6031 Shallowford Road, Suite 101 Chattanooga, TN, 37421 (423) 876-2229 Contact Us Directions

Fertility Testing

Preconception Counseling

Woman The purpose of Preconception Counseling is to identify factors which could negatively affect your health or your pregnancy. A general history, including family history and laboratory testing, are essential to identify potential issues which may need to be addressed prior to conception.

A Routine Prenatal Screen includes testing for anemia, blood type and infectious diseases. Based on your medical history and ethnic background, additional tests may be recommended.

The routine panel includes: a complete blood count (CBC), blood type and screen, testing for immunity to Rubella and Varicella (if you have not had chickenpox previously), and Hepatitis B, HIV and Syphilis infection testing.

Complete Blood Count: This test checks for anemia, or low iron and/or blood count, which could negatively affect your pregnancy.

Blood Type and Screen:
Your red blood cells have two important proteins, the AB protein and the Rh protein. These proteins identify your blood type. Depending on the proteins that coat your red blood cells, your blood type is either A, B, AB, or O (when no protein is present). The other protein, Rh (Rhesus factor), is either present or absent and designates your cells as A-positive, A-negative, B-positive, B-negative and so forth.

Eighty five percent of people are Rh-positive and 15% are Rh-negative. If a woman is Rh-negative and her partner is Rh-positive, then her baby has a chance of being Rh-positive. In these cases, a woman can develop antibodies to the baby’s blood. These antibodies can lead to complications of pregnancy in future pregnancies (not the first pregnancy), such as pregnancy loss or growth restriction.

In addition to Rh antibodies there are other antibodies which can affect the health of your pregnancy. The type and screen searches for these, as well.

There are ways to significantly reduce the chances of pregnancy complications due to mismatched blood types and antibodies. Therefore it is extremely important to identify which patients will need observation and treatment during pregnancy.

Rubella: All women of reproductive age should be screened for Rubella, and if not immune, offered the Rubella vaccine prior to conception.

Rubella, also known as the German Measles, is caused by a virus which is transmitted through breathing. Pregnant women who contract Rubella are at risk for having a miscarriage, early death of a newborn, or a child with Congenital Rubella Syndrome (CRS) characterized by deafness, blindness, cataracts, heart defects, mental retardation, bone defects, and damage to the liver and spleen. Serious complications for the mother are rare.

A simple blood test can determine if you are immune to Rubella. If you are immune Rubella essentially poses no risk to your pregnancy.

Most people born in the United States have received the MMR, or measles, mumps, rubella vaccine. However, upon testing, not all reproductive age women developed immunity. Therefore, all women of reproductive age should be screened.

Women who are not immune should receive vaccination 4 weeks prior to attempting conception. Two vaccines are now recommended for women who previously had the vaccine, but now fail to demonstrate immunity. These women get the shots 1 month apart and must wait 1 month to attempt conception.

Hepatitis is a condition caused by various viruses which affect the liver. Hepatitis B and C are the most common viruses to adversely affect pregnancy. Some women carry this virus without knowing it and can transmit it to their child. It is important to identify these women so that they can be properly counseled on pregnancy risks and to ensure they are healthy enough to proceed with pregnancy.

There is a vaccine for Hepatitis B, which can be received during pregnancy. There is no vaccine for Hepatitis C.

HIV (human immunodeficiency virus) is the virus that causes AIDS, a condition in which the immune system fails and life-threatening opportunistic infections may occur. Many women and men with HIV have no symptoms for years prior to developing AIDS. If left unidentified and untreated in pregnancy, transmission rates to the baby are approximately 25%. With vigilent treatment and management of the mother during pregnancy, transmission rates to pregnancies may fall to less than 2%.

There is no vaccine for HIV.

Syphilis is a sexually transmissible disease caused by the bacterium Treponema pallidum. Like HIV, syphilis can remain silent for years. It can also mimic many other diseases and cause a wide array of symptoms. Syphilis can be transmitted to a baby, resulting in stillbirth or infant death. Babies can be born without symptoms and later become developmentally delayed or even die. If infected, women can be treated prior to pregnancy.

Cystic Fibrosis (CF) is an inherited lung and digestive disease causing variable symptoms which may include lung congestion, pneumonia, diarrhea and poor growth. More than 25,000 Americans have CF, and 850 new cases are diagnosed each year. CF is an inherited disease caused by gene abnormalities:

Most people have two normal copies of the CF gene.
Couples with normal copies of CF genes are not at increased risk for having a baby with CF.
CF carriers have one normal copy and one abnormal copy of the CF gene.
If both parents are carriers (each has a copy of the abnormal gene), there is a 1 in 4 (25%) chance that the baby will have CF.
People with CF have 2 copies of the abnormal gene.

Approximate risk that a couple with no family history of CF will have a child with CF:

ETHNIC BACKGROUND	CHANCES YOU ARE A CARRIER	RISK OF A BABY WITH CF	DETECTION RATE OF THE TEST
Caucasian Couple	1 in 25	1 in 2,500	80%
Ashkenazi Jewish Couple	1 in 25	1 in 2,500	97%
Hispanic Couple	1 in 46	1 in 8,000	57%
African American Couple	1 in 65	1 in 15,300	69%
Asian Couple	1 in 90	1 in 32,000

Many people with CF have severe symptoms and die at a young age despite extensive medical intervention. CF does not affect intelligence or the overall appearance of a child. Some people with CF have so few symptoms that they are unaware that they are even affected. The average life expectancy for a person affected with CF is approximately 30 years.

The average medical cost for an individual with CF is approximately $15,000 to $20,000/ year, or between $300,000 and $500,000 over their lifetime.

Currently there is no cure for CF, though this is an active area of research in the scientific and medical community. The American College of Obstetricians and Gynecologists recommends that your doctor offer screening for CF if you are considering pregnancy.

CF testing

A blood test can determine if you are a carrier of the most common CF gene mutations.
This blood test does not detect all possible mutations and the risk of having a baby with CF is never zero.
If testing shows that both partners are carriers, testing can be performed in pregnancy to determine if your baby is affected with CF.
Alternatively:

In vitro fertilization, and Preimplantation Genetic Diagnosis can be performed to test embryos for CF to ensure that a couple does not have an affected child, or
Donor oocytes (eggs) or donor sperm from a non-CF carrier may be used to ensure the couple does not have an affected child.

Strongly consider testing if you are:

A couple with a family history of CF.
A couple who would like to know, so that you can prepare for a child with special needs.
A couple who would terminate a pregnancy affected by CF.
A couple who would pursue IVF to avoid the possibility of a child with CF.

What does a negative test mean?
If one individual out of the couple (either the man or the wife) tests negative for the most common CF gene mutations, the overall risk of having a baby with CF is reduced markedly but not eliminated. If both couples test negative, the risk is further reduced. Both partners must be carriers to have a child whom is affected.

For example:
If a Caucasian woman tests negative for the CF gene, the couple’s risk goes from 1 in 2,500 to 1 in 12,500 (an 80% risk reduction). If both partners test negative, the risk is further reduced to 1 in 62,500.

If one couple is found to be a carrier, is known to be a carrier, or actually has CF, a negative test in the other partner does not reduce the risk as much.

For example:
If the man is a carrier (has 1 copy of the CF gene), and the wife is unaffected, the risk to the offspring is 1 in 250.

The actual risk may be lower, depending on the mutations carried, and consultation with a genetic counselor may be warranted.

Sickle Cell Disease

Sickle cell anemia is a chronic, inheritable disorder of the blood. It is caused by an abnormal hemoglobin molecule which makes the oxygen-carrying red blood cells misshaped and prone to collapsing. The blood cells create blockages in small blood vessels, resulting in painful episodes called “crises” which usually occur as severe, debilitating bone pain. Sickle cell patients are much more prone to infections and are at increased risk for strokes.

Children often have delayed physical and sexual maturation, low self esteem and depression. They require frequent medical interventions.

What are the chances my baby will have Sickle Cell Anemia?
Approximately 1/500 African Americans and 1/1,000 Hispanics have sickle cell anemia. Males and females are equally affected. Other ethnic groups at increased risk include Greeks, Italians, Turks, Arabs, Southern Iranians and Asian Indians.

An affected person must have 2 copies of the sickle cell gene. People with 1 copy of the gene are generally unaffected. They are called “carriers.” Carriers who have children have a 50% chance of passing the abnormal gene to their child.

Approximately 1 in 12 African Americans is a carrier for sickle cell anemia.
For a child to get sickle cell anemia, both parents need to carry an abnormal gene.

	Both parents have sickle cell anemia	Both parents are carriers	One patient is a carrier
Chances child will have the disease	50%	25%	0%
Chances the child will be a carrier	50%	50%	50%
Chances the child will be unaffected	0%	25%	50%

Testing for Sickle Cell Anemia
Testing for sickle cell is simple, requiring only a blood test. Insurance generally reimburses the cost of sickle cell screening.

What to if my test is positive?
If one parent’s test is positive, meaning they are a carrier, then the other partner should be tested to determine the risk to a child.
If both parents are positive (carriers), several management options exist:

Prior to pregnancy:
a. Couples may opt to undergo In vitro Fertilization (IVF) and perform Pre-Iimplantation Genetic Diagnosis (PGD) to ensure that embryos being placed into the uterus are not affected.
b. Donor sperm or donor oocytes from a non-carrier could also be considered.
During pregnancy:
a. Invasive testing such as amniocentesis or chorionic villi sampling can determine if the baby is affected. Choices regarding termination of an affected child would be made based on the personal beliefs of the parents.
After pregnancy:
a. Currently, management of symptoms and vigilant medical care is the mainstay of treatment.
b. Affected individuals can be cured with bone marrow transplants, but these treatments are not widely available.

Tay Sachs/Canavan/Gaucher/Dysautonomia
Tay-Sachs, Canavan and Gaucher are incurable, heritable diseases primarily affecting the central nervous system. They result from enzyme deficiencies causing abnormal metabolism of fatty substances in the brain. These substances accumulate and destroy brain cells. In most cases of Tay-Sachs and Canavan, the children die before the age of 5. The severity of Gaucher is more variable.

Like cystic fibrosis, both parents need to carry the genes causing these diseases. In general, the only way for a child to be affected is if he or she inherits an abnormal copy from the mother and the father.

All three of these diseases are most common in people with Eastern European Jewish anscestry (Ashkenazi Jews). However, especially for Tay-Sachs, other ethnicities are at increased risk.

Disease	Ethnicity	Carrier Rate
Tay-Sachs	Eastern European Jewish	1 in 30
	French Canadian	1 in 30
Gaucher	Eastern European Jewish	1 in 15
Canavan	Eastern European Jewish	1 in 40
Dysautonomia	Eastern European Jewish	1 in 32

Approximately 1 in 30 Ashkenazi Jews is a carrier for the Tay-Sachs gene, meaning they carry one gene for the disorder. An affected individual has both genes affected.

Couples with normal copies of Tay-Sachs genes are not at increased risk for having a baby with Tay-Sachs.
Carriers have one normal copy and one abnormal copy of the Tay-Sachs gene.
If both parents are carriers (each has a copy of the abnormal gene), there is a 1 in 4 (25%) chance that the baby will have Tay-Sachs.
People with Tay-Sachs have 2 copies of the abnormal gene.

Simple blood tests can determine if you are a carrier of the Tay-Sachs, Canavan or Gaucher mutations.

If both partners are carriers, additional testing can be performed in pregnancy to determine if your baby is affected with Tay-Sachs. Alternatively, in vitro fertilization can be performed to test embryos for Tay-Sachs or donor gametes from non-carrier individuals may be used to ensure that a couple does not have an affected child (See our section on IVF and Pre-Implantation Genetic Diagnosis).

Fragile X Premutation
Fragile X is the most common cause of inherited mental impairment, resulting in a spectrum of dysfunction ranging from learning disabilities to autism and severe mental retardation. Fragile X occurs in approximately 1 in 3,600 males and 1 in 5,000 females.

The disorder is caused by the inactivation of a gene, called the FMR1 gene, which is on the X chromosome. Because females have two copies of the X chromosome, a woman might carry the full mutation on one chromosome without knowing it. However, she is at increased for premature menopause and for having a baby with the disorder.

Males have one X chromosome and one Y chromosome and therefore do not get a back-up copy of the FMR1 gene. This is why they are more severely affected when they inherit one abnormal copy of the FMR1 gene.

Like many disorders discussed here, the most common family history is that no previous family member was known to be affected. Frequently, until a child is born severely mentally retarded, no one ever knew the family was at risk. In fact, the mutation can develop in a family over time.

All X chromosomes contain a section of what are called tri-nucleotide repeats. A normal X chromosome has fewer than 60 tri-nucleotide repeats in Fragile X region. However, these tri-nucleotide sections can expand from generation to generation. Once the tri-nucleotide repeat section becomes long enough (between 60-200 repeats), it becomes unstable and is very likely to expand in the next generation and results in the full mutation. One in 250 women carries the Fragile X premutation.

Those who should consider testing are individuals with:

Family history of autism, learning disabilities or otherwise unexplained mental retardation.
Premature ovarian failure – these women are at increased risk for having the premutation, and testing should be considered for their siblings.

The prevalence of Fragile X mutations among women with diminished ovarian reserve is being actively studied, but at this time is unknown. Some experts recommend screening for Fragile X mutations among any woman with diminished ovarian reserve under the age of 40. However, we agree with the committee statement of the American Society for Reproductive Medicine, recommending that genetic testing among this population not be widely performed until ongoing studies determine the prevalence of Fragile X premutations among these women.