Complement Activation in RPE Function and AMD Pathogenesis

Progress Updates

Complement is part of the body’s defense system against viral and bacterial infections. Usually, it is controlled precisely so that it does not cause “friendly fire” and injure the body itself. However, if the control mechanism is not working properly, then complement can cause damage and disease. It is now known that improper complement activity contributes to the development of macular degeneration. In this project, Dr. Song’s and Dr. Mohammed’s team is trying to produce a mouse model whereby they disable the complement control mechanism specifically in the eye, in the hope that this will lead to retinal injury that more closely mimics human macular degeneration. The complement control mechanisms are multiple and often redundant, therefore they may need to disable more than one mechanism to be sufficient to cause severe eye disease.

During the past year, the team has achieved disabling one particular control mechanism in a special type of mouse. Preliminary examination showed that the mice exhibited some signs of retinal degeneration, which is really quite exciting to see after disabling only one type of complement control. While they are continuing to observe and study these mice to see if the retinal disease will get worse and resemble the type of macular degeneration seen in humans, they are also disabling a second control mechanism. The team hopes that by concurrently removing these two control mechanisms, complement activity in the retinal cells will be switched into overdrive that will cause severe and fast-developing retinal disease. Such a mouse model of disease will allow testing of new anti-complement drugs, which could eventually be developed and used in human patients with AMD.