| 11 Mars 2015
(Okayama, 11 March) Researchers  at Okayama demonstrate the promise of a new approach for stimulating  neurons in the eyes of patients with dead photoreceptor cells.
 “The basic concept of retinal  prostheses is to replace dead photoreceptor cells with artificial  devices,” explain in a review of their recent research Toshihiko Matsuo,  eye doctor, and Tetsuya Uchida, polymer scientist, from Okayama  University, in collaboration with Kenichi Takarabe, semiconductor  scientist, from Okayama University of Science in Japan. Blind patients  with hereditary diseases such as retinitis pigmentosa, have dead  photoreceptor cells but other neurons remain alive. The Okayama  University researchers are exploiting the working functions of these  living neurons to send messages to the brain by artificial stimulation  from photoelectric dyes that respond to light. Other work on retinal  prostheses has focused on the use of arrays of electrodes – as in a  digital camera – or photodiodes. The challenges with these approaches  include miniaturising the devices, biocompatibility, low sensitivity and  low currents which often demand an external power source. “The  prototype of the photoelectric dye-coupled retinal prosthesis, OURePTM,  is unique in using electric potentials to stimulate retinal neurons, in  contrast with the other systems of retinal prostheses that generate  electric currents,” ” say the Okayama University researchers. Kelvin probe studies confirmed  the presence of electric potentials on the film surface induced in rapid  response to light. The researchers also tested the effect of the dye in  the eyes of Royal College of Surgeons rats. Cytotoxicity analyses  proved promising and behavioural tests on the rats suggested that the  treatment was effective. In addition the researchers  have plans for ways of testing the likelihood of treatment success by  using optical coherence tomography to assess the level of degeneration  in the patient’s retina. In terms of coming work they say, “Clinical  studies of photoelectric dye-based retinal prostheses, OURePTM,  in patients with retinitis pigmentosa who lose sight will be planned  since the manufacturing control and the quality control have been  already established for the medical device.” Background The photoelectric dye The Okayama researchers used the dye  2-[2-[4-[dibutylamino)phenyl]ethenyl]-3-carboxymethylbenzothiazolium  bromide ,which has an absorption spectra that spans the visible range  from 400 nm to 600 nm. It is also stable, readily synthesised and has a  low molecular weight and no obvious toxic components. They coupled the photoelectric dye to a soft thin polyethylene film at a concentration of around 106 dye molecules per μm2.  The film could also be rolled up before inserting into the subretinal  area through a small opening so that a large film could be fitted  providing a large field of view. Safety Polyethylene has been used for  medical implants for some time and its safety and stability has already  been proved. The researchers tested the toxicity of the dye in vitro using cultured retinal cells, as these are the cells the dye would come  into contact with first. No cytotoxicity was observed. Furthermore, no  toxicity has been found for OURePTM or for the photoelectric  dye in any tests for biological evaluation of medical devices, based on  the International Organization for Standardization (ISO) 10993. The photoelectric dye coupled polyethylene film was then implanted  into the retina of living rats. Apoptosis was reduced in the retinal  neurons which were in contact with dye-coupled polyethylene film, OURePTM. The photoelectric dye may have a neuroprotective effect on retinal neurons. Further tests are needed. Efficacy Kelvin probe measurements of  the electric potential on the dye-coupled film surface when exposed to  light showed rapid responses over the same range of wavelengths as the  known absorption spectrum of the dye. The sensitivity to different light  intensities was also promising. The researchers tested the dye on chick embryo retinal cells in vitro using a fluorescent dye to monitor calcium ions. They found that the  dye-stimulated responses triggered the increased calcium ion  concentrations. Dye coupled films were also implanted into Royal College  of Surgeons rats, who were then subjected to behaviour tests. When the  rats were placed in a drum with spinning walls painted in white and  black vertical stripes, the rats moved in the direction of the rotating  stripes, suggesting some level of sight had been retrieved. References  Matsuo T, Uchida T, Takarabe K.  Safety, efficacy, and quality control of a photoelectric dye-based  retinal prosthesis (Okayama University-type retinal prosthesis) as a  medical device. J Artif Organs 2009;12:213-225. DOI 10.1007/s10047-009-0471-6 Alamusi, Matsuo T, Hosoya O,  Tsutsui KM, Uchida T. Behavior tests and immunohistochemical retinal  response analyses in RCS rats with subretinal implantation of  Okayama-University-type retinal prosthesis. J Artif Organs. 2013  Sep;16(3):343-51. DOI 10.1007/s10047-013-0697-1 Alamusi, Matsuo T, Hosoya O, Tsutsui KM, Uchida T. Vision  maintenance  and retinal apoptosis reduction in RCS rats with Okayama  University-type retinal prosthesis (OURePTM) implantation.  J Artif Organs. 2015. DOI 10.1007/s10047-015-0825-1 Photoelectric dye-coupled thin film as a novel type of retinal prosthesis. Okayama Univ. e-Bulletin Vol.8, September 2014. http://www.okayama-u.ac.jp/user/kouhou/ebulletin/ipe/vol8/ipe_001.html Figure caption Behaviour test to establish the presence of sight in Royal College of  Surgeons rats with retinal prosthesis implantation. The researchers  rotated a drum with black-and-white vertical stripes either clockwise or  anticlockwise at a slow speed of 2 or 4 rpm. A rat that had prosthetic  retinal implants was put in a round transparent-walled cage inside the  drum. Instances when the rat turned its head in a direction consistent  with the direction of drum rotation were counted as indications that the  rat had retrieved some level of sight. Correspondence to Associate Professor Toshihiko Matsuo, M.D., Ph.D. Department of Ophthalmology,  Okayama University Medical School and Graduate School of Medicine,  Dentistry, and Pharmaceutical Sciences, 2-5-1 Shikata-cho, Kita-ku,  Okayama 700-8558, Japan E-mail: 
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