Miller-Dieker syndrome

Miller–Dieker syndrome is abbreviated (MDS), and can be called Micro Deletion Syndrome, Miller–Dieker lissencephaly syndrome (MDLS) and chromosome 17p13.3 deletion syndrome. Miller Dieker syndrome is a congenital malformation (a physical defect detectable in an infant at birth which can involve many different parts of the body including the brain, hearts, lungs, liver, bones, intestinal tract) In this case it is usually mainly the brain being affected. The congenital malformation can be genetic random and of unknown origin. The malformation is in fact characterized by lissencephaly (smooth brain). MDS is a contiguous gene syndrome as well, which is a disorder due to the deletion of multiple gene loci that are adjacent to one another. The disorder arises from the deletion of part of the small arm of chromsome 17p (which includes both the LIS1 and 14-3-3 epsilon gene), leading to partial monosomy. There may be unbalanced translocations (i.e. 17q:17p or 12q:17p), or the presence of a ring chromosome 17.

This syndrome should not be confused with Miller syndrome - an unrelated rare genetic disorder - or Miller Fisher syndrome - a form of Guillain-Barré syndrome.

Early Detection
With the use of prenatal ultrasonographic imaging, early detection of abnormal brain development in the fetus with MDS can be seen. At birth, facial dysmorphism can be present in the infant. Young children, when affected, can suffer from feeding difficulties, severe intellectual disability, developmental delay, and seizures. An early way to detect this syndrome in children can be by brain MRI which can show the image of smooth brain, also called lissencephaly. It is possible that children with this syndrome may remain under-diagnosed because of how rare it is, and how common it is to have facial features that appear to be dysmorphic. They are highly variable and not easily recognizable because this syndrome shares distinct external features (phenotype) similar to more common syndromes. Lack of relevant family history can also prevent suspicion in many cases. FDNA provides a service that in turn increases the chances of detecting these distinct characteristics, which, when shown to a geneticist can assist in reaching the right medical diagnosis. If a couple has had one child with MDS, they can be offered prenatal diagnosis in future pregnancies. This option is particularly important for the 20% of MDS families where one parent carries a balanced chromosome rearrangement. The risk for these couples to have another affected child depends on the exact type of chromosome rearrangement present and may be as high as 25-33%. For families in which both parents' chromosomes are normal, the risk of having another child with MDS is low (1% or less). Either chorionic villus sampling (CVS) or amniocentesis can be used early in a pregnancy to obtain a small sample of cells from the developing embryo for chromosome studies. Early prenatal diagnosis by ultrasound is not reliable because the brain is normally smooth until later in pregnancy. Couples who are considering prenatal diagnosis should discuss the risks and benefits of this type of testing with a geneticist or genetic counselor.

Visuals of the Brain
-The brain is usually grossly abnormal in outline when someone is diagnosed with Miller Dieker Syndrome. There are only a few shallow sulci and shallow Sylvian fissures; this takes on an hour glass or figure-8 appearance on the axial imaging. The thickness and measurement for a person without MDS is 3-4mm. With MDS, a persons cortex is measured at 12-20mm.

Characteristics
The brain is abnormally smooth, with fewer folds and grooves. The face [especially in children] has distinct characteristics including a short nose with upturned nares, thickened upper lip with a thin vermillion upper border, frontal bossing, small jaw, low-set posteriorily rotated ears, sunken appearance in the middle of the face, widely spaced eyes, and hypertelorism. The forehead is prominent with bitemporal hollowing. Characteristics that are not visual include mental retardation, pre- and postnatal growth retardation, epilepsy, and reduced life span. Failure to thrive, feeding difficulties, seizures and decreased spontaneous activity are often seen, and death often occurs in infancy and childhood. There can also be multiple abnormalities of the brain, kidneys, and gastrointestinal tract (the stomach and intestines)

Cause and Genetics
In approximately 80% of the cases the origin of Miller Dieker syndrome is classified as unknown, according the statistical chart on healthline.com MDS is a random event during the formation of reproductive cells or in early fetal development. The other 20% of cases are caused by a familial chromosomal rearrangement called chromosomal translocation. In these cases, a chromosomal rearrangement in the parents is called a balanced translocation, in which no genetic material is gained or lost. Usually, the balanced translocations do not cause any health problems. However, they can become unbalanced as they are passed to the next generation. Miller–Dieker syndrome is usually not inherited. The deletion event occurs randomly during gametogenesis (formation of eggs or sperm) or in early foetal development. Therefore there is usually no history of the disorder in their family. Most individuals with this condition do not survive beyond childhood. In fact, most die in infancy. Individuals with MDS usually die in infancy. Because they do not live to the age where they can reproduce, they cannot transmit MDS to their offspring.

Less than 20% of cases are inherited through an autosomal dominant pattern. The parent is usually unaffected but carries a chromosomal rearrangement called a balanced translocation. Balanced translocations usually do not cause any health problems in the carrier; however, they can become unbalanced as they are passed to the next generation.

Miller-Dieker occurs in less than 1 in 100000 people and can occur in all races.

Diagnosis
The disease may be diagnosed by cytogenetic techniques, testing for a microdeletion at LIS1.

Treatment
While there is no cure for MDS at this time, many complications associated with this condition can be treated, and a great deal can be done to support or compensate for functional disabilities. Because of the diversity of the symptoms, it can be necessary to see a number of different specialists and undergo various examinations, including the following:
 * Developmental evaluation
 * Cardiologists evaluation
 * Otolaryngology
 * Treatment of seizures
 * Urologic evaluation
 * Genetic counseling--balanced chromosomal translocation should be excluded in a parents with affected child planning another pregnancy and so parents with affected children should visit a genetic counselor

History of Miller Dieker Syndrome
MDS was named for the two physicians, J. Miller and H. Dieker who independently described the condition in the 1960s. The hallmark of MDS is lissencephaly (smooth brain), a condition in which the outer layer of the brain, the cerebral cortex, is abnormally thick and lacks the normal convolutions (gyri). In some areas of the brain, gyri are fewer in number but wider than normal (pachygyri). Other areas lack gyri entirely (agyri). Normally, during the third and fourth months of pregnancy, the brain cells in the baby multiply and move to the surface of the brain to form the cortex. Lissencephaly is caused by a failure of this nerve cell migration. MDS is often called Miller-Dieker lissencephaly syndrome. It is named for James Q. Miller and H. Dieker. JQ Miller described the disease and in 1969 H Dieker emphasized that it should also take the name of lissencephaly syndrome because there are several malformations beyond the brain itself. When MDS was described in the beginning, geneticists assumed it followed an autosomal recessive pattern of inheritance. In the early 1990s several patients with Miller Dieker Syndrome were found to be missing a small portion of the chromosome 17. (17p13.3) (Partial deletion)