Photobiomodulation inhibits the expression of chondroitin sulfate proteoglycans after spinal cord injury via the Sox9 pathway

Both glial cells and glia scar greatly affect the development of spinal cord injury and have become hot spots in research on spinal cord injury treatment.The cellular deposition of dense extracellular matrix proteins such as chondroitin sulfate proteoglycans inside and around the glial scar is known to affect axonal growth and be a major obstacle to autogenous repair.These proteins are thus candidate targets for spinal cord injury therapy.Our previous studies demonstrated that 810 nm photo biomodulation inhibited the formation of chondroitin sulfate proteoglycans after spinal cord injury and greatly improved motor function in model animals.However,the specific mechanism and potential targets involved remain to be clarified.In this study,to investigate the therapeutic effect of photo biomodulation,we established a mouse model of spinal cord injury by T9 clamping and irradiated the injury site at a power density of 50 mW/cm~2 for 50 minutes once a day for 7 consecutive days.We found that photobiomodulation greatly restored motor function in mice and down regulated chondroitin sulfate proteoglycan expression in the injured spinal cord.Bioinformatics analysis revealed that photobiomodulation inhibited the expression of proteoglycan-related genes induced by spinal cord injury,and versican,a type of proteoglycan,was one of the most markedly changed molecules.Immunofluorescence staining showed that after spinal cord injury,versican was present in astrocytes in spinal cord tissue.The expression of versican in primary astrocytes cultured in vitro increased after inflammation induction,whereas photobiomodulation inhibited the expression of ve rsican.Furthermore,we found that the increased levels of p-Smad3,p-P38 and p-Erk in inflammatory astrocytes were reduced after photobiomodulation treatment and after delivery of inhibitors including FR 180204,(E)-SIS3,and SB 202190.This suggests that Sma d 3/Sox9 and MAP K/Sox9 pathways may be involved in the effects of photobiomodulation.In summary,our findings show that photobiomodulation modulates the expression of chondroitin sulfate proteoglycans,and versican is one of the key target molecules of photo biomodulation.MAPK/Sox9 and Smad3/Sox9 pathways may play a role in the effects of photo biomodulation on chondroitin sulfate proteoglycan accumulation after spinal cord injury.

Photobiomodulation:a novel approach to promote trans-differentiation of adipose-derived stem cells into neuronal-like cells

Photobiomodulation,originally used red and near-infrared lasers,can alter cellular metabolism.It has been demonstrated that the visible spectrum at 451-540 nm does not necessarily increase cell proliferation,near-infrared light promotes adipose stem cell proliferation and affects adipose stem cell migration,which is necessary for the cells homing to the site of injury.In this in vitro study,we explored the potential of adipose-derived stem cells to differentiate into neurons for future translational regenerative treatments in neurodegenerative disorders and brain injuries.We investigated the effects of various biological and chemical inducers on trans-differentiation and evaluated the impact of photobiomodulation using 825 nm near-infrared and 525 nm green laser light at 5 J/cm2.As adipose-derived stem cells can be used in autologous grafting and photobiomodulation has been shown to have biostimulatory effects.Our findings reveal that adipose-derived stem cells can indeed trans-differentiate into neuronal cells when exposed to inducers,with pre-induced cells exhibiting higher rates of proliferation and trans-differentiation compared with the control group.Interestingly,green laser light stimulation led to notable morphological changes indicative of enhanced trans-differentiation,while near-infrared photobiomodulation notably increased the expression of neuronal markers.Through biochemical analysis and enzyme-linked immunosorbent assays,we observed marked improvements in viability,proliferation,membrane permeability,and mitochondrial membrane potential,as well as increased protein levels of neuron-specific enolase and ciliary neurotrophic factor.Overall,our results demonstrate the efficacy of photobiomodulation in enhancing the trans-differentiation ability of adipose-derived stem cells,offering promising prospects for their use in regenerative medicine for neurodegenerative disorders and brain injuries.

Is it possible to anchor a tooth with photobiomodulation?

During orthodontic treatment,we can achieve differential movements by using photobiomodulation(PBM)as an adjuvant before applying force.We can expect a greater bone density that initially resists movement while applying PBM to the other teeth to achieve an accelerating effect.The proposed protocol is to use an 810 nm laser at 0.1W power,applying between 4 and 6J per tooth for 22 s on the vestibular and lingual root surfaces,following the axial axis of the tooth.The energy density depends on the tip selected in the instrument.Normal bone remodeling cannot be avoided by applying high doses of PBM.PBM should be applied before orthodontic force to reduce tooth movement.In addition,PBM can be used during force application to teeth that require acceleration to achieve differential movement in orthodontic treatments.The protocol is the same in both scenarios.

Photobiomodulation provides neuroprotection through regulating mitochondrial fission imbalance in the subacute phase of spinal cord injury

Increasing evidence indicates that mitochonarial lission imbalance plays an important role in derayed neuronal cell death. Our previous study round that photo biomodulation improved the motor function of rats with spinal cord injury.However,the precise mechanism remains unclear.To investigate the effect of photo biomodulation on mitochondrial fission imbalance after spinal cord injury,in this study,we treated rat models of spinal co rd injury with 60-minute photo biomodulation(810 nm,150 mW) every day for 14 consecutive days.Transmission electron microscopy results confirmed the swollen and fragmented alte rations of mitochondrial morphology in neurons in acute(1 day) and subacute(7 and 14 days) phases.Photo biomodulation alleviated mitochondrial fission imbalance in spinal cord tissue in the subacute phase,reduced neuronal cell death,and improved rat posterior limb motor function in a time-dependent manner.These findings suggest that photobiomodulation targets neuronal mitochondria,alleviates mitochondrial fission imbalance-induced neuronal apoptosis,and thereby promotes the motor function recovery of rats with spinal cord injury.

Potential targets and mechanisms of photobiomodulation for spinal cord injury

As a classic noninvasive physiotherapy,photobiomodulation,also known as low-level laser therapy,is widely used for the treatment of many diseases and has anti-inflammatory and tissue repair effects.Photobiomodulation has been shown to promote spinal cord injury repair.In our previous study,we found that 810 nm low-level laser therapy reduced the M1 polarization of macrophages and promoted motor function recovery.However,the mechanism underlying this inhibitory effect is not clear.In recent years,transcriptome sequencing analysis has played a critical role in elucidating the progression of diseases.Therefore,in this study,we performed M1 polarization on induced mouse bone marrow macrophages and applied low-level laser therapy.Our sequencing results showed the differential gene expression profile of photobiomodulation regulating macrophage polarization.We analyzed these genes using gene ontology and Kyoto Encyclopedia of Genes and Genomes enrichment analyses.Networks of protein-protein interactions and competing RNA endogenous networks were constructed.We found that photobiomodulation inhibited STAT3 expression through increasing the expression of miR-330-5p,and that miR-330-5p binding to STAT3 inhibited STAT3 expression.Inducible nitric oxide synthase showed trends in changes similar to the changes in STAT3 expression.Finally,we treated a mouse model of spinal cord injury using photobiomodulation and confirmed that photobiomodulation reduced inducible nitric oxide synthase and STAT3 expression and promoted motor function recovery in spinal cord injury mice.These findings suggest that STAT3 may be a potential target of photobiomodulation,and the miR-330-5p/STAT3 pathway is a possible mechanism by which photobiomodulation has its biological effects.

Photobiomodulation with Super-Pulsed Laser Shows Efficacy for Stroke and Aphasia: Case Studies

Background: Brain disorders have become more and more common today, due to both the aging population and the ever-expanding sports community. However, a new therapeutic technology called photobiomodulation (PBM) is giving hope to thousands of individuals in need. Traumatic brain injury (TBI), dementia, post traumatic stress (PTSD) and attention deficit (ADD) disorders are in many cases quickly and safely improved by PBM. PBM employs red or near-infrared (NIR) light (600 - 1100 nm) to stimulate healing, protect tissue from dying, increase mitochondrial function, improve blood flow, and tissue oxygenation. PBM can also act to reduce edema, increase antioxidants, decrease inflammation, protect against apoptosis, and modulate the microglial activation state. All these effects can occur when light is delivered to the head, and can be beneficial in both acute and chronic brain conditions. Methods: In this case series, we used a high power, FDA-approved superpulsed laser system applied to the head to treat four chronic stroke patients. Patients received as few as three 6 - 9 minute treatments over a one-week period. The follow up time varied, but in one case was two years. Results: Patients showed significant improvement in their speech and verbal skills. Improvements were also noticed in walking ability, limb movement, less numbness, and better vision. Conclusion: The use of PBM in stroke rehabilitation deserves to be tested in controlled clinical trials, because this common condition has no approved pharmaceutical treatment at present.

半导体激光对大鼠正畸性创伤性溃疡的影响研究

正畸患者常常因为正畸部件对口内黏膜的摩擦刺激出现黏膜不适的情况,而半导体激光可以治疗因正畸治疗引起的口腔黏膜不适,如红肿、溃疡等。本研究创新性地在大鼠口腔中制造持续创伤性环境,模拟正畸患者的口内情况,旨在利用动物模型来深入理解半导体激光对正畸性创伤性溃疡的修复机制。将32只雄性Wistar大鼠随机分成6组:1)空白对照组;2)对照组;3)氯己定组;4)激光组1;5)激光组2;6)激光组3。研究内容包括溃疡愈合程度评分、酶联免疫吸附试验、溃疡组织染色切片的组织学观察、溃疡面微生物附着量分析等。研究发现:持续创伤性环境会显著延长溃疡的愈合时间(P<0.05);溃疡持续期间,激光组溃疡组织的促炎因子水平更低,抗炎因子水平更高,愈合评分更高(P<0.05);半导体激光抗菌效果不及0.12%氯己定溶液;苏木精-伊红染色组织切片显示,激光组各时期的炎性细胞浸润程度均较低,上皮愈合程度更好。本研究表明,持续创伤性环境能延缓溃疡愈合,在减少炎症、减轻疼痛、促进溃疡组织愈合等方面,相比传统0.12%氯己定溶液,合适照射时间的半导体激光更具优越性。本研究的动物模型较以往研究有一定的进步,更贴近正畸患者的口腔真实情况。研究结果进一步证明了半导体激光治疗正畸时口腔创伤性溃疡的潜力。

面向阿尔茨海默病的非侵入性光生物调节治疗

据我国阿尔茨海默病协会官方网站显示,在我国60岁及以上老年人中约有1500万痴呆患者,其中1000万是阿尔茨海默病患者。随着我国人口结构老龄化,这一数据还将不断攀升。目前,按照现代医学寻找治疗靶点的逻辑思路,尚无有效治疗阿尔茨海默病的因应对策,药物治疗有许多限制,外科手术也无能为力。对此,我们不得不重新思考传统的系统化、整体化和功能化观点,并针对产生阿尔茨海默病背后的先导因素采取相应的治疗策略。近年来,关于光生物调节(PBM)治疗神经退行性疾病的研究逐渐增多,越来越多的学者尝试采用非侵入性PBM方式延缓、抑制,甚至逆转神经元退行性病变。在神经疾病治疗方面,PBM作为一种新的治疗方式,具有无创伤、无副作用、可以调节氧自由基浓度、激活干细胞调节细胞转录、刺激神经递质分泌、激发突触与神经元生长等显著优点。这些优点是其他治疗方式无与伦比的。本文综述了现代医学关于阿尔茨海默病治疗的靶点,阐释了PBM治疗阿尔茨海默病的机制,从动物模型、临床试验、病理与细胞模型方面系统总结了PBM治疗阿尔茨海默病的进展,并对未来发展做出展望,旨在为探索阿尔茨海默病临床干预新措施以及发展先进治疗方法和医疗器械提供参考。

光生物调节控制近视的研究进展

光生物调节(PBM),在促进皮肤愈合、治疗神经损伤等方面均发挥重要作用。近年来,PBM通过增加脉络膜厚度、延缓眼轴增长等途径,在控制儿童近视进展方面得到密切关注。这种新型的光生物学方法,对儿童视网膜、脉络膜的生物安全性及其作用机制是目前关注的焦点,本研究拟综述前期文献,从PBM的原理、功能、尤其是其安全性、作用机制等方面阐述其在近视及眼科临床中的应用,为阐明PBM在近视及眼科相关疾病中应用前景及潜在安全性思考。

光生物调节疗法在骨关节炎治疗中的研究进展

光生物调节疗法(PBMT)是一种根据不同治疗目的将生物组织暴露于特定波长光源的光疗法,长期应用于口腔科学、皮肤病学、骨科学等领域。在骨关节炎(OA)治疗中,大量的临床实践和基础医学研究已经证实,PBMT作为一种物理治疗方法,能够有效减轻OA患者的疼痛,促进炎症因子的代谢和清除,显著增强组织的修复能力,并加快不同组织和神经的再生,为OA患者提供了崭新的治疗选择。然而,PBMT的操作方式和剂量控制尚未形成统一的标准,治疗效果的评估具有一定的主观性和不确定性,仍存在较大的研究空间。尽管已有一些文章探讨了PBMT在OA领域的研究现状,但其主要是通过PBMT对OA的治疗讨论PBMT在抗炎方面的作用,而忽略了OA作为一种涉及全关节组织疾病的整体性和PBMT对OA作用效果的复杂性。本文系统梳理了PBMT在OA非手术治疗和手术治疗中的应用,分析了PBMT在OA整体治疗中的局限性,特别关注了PBMT在实际操作中存在的问题,深入思考了其未来的发展趋势,为充分利用PBMT无创、无痛和无副作用的特性发展先进的OA治疗手段与医疗器械提供了参考。

光生物调节诱导间充质干细胞的成骨分化

背景:间充质干细胞是从多种组织中分离出来的多能基质细胞,能够在特定的条件下分化为成骨细胞,光生物调节作为一种外部刺激能够单独或与其他诱导物联合使用加速间充质干细胞成骨分化的进程,从而为解决系列骨疾病提供新的思路。目的:综述光生物调节诱导间充质干细胞成骨分化的相关研究及机制,旨在为选用间充质干细胞作为种子细胞的骨组织工程奠定理论基础,并提出一些发展方向的建议。方法:检索中国知网、PubMed及Wed of Science数据库近年来发表的相关文献,中文检索词为“光生物调节,低功率激光,低水平激光,发光二极管,间充质干细胞,成骨分化,生物材料”;英文检索词为“Photobiomodulation,low level laser(light),light-emitting diode(LED),mesenchymal stem cell,osteogenic differentiation,Biomaterials”,最终纳入88篇文献进行分析。结果与结论:①以低水平激光和发光二极管为代表的光生物调节对于促进间充质干细胞的增殖与分化有着积极的影响。②光生物调节诱导间充质干细胞成骨分化的可行性已在细胞实验、动物实验中得到验证,一方面,光生物调节能够通过激活相关信号通路、上调成骨标志物的表达促进干细胞在体外扩增与分化;另一方面,光生物调节可以提高系统移植的干细胞体内存活率及归巢效应,缩短骨缺损愈合时间。但是光生物调节存在双相剂量效应,各项研究中激光参数、实验环境及细胞类型等要素参差不齐,使得研究结果缺乏一致性,难以推广。③光生物调节可以与生物材料、其他物理因子及药物联合使用加速干细胞成骨分化的进程。④总之,光生物调节因其无创、高效且无明显副反应等优势在医疗领域的应用逐渐广泛;近年来,其在骨组织工程中的作用也逐渐凸显,为骨缺损等疾病的治疗提供了新策略,后续研究应进一步探索光生物调节的标准化治疗参数。

光生物调节疗法在口腔颌面外科领域的应用研究进展

光生物调节疗法(PBMT)不会引起局部温度升高,不会造成组织不可逆的损伤,而且具有止痛、控制炎症、促进骨再生等多种作用,是一种非创伤性、非侵入性、不良反应少、低成本的治疗方法。该文就PBMT机制及其在口腔颌面外科领域的应用进行了综述。

光生物调节疗法治疗膝骨关节炎作用机制的研究进展

膝骨关节炎(knee osteoarthritis,KOA)是一种好发于中老年人的退行性疾病,以软骨退变、软骨下骨重塑、滑膜炎症为主要临床表现,常导致患者慢性关节疼痛、肢体功能障碍甚至残疾,随着目前社会老龄化的加剧,给社会经济带来巨大负担。然而,目前临床上主要以早期对症治疗、晚期关节置换的方案进行治疗,尚无有效治疗方法延缓KOA进展。近年来,光生物调节疗法(photobiomodulation therapy,PBMT)因其无痛、无创、安全有效的治疗效果引起了很多研究者的关注。PBMT通过刺激ATP的合成来提升细胞的能量水平并优化其状态;它还调整血流状况,以改善血运条件;调节相关细胞因子的水平,以缓解细胞炎症反应;以及调节相关酶的分泌,以缓解软骨退变。该文概述了PBMT通过上述一系列的作用机制对KOA进行治疗,以及其在促进软骨再生、缓解滑膜炎症以及减轻疼痛方面的治疗效果及潜在机制。

蓝光照射治疗对改善住院阿尔茨海默病患者认知功能的效果

背景阿尔茨海默病(AD)是最常见的痴呆类型,发病率逐年上升。药物治疗对改善AD患者认知功能、延缓疾病进展的效果不理想,进而影响治疗依从性。既往基础研究表明,蓝光照射有助于改善AD动物模型的认知功能,但目前缺乏相应关于蓝光照射治疗对AD患者认知功能改善效果的临床研究。目的探讨蓝光照射治疗对改善AD患者认知功能的效果,以期为改善AD患者的认知功能提供参考。方法回顾性选取2019年6月—2023年12月于深圳市康宁医院老年科住院治疗的、符合《国际疾病分类(第10版)》(ICD-10)AD诊断标准的患者155例。其中接受蓝光照射联合美金刚射治疗及常规心理治疗的80例为研究组,仅接受美金刚治疗及常规心理治疗的75例为对照组。蓝光照射治疗为期4周、每周5次、每次30 min。于治疗前后,采用简易精神状态评价量表(MMSE)和日常生活能力量表(ADL)进行评定。结果治疗后,研究组MMSE总评分、定向力、即刻回忆、注意力和计算力、延迟回忆以及语言功能评分均高于治疗前,差异均有统计学意义(Z=-6.931、-5.773、-4.123、-3.649、-3.508、-4.733,P均<0.05),ADL总评分低于治疗前,差异有统计学意义(Z=-7.020,P<0.05)。治疗后,研究组MMSE总评分、定向力、即刻回忆、语言功能评分均高于对照组,差异均有统计学意义(Z=-2.784、-4.621、-2.483、-3.463,P均<0.05),且研究组ADL总评分低于对照组,差异有统计学意义(Z=-3.704,P<0.05)。结论蓝光照射治疗可能有助于改善AD患者的认知功能和日常生活能力。

光生物调节对大鼠脊髓损伤结构性生物标志物的影响以及临床验证

目的探索光生物调节(PBM)对脊髓损伤(SCI)结构性生物标志物的影响,为后期SCI结构性生物标志物作为PBM疗效评估指标创造可能性。方法在动物实验中,将大鼠分为假手术组(Sham组)、SCI组、SCI+光照组(PBM组)3组,每组9只,在造模前与造模后1、3、7 d进行BBB评分并采集血清与脑脊液,利用酶联免疫法检测各组大鼠各时间点血清与脑脊液中结构性生物标志物(S100β、GFAP、TAU、MMPs、pNF-H、NSE)的浓度,对比分析其与大鼠BBB评分在PBM干预下的变化特征,并以此结果为基础,在临床展开验证。在临床实验中,根据纳入排除标准,将招募的SCI患者按照是否接受PBM治疗分为单纯减压手术+光照组(DP组)和单纯减压手术组(D组),在术前对两组患者进行ASIA评分,并于术前与术后1、3、7 d采集两组患者血清标本,检测并比较在动物实验中受PBM影响较大的结构性生物标志物(S100β、TAU、pNF-H、GFAP),在术后3个月随访时再次对患者进行ASIA评分,并与术前检查结果进行比较。结果在动物实验中,PBM组大鼠的BBB评分在造模后第3日开始高于SCI组,并于第7日显著高于SCI组(P<0.01)。PBM组与SCI组大鼠血清与脑脊液中的结构性生物标志物浓度均在造模后开始升高,并都在1~3 d内达到峰值,PBM组大鼠1、3、7 d血清中S100β、GFAP、TAU、pNF-H的浓度均显著低于SCI组(P<0.01),PBM组大鼠1、3、7 d脑脊液中的S100β、GFAP、TAU、MMPs、pNF-H、NSE浓度显著低于SCI组(P<0.01)。在临床实验中,DP组患者术后3、7 d血清中的TAU、pNF-H、GFAP浓度显著低于D组(P<0.01),并且随访发现,术后3个月DP组患者的ASIA针刺觉与轻触觉评分显著高于术前(P<0.05)。结论PBM在促进神经功能恢复的同时,可降低血清和脑脊液中SCI结构性生物标志物的浓度。

光生物疗法影响正畸牙根吸收的研究进展

牙根吸收是正畸治疗中最危险的并发症之一,轻度的牙根吸收可在停止加力后自行修复,而对于严重的牙根吸收尚无行之有效的应对手段。光生物疗法作为一种新的物理治疗手段,与传统方法相比,具有设备体积小、无创性、波长范围广、作用范围局限、生物安全性高等优点,其波长范围覆盖了线粒体吸收波长的范围。组织或细胞接受红光或近红外光照射后生物活性改变,上调抗炎相关因子表达,促进细胞三磷酸腺苷生成、加速局部血液微循环、促进软硬组织的修复,抑制或修复牙根吸收。光生物疗法的疗效取决于其波长、能量密度、功率密度、照射频率四个要素,遵循“Arndlt-Schulz”定律,即“双向剂量效应”,生物疗效具有参数相关性,因而难以确定最佳使用参数。但光生物疗法独特的优势,使其在正畸领域有着巨大的应用潜力。

Photobiomodulation for the treatment of retinal diseases: a review

Photobiomodulation（PBM）,also known as low level laser therapy,has recently risen to the attention of the ophthalmology community as a promising new approach to treat a variety of retinal conditions including agerelated macular degeneration,retinopathy of prematurity,diabetic retinopathy,Leber’s hereditary optic neuropathy,amblyopia,methanol-induced retinal damage,and possibly others.This review evaluates the existing research pertaining to PBM applications in the retina,with a focus on the mechanisms of action and clinical outcomes.All available literature until April 2015 was reviewed using Pub Med and the following keywords：＂photobiomodulation AND retina＂,＂low level light therapy AND retina＂,＂low level laser therapy AND retina＂,and＂FR/NIR therapy AND retina＂.In addition,the relevant references listed within the papers identified through Pub Med were incorporated.The literature supports the conclusion that the low-cost and noninvasive nature of PBM,coupled with the first promising clinical reports and the numerous preclinical-studies in animal models,make PBM well-poised to become an important player in the treatment of a wide range of retinal disorders.Nevertheless,large-scale clinical trials will be necessary to establish the PBM therapeutic ranges for the various retinal diseases,as well as to gain a deeper understanding of its mechanisms of action.

Current application and future directions of photobiomodulation in central nervous diseases

Photobiomodulation using light in the red or near-infrared region is an innovative treatment strategy for a wide range of neurological and psychological conditions.Photobiomodulation can promote neurogenesis and elicit anti-apoptotic,antiinflammatory and antioxidative responses.Its therapeutic effects have been demonstrated in studies on neurological diseases,peripheral nerve injuries,pain relief and wound healing.We conducted a comprehensive literature review of the application of photobiomodulation in patients with central nervous system diseases in February 2019.The NCBI PubMed database,EMBASE database,Cochrane Library and ScienceDirect database were searched.We reviewed 95 papers and analyzed.Photobiomodulation has wide applicability in the treatment of stroke,traumatic brain injury,Parkinson’s disease,Alzheimer’s disease,major depressive disorder,and other diseases.Our analysis provides preliminary evidence that PBM is an effective therapeutic tool for the treatment of central nervous system diseases.However,additional studies with adequate sample size are needed to optimize treatment parameters.

Comparative study on Photobiomodulation between 630 nm and 810 nm LED in diabetic wound healing both in vitro and in vivo

Photobiomodulation(PBM)promoting wound healing has been demonstrated by many studies.Currently,630 nm and 810 nm light-emitting diodes(LEDs),as light sources,are frequently used in the treatment of diabetic foot ulcers(DFUs)in clinics.However,the dose-effect relationship of LED-mediated PBM is not fully understood.Furthermore,among the 630 nm and 810 nm LEDs,which one gets a better effect on accelerating the wound healing of diabetic ulcers is not clear.The aim of this study is to evaluate and compare the effects of 630 nm and 810 nm LED-mediated PBM in wound healing both in vitro and in vivo.Our results showed that both 630 nm and 810 nm LED irradiation significantly promoted the proliferation of mouse fibroblast cells(L929)at different light irradiances(1,5,and 10 mW/cm^(2)).The cell proliferation rate increased with the extension of irradiation time(100,200,and 500 s),but it decreased when the irradiation time was over 500 s.Both 630 nm and 810nm LED irradiation(5 mW/cm^(2))significantly improved the migration capability of L929 cells.No difference between 630 nm and 810 nm LED-mediated PBM in promoting cell proliferation and migration was detected.In vivo results presented that both 630 nm and 810 nm LED irradiation promoted the wound healing and the expression of the vascular endothelial growth factor(VEGF)and transforming growth factor(TGF)in the wounded skin of type 2 diabetic mice.Overall,these results suggested that LED-mediated PBM promotes wound healing of diabetic mice through promoting fibroblast cell proliferation,migration,and the expression of growth factors in the wounded skin.LEDs(630 nm and 810 nm)have a similar outcome in promoting wound healing of type 2 diabetic mice.

Remote photobiomodulation: an emerging strategy for neuroprotection

Photobiomodulation (PBM)- the irradiation of cells or tissues with low-intensity red to near-infrared light - is emerging as an effective means of enhancing cell and tissue resilience and repair. As reviewed elsewhere (Gordon et al., 2019), the intracellular effects of PBM appear to be primarily mediated by cytochrome C oxidase, a key enzyme in the mitochondrial respiratory chain and a primary photoacceptor of red to near-infrared light. Absorption of light by cytochrome C oxidase alters its redox state, resulting in increased ATP production, the liberation of nitric oxide and a transient burst in reactive oxygen species.