![Dr. Eva Morava-Kozicz, M.D, Ph.D., Geneticist](/doctor_images/5/54/74793.jpg?v=db9d)
Dr. Eva Morava-Kozicz, M.D, Ph.D.
Geneticist | Clinical Biochemical Genetics
200 1st St SW Rochester MN, 55905About
Dr. Eva Morava-Kozicz practices Genetic Medicine in Minnesota at Mayo Clinic. As a geneticist, Dr. Morava-Kozicz evaluates rare disorders and their genetic background in patients. A geneticist evaluates, diagnoses, and manages patients with hereditary conditions or congenital malformations, genetic risk calculations, and mutation analysis. Dr Morava is specialized in inborn errors of metabolism. Her major expertiese are in congenotal disorders of glycosylation (CDG) and mitochondrial disease. Dr. Morava-Kozicz carries out studies, tests, and counsels patients with genetic diseases. Dr Morava-Kozicz is a clinician scientist and also involved in clinical trials.
Board Certification
American Board of Medical Genetics
Provider Details
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Dr. Eva Morava-Kozicz, M.D, Ph.D.'s Expert Contributions
Is there a way to understand if my child has any genetic issue during pregnancy?
1) If your screening test results are positive or worrisome, 2) or you're at high risk of having a baby with Down syndrome, you might consider more testing to confirm the diagnosis, even at the stage when you are 4 months pregnant. Your health care provider can help you weigh the pros and cons of these tests. Diagnostic tests that can identify Down syndrome early in the pregnancy include Chorionic villus sampling (CVS). In CVS, cells are taken from the placenta and used to analyze the fetal chromosomes. This test is typically performed in the first trimester, between 10 and 13 weeks of pregnancy. The risk of pregnancy loss (miscarriage) from a CVS is very low. Diagnostic tests that can identify Down syndrome later in the pregnancy include: Amniocentesis. A sample of the amniotic fluid surrounding the fetus is withdrawn through a needle inserted into the mother's uterus. This sample is then used to analyze the chromosomes of the fetus. Doctors usually perform this test in the second trimester, after 15 weeks of pregnancy. This test also carries a very low risk of miscarriage. READ MORE
Can doctors identify congenital heart disease while the baby is in the womb?
A mild heart murmur doesn’t mean that the baby has a heart disease; it can be an innocent, functional murmur. In general, complex heart disease can definitely show up by prenatal testing, but not all types of defects, unfortunately. READ MORE
Do I have to go to a geneticist for genetic testing?
For cancer-related counseling, most genetic departments have certified genetic counselors. They can offer you a video consult and you can send a sample for testing (buccal swab), without personally attending the genetics clinics. Dr. Eva Morava READ MORE
Clinical Trials
Areas of expertise and specialization
Faculty Titles & Positions
- Professor of Medical Genetics Mayo Clinic, Rochester 2018 - Present
Awards
- CDG Hope and Dream Award 2013 World Conference on Congenital Disorders of Glycosylation
Professional Memberships
- American Society of Human Genetics
- Society for the Study of Inborn Errors of Metabolism
- European Society of Human Genetics
- American College of Medical Genetics
Fellowships
- Medical School of the University of Pecs, Pecs, Hungary 1999
- Tulane University School of Medicine, New Orleans, LA 1998
Areas of research
Eva Morava-Kozicz, M.D., Ph.D., conducts translational research in congenital disorders of glycosylation (CDG) mitochondrial disorders and mitochondrial medicine. Dr. Morava is actively involved in developing dietary therapies in genetic disorders and is the principal investigator of a multicenter study on the natural history of CDG.
Focus areas- Discovering new congenital disorders of glycosylation. Using next-generation sequencing, Dr. Morava played a crucial role in the definition of ATP6V0A2-CDG, SRD5A3-CDG, SLC35A1-CDG, ATP6V1A-CDG, ATP6V1E1-CDG and PGM1-CDG. She was also involved in the discovery of DPM2-CDG, DPM1-CDG, COG7-CDG, MAN1B1-CDG, ATP6VAP1-CDG, CCDC115-CDG and TMEM199-CDG, and is currently involved in unsolved disease discovery.
- Developing therapies for CDGs. Dr. Morava is involved in evaluating therapies in CDGs, including transplantation and dietary therapies such as D-galactose therapy. She is investigating the D-galactose working mechanism and is involved in clinical trials of many types of CDGs. Dr. Morava is working in close collaboration with the patient associations United Mitochondrial Disease Foundation (UMDF) and CDG CARE.
- Diagnostics therapy and follow-up of mitochondrial disease. Dr. Morava's modified scoring system has been used for more than 10 years to diagnose mitochondrial disease. It is now being adapted for the next-generation sequencing era to discover novel types of mitochondrial disorders, including the novel group of phospholipid synthesis defects.
- Defining the new syndrome group of metabolic cutis laxa. Previously called ARCL type 2A, metabolic cutis laxa is a connective tissue disorder that causes premature aging. Dr. Morava first described the glycosylation abnormalities in ARCL type 2A, and defined the characteristic phenotype of the new disease, metabolic cutis laxa. Since then, several new inborn errors have been found with different metabolic abnormalities.
The findings from Dr. Morava's research have a major impact on patient care and counseling, and provide a better understanding of metabolic disease.
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Nearby Providers
- Dr. Dusica Babovic-vuksanovic M.D.200 1st St SW Rochester MN 55905
- Dr. Jay W Ellison M.D.200 1st St SW Rochester MN 55905
- Dr. Noralane M Lindor M.D.200 1st St SW Rochester MN 55905
- Dr. Apostolos Psychogios MD200 1st St SW Rochester MN 55905
- Dr. Virginia V Michels M.D.200 1st St SW Rochester MN 55905
- Dr. Pamela S Mcgrann M.D.200 1st St SW Rochester MN 55905
Nearest Hospitals
MAYO CLINIC HOSPITAL ROCHESTERl
1216 SECOND STREET SOUTHWEST ROCHESTER MN 55902OLMSTED MEDICAL CENTERl
1650 FOURTH STREET SOUTHEAST ROCHESTER MN 55904MAYO CLINIC HEALTH SYSTEM - LAKE CITYl
500 WEST GRANT STREET LAKE CITY MN 55041