological and psychological effects of screen time on children and adolescents: literature review and case study. Environ Res. 2018;164:149–57.
Chang AM, Aeschbach D, Duffy JF, Czeisler CA. Evening use of light-emitting eReaders negatively affects sleep, circadian timing, and next-morning alertness. Proc Natl Acad Sci U S A. 2015;112(4):1232–7.
Cho Y, Ryu SH, Lee BR, Kim KH, Lee E, Choi J. Effects of artificial light at night on human health: a literature review of observational and experimental studies applied to exposure assessment. Chronobiol Int. 2015;32(9):1294–310.
LeBourgeois MK, Hale L, Chang AM, Akacem LD, Montgomery-Downs HE, Buxton OM. Digital media and sleep in childhood and adolescence. Pediatrics. 2017;140(Suppl 2):S92–6.
Hale L, Guan S. Screen time and sleep among school-aged children and adolescents: a systematic literature review. Sleep Med Rev. 2015;21:50–8.
Mander BA, Winer JR, Walker MP. Sleep and human aging. Neuron. 2017;94(1):19–36.
Musiek ES, Holtzman DM. Mechanisms linking circadian clocks, sleep, and neurodegeneration. Science. 2016;354(6315):1004–8.
Ma Y, Liang L, Zheng F, Shi L, Zhong B, Xie W. Association between sleep duration and cognitive decline. JAMA Netw Open. 2020;3(9):e2013573.
Carroll JE, Ross KM, Horvath S, et al. Postpartum sleep loss and accelerated epigenetic aging. Sleep Health. 2021;7(3):362–7.
Baldelli L, Pirazzini C, Sambati L, et al. Epigenetic clocks suggest accelerated aging in patients with isolated REM sleep behavior disorder. NPJ Parkinsons Dis. 2023;9(1):48.
Wynchank D, Bijlenga D, Penninx BW, et al. Delayed sleep-onset and biological age: late sleep-onset is associated with shorter telomere length. Sleep. 2019;42(10):zsz139.
Wagner SK, Fu DJ, Faes L, et al. Insights into systemic disease through retinal imaging-based oculomics. Transl Vis Sci Technol. 2020;9(2):6.
Cheung CY, Thomas GN, Tay W, et al. Retinal vascular fractal dimension and its relationship with cardiovascular and ocular risk factors. Am J Ophthalmol. 2012;154(4):663-74.e1.
Liu R, Jian W, Zhao Y, Lu X, Wu Y, Duan J. Retinal oxygen saturation and vessel diameter in patients with chronic kidney disease. Acta Ophthalmol. 2021;99(3):e352–9.
Zhu Z, Shi D, Guankai P, et al. Retinal age gap as a predictive biomarker for mortality risk. Br J Ophthalmol. 2023;107(4):547–54.
Hu W, Wang W, Wang Y, et al. Retinal age gap as a predictive biomarker of future risk of Parkinson’s disease. Age Ageing. 2022;51(3):afac062.
Chen R, Xu J, Shang X, et al. Association between cardiovascular health metrics and retinal ageing. Geroscience. 2023;45(3):1511–21.
Zhu Z, Hu W, Chen R, et al. Retinal age gap as a predictive biomarker of stroke risk. BMC Med. 2022;20(1):466.
Zhu Z, Liu D, Chen R, et al. The association of retinal age gap with metabolic syndrome and inflammation. J Diabetes. 2023;15(3):237–45.
Chen R, Chen Y, Zhang J, et al. Retinal age gap as a predictive biomarker for future risk of clinically significant diabetic retinopathy. Acta Diabetol. 2024;61(3):373–80.
Zhang S, Chen R, Wang Y, et al. Association of retinal age gap and risk of kidney failure: a UK Biobank study. Am J Kidney Dis. 2023;81(5):537-44.e1.
Cheung CY, Sabanayagam C, Law AK, et al. Retinal vascular geometry and 6 year incidence and progression of diabetic retinopathy. Diabetologia. 2017;60(9):1770–81.
Rijnhart JJM, Lamp SJ, Valente MJ, MacKinnon DP, Twisk JWR, Heymans MW. Mediation analysis methods used in observational research: a scoping review and recommendations. BMC Med Res Methodol. 2021;21(1):226.
Touitou Y, Point S. Effects and mechanisms of action of light-emitting diodes on the human retina and internal clock. Environ Res. 2020;190:109942.
Cougnard-Gregoire A, Merle BMJ, Aslam T, et al. Blue light exposure: ocular hazards and prevention-a narrative review. Ophthalmol Ther. 2023;12(2):755–88.
Tosini G, Ferguson I, Tsubota K. Effects of blue light on the circadian system and eye physiology. Mol Vis. 2016;22:61–72.
Marie M, Bigot K, Angebault C, et al. Light action spectrum on oxidative stress and mitochondrial damage in A2E-loaded retinal pigment epithelium cells. Cell Death Dis. 2018;9(3):287.
Fletcher EL, Chung ST, Downie LE, Guymer RH, Vingrys AJ. Age-related macular degeneration: what’s new and on the horizon. Optom Vis Sci. 2014;91(8):816–8.
Campello L, Singh N, Advani J, Mondal AK, Corso-Díaz X, Swaroop A. Aging of the retina: molecular and metabolic turbulences and potential interventions. Annu Rev Vis Sci. 2021;7:633–64.
Kaya S, Weigert G, Pemp B, et al. Comparison of macular pigment in patients with age-related macular degeneration and healthy control subjects - a study using spectral fundus reflectance. Acta Ophthalmol. 2012;90(5):e399-403.
Shen J, Tower J. Effects of light on aging and longevity. Ageing Res Rev. 2019;53:100913.
Kondratov RV, Kondratova AA, Gorbacheva VY, Vykhovanets OV, Antoch MP. Early aging and age-related pathologies in mice deficient in BMAL1, the core component of the circadian clock. Genes Dev. 2006;20(14):1868–73.
Hendricks JC, Lu S, Kume K, Yin JC, Yang Z, Sehgal A. Gender dimorphism in the role of cycle (BMAL1) in rest, rest regulation, and longevity in Drosophila melanogaster. J Biol Rhythms. 2003;18(1):12–25.
Klarsfeld A, Rouyer F. Effects of circadian mutations and LD periodicity on the life span of Drosophila melanogaster. J Biol Rhythms. 1998;13(6):471–8.
Manwell LA, Tadros M, Ciccarelli TM, Eikelboom R. Digital dementia in the internet generation: excessive screen time during brain development will increase the risk of Alzheimer’s disease and related dementias in adulthood. J Integr Neurosci. 2022;21(1):28.
Révész D, Milaneschi Y, Terpstra EM, Penninx BW. Baseline biopsychosocial determinants of telomere length and 6-year attrition rate. Psychoneuroendocrinology. 2016;67:153–62.
Kanagasabai T, Chaput JP. Sleep duration and the associated cardiometabolic risk scores in adults. Sleep Health. 2017;3(3):195–203.
Kessel L, Lundeman JH, Herbst K, Andersen TV, Larsen M. Age-related changes in the transmission properties of the human lens and their relevance to circadian entrainment. J Cataract Refract Surg. 2010;36(2):308–12.
Funding
The study was funded by Key Disciplinary Projects of the 3-year Action Plan to Strengthen the Construction of the Public Health System in Shanghai (GWVI-11.1–30), Science and Technology Commission of Shanghai Municipality (23ZR1481000), Shanghai Municipal Health Commission (2022YQ051, 2024HP44 and 20234Y0062), and Shanghai First People’s Hospital featured research projects (CCTR-2022C08). The funding body did not participate in the design of the study and collection, analysis, and interpretation of data and in writing the manuscript.
Author information
Authors and Affiliations
Contributions
SLL, MG, DSL, and YYM contributed to the conceptualization and design of the study. MG, JZZ, TY, YJP, and DSL collected the data. SLL, MG, JZZ, YTW, and YYM analyzed the data. SLL, MG, JZZ, YTW, and YYM drafted the manuscript. SLL, YNJ, HDZ, LNL, DSL, and YYM extensively revised the manuscript. All authors read and approved the final manuscript submitted.
Corresponding authors
Ethics declarations
Ethics approval and consent to participate
This research received approval from the Ethics Committee of Shanghai Eye Disease Prevention and Treatment Center (2023SQ012), aligning with the principles of the Helsinki Declaration. All participants signed a written informed consent.
Consent for publication
Informed consent for publication was obtained from all authors.
Competing interests
The authors declare no competing interests.
Additional information
Publisher's Note
Springer Nature remains neutral with regard to jurisdictional claims in published maps and institutional affiliations.
Senlin Lin, Meng Gao, Juzhao Zhang, and Yuting Wu have contributed equally to this work and share first authorship.
Supplementary Information
Below is the link to the electronic supplementary material.
Rights and permissions
This article is published under an open access license. Please check the 'Copyright Information' section either on this page or in the PDF for details of this license and what re-use is permitted. If your intended use exceeds what is permitted by the license or if you are unable to locate the licence and re-use information, please contact the Rights and Permissions team.
About this article
Cite this article
Lin, S., Gao, M., Zhang, J. et al. Sleep onset time as a mediator in the association between screen exposure and aging: a cross-sectional study. GeroScience (2024). https://doi.org/10.1007/s11357-024-01321-x
Received:
Accepted:
Published:
DOI: https://doi.org/10.1007/s11357-024-01321-x