Congenital hypertrophy of the retinal pigment epithelium (CHRPE) is a harmless, pigmented fundus lesion that can be of various forms: solitary, grouped, and atypical,[1] and are found through clinical eye screenings from digital retinal imaging often established by ophthalmologists.[2] It is an uncommon diagnostic that is primarily found in patients before reaching their 30s, with the lesions often enlarging with time, thus being difficult to detect in younger ages.[3] With the detection of CHRPE, patients with CHRPE appearing with multiple shaped lesions are often the ones known to have Familial adenomatous polyposis (FAP).[4] Procedures are done to help establish further understanding of what is to be done when traces of CHRPE are found through eye exams, with education being a top priority for patients who have the CHRPE lesions to help them determine what the next steps are.[5] With this discovery, patients are highly encouraged to receive a colonoscopy in order to detect colorectal polyps, these often having high risks of being cancerous.[4]
CHRPE is a lesion with the retinal pigment epithelial (RPE)— densely packed cells in a single layer forming a blockage between the retina and the choroid—[6] that is generally cordial. There are three variations of CHRPE: solitary, grouped, and atypical, with these being found in ophthalmoscopes.[5] These exhibit an increase in cell size, normally elongated and rod-like shape, causing the RPE layer to become more dense in dimension.[5]
CHRPE is often developed through birth, with patients only showing signs of it in late adulthood, as CHRPE is often difficult to identify in younger ages due to the lesions being smaller, while growing with time.[3] CHRPE gene can establish from intra-familial variation, indicating that those individuals who are a part of CHRPE positive families should be tested from the colonoscopy biopsy and or genetic analysis to establish whether the gene is positive or negative.[7]
Risk factors include:
CHRPE is often discovered in annual eye exams, discovered by the digital imaging.[9] It is uncommon to identify this by staring into a mirror as the lesions that are grouped together is to small to see with the human eye.[10] There are three separate versions of CHRPE: solitary, grouped and atypical.[1]
FAP is a connecter to atypical CHRPE.[1] FAP spawns from a mutation located on chromosome 5q21.1, this mutation is the adenomatous polyposis coli (APC)— a tumor suppressor gene.[12] It is a condition in which hundreds of polyps are found within the colon through a colonoscopy that, if left untreated, can lead to colorectal cancer.[5]