CYTOGENETICS LABORATORY

The Human Genetics Diagnostic Laboratories provide state-of-the-art diagnostic laboratory services to many hospitals and clinical laboratories, both locally and throughout the country. The Cytogenetics Laboratory was established at Tulane in 1960 and was one of the first such labs in the country. We are currently the only regional laboratory performing a comprehensive list of cytogenetic studies including fluorescent in situ hydbridization(FISH), solid tumor analysis and bone marrow cytogenetics. A lab test order form can be found at the end of this page.

Quality Assurance
The Cytogenetic Laboratory is certified by CAP (College of American Pathologists), and certified by CLIA (Clinical Laboratory Improvement Act), SWOG (South Western Oncology Group). The laboratory participates in regular internal and external quality assurance programs, including sample exchanges and proficiency testing.

State of the Art Services
The laboratories are equipped with the state of the art color imaging system and computerized karyotyping system. This not only enables a broader spectrum of our services, a substantial shortening of turn around time of the results, but also provides the referring physician with higher quality of results.

Skilled Analysis and Cost-Effective Results
The clinical staff of the Human Genetics Program is available for telephone consultation regarding utilization of the services provided by our facility. Assistance in choosing the proper test, questions about appropriate specimens, testing procedures, and the interpretation of results, is available. Our faculty and staff can help you choose the best, most cost-effective test or tests, sometimes avoiding unnecessary, inappropriate, or repetitive testing. The Human Genetics telephone number is 504-988-5229; hours are 8:30 am to 5:00 PM Central Time. After hours, Cytogenetics Paging is available at 504-501-6096.

Communicating Results
Both the Cytogenetic and Molecular Diagnosis Laboratories provide:
· Initial telephone notification of abnormal results in most cases.
· Written reports containing a full analysis of results.
· Prompt turnaround time.

Urgent Contact

The services of the Human Genetics Program Diagnostic Laboratories are available 24 hours a day, 7 days per week. A staff member is always available on-call for urgent physician consultations and lab analyses on pager 504-501-6096.

CYTOGENETIC STUDIES

Cytogenetic studies are performed on the following tissues:

Peripheral Blood:

1. Metaphase Studies: This is the most commonly used cytogenetic study on peripheral blood providing the information on numerical and structural abnormalities of the chromosomes. Patients with suspected chromosomal anomalies can be evaluated with this study. Also, couples with a suspected balanced chromosomal translocation as the underlying cause for recurrent miscarriages can be evaluated using this method.

2. Prometaphase Studies: These studies are indicated whenever subtle chromosomal disarrangements that have not been identified by metaphase studies are suspected. It provides higher resolution with more detailed banding enabling the recognition of small deletions, duplications, and balanced or unbalanced translocations.

Prometaphase chromosomal study at 650 ~ 700 band level. a. metaphase spread; b. Karyotype of the same metaphase: 46, XX

3. Fragile X Study package: These studies are indicated in patients and families in whom X-linked mental retardation is suspected. In general, the package includes prometaphase chromosomal studies and DNA based molecular diagnosis for fragile X syndrome (please see detailed information in molecular tests for fragile X syndrome).

4. Chromosomal Breakage Studies - These studies are indicated as part of the diagnostic work-up for Fanconi's Pancytopenia, Ataxia-telangiectosia syndrome, and Bloom syndrome.

Bone Marrow or leukemic blood

Chromosome analysis is essential in the initial diagnosis, the prognosis of the hematological malignancy, including acute and chronic leukemia and lymphomas. It also plays an important role in the monitoring of the disease development, and the patient's response to treatment. Our chromosome study allows the identification of rearrangements observed in many types of these hematological disorders. An example of a common chromosomal abnormality found in leukemia is the presence of the Philadelphia chromosome (Ph). The presence of the Ph chromosome is diagnostic of chronic myelogenous leukemia. In addition to the Ph, as the course of the disease progresses, other chromosomal abnormalities may appear as well. With successful treatment, these abnormalities, except for the Ph chromosome, may disappear.

Prenatal Cytogenetic Studies

1. Amniotic Fluid -These studies are performed on patients with a history of chromosomal rearrangements, advanced maternal age, increased or decreased alpha-fetoprotein levels, and abnormalities seen on ultrasound. Amniotic fluid can be obtained at approximately 12 to 17 weeks gestation, and the results of the karyotype are reported within 7 to 10 days, depending on the rate of growth of the cells in tissue culture.

2. Chorionic Villus Sampling (CVS) - These studies are also performed for the above mentioned indications for study as amniotic fluid. However, CVS can be performed at 9 to 12 weeks gestation, and the results are reported within 6 to 8 days, also depending on the rate of growth of the cultured cells. Currently, our lab is the only one in the state of Louisiana performing chromosome analysis on CVS.

3. Percuntaneous umbilical blood sampling (PUBS) - Fetal blood sampling obtained from the umbilical cord may be indicated when mosaicism is detected in amniotic fluid studies, when there is a high risk of chromosomal abnormality and gestational age is advanced, for third trimester diagnosis when delivery is imminent, and for diagnosis of Fragile X or chromosomal instability syndromes.

Solid Tissue

1. Products of Conception - As many as 50% of spontaneous miscarriages are associated with chromosomal abnormalities. Successful karyotyping of the tissue may reveal critical information concerning the recurrence risk in future pregnancies. A late second trimester or a third trimester miscarriage of a nonviable fetus combined with clinical and pathological findings also raises the possibilities of chromosomal rearrangements.

2. Skin Fibroblasts - These can be submitted when peripheral blood is not available such as in the event that a patient has expired or in rare situations when mosaicism is suspected and the ratio of cells with chromosomal abnormalities of different tissues is evaluated.

3. Solid Tumors - Chromosomal abnormalities found in solid tumor are increasing daily. Many of them are associated with a specific type of solid tumor, and therefore, are of great importance in early diagnosis, prognosis and in the monitoring of the disease development. The type of tissue for the study is determined by the nature of the tumor.

MOLECULAR CYTOGENETIC STUDIES (Fluorescence In Situ Hybridization, FISH)

Standard cytogenetic analysis permits diagnosis of numerical and structural chromosome analysis, but it has limitations. Deletions smaller than several million base pairs are not routinely detectable. Chromosomal abnormalities with indistinct or novel banding patterns can be difficult or impossible to interpret. Analyzable metaphases may not be always possible to obtain (e.g. some types of solid tumors, autopsy material that has already been fixed). Chromosomal abnormalities which were previously difficult or impossible to detect with standard cytogenetic methods are now easily ascertained with FISH. This technique efficiently enables cytogeneticists to identify various numerical and structural alterations including aneuploidy, inversions, marker chromosomes, complicated or subtle translocations, and submicroscopic deletions and duplications. Our laboratory is equipped with the most updated knowledge and the best image system required providing this state-of-art service. Currently, we are implementing Multicolor FISH (M-FISH) and Comparative Genomic Hybridization (CGH) systems, which will greatly benefit cancer genetics studies and some difficult genetic cases.

Clinical application of FISH

1. Chromosome microdeletion syndromes:

Microdeletion Syndromes and Percentage of Cases Resolved with FISH

Microdeletion syndrome	Chromosomal Location	Probe	Percentage detected with FISH
Prader-Willi	(15q11-13)	SNRPN	70%
Angelman	(15q11-13)	D15S12	70%
Miller-Dieker	(17p13.3)	LIS-1	90%
Isolated lissencephaly sequence	(17p13.3)	LIS-1	33%
DiGeorge	(22q11.2)	D22S75(N25)	85%
Velocardiofacial (VCFS)	(22q11.2)	D22S75(N25)	53%
Williams	(7q11.23)	LIM kinase Elastin gene	97%
Smith-Magenis	(17p11.2)	D17S258	95%
Rubinstein Taybi	(16p13.3)	Cosmids RT1 and N2	25%
X-Linked icthyosis	(Xp22.3)	Steroid sulfatase gene	85%
Kallmann	(Xp22.3)	KAL gene	Unknown
X-Linked ocular albinism	(Xp22.3)	DXS1140	Unknown
Wolf-Hirschorn	(4p16.3)	WHSCR 165 Kb	presumably > 95%

2. Chromosomal structural abnormalities: Translocations, inversions, and duplications. Large translocation can be diagnosed by routine cytogenetics. However, complicated translocations and cryptic translocations often need the help of FISH analyses.

3. Oncogene amplifications or losses of antioncogene or gene rearrangement. For example: N-myc amplification in neuroblastoma and loss of P53 in B-cell CL.

4. Characterization of marker chromosome: Marker chromosomes are extra chromosomes of unknown origin. FISH, by far is the most effective and accurate method to identify the origin of markers.

5. Prenatal aneuploidy screen: Screen for chromosomes 13, 18, 21, X and Y.

FISH with probe TUPLE1 within DGS/VCFS chromosome region in a patient with VCFS. Solid arrow shows the deletion

Interphase FISH with bcr/abl probe on a bone marrow specimen from a patient suspected of CML. A positive fusion signal [t(9;22)] was present in each of the cells shown above

Cytogenetic Diagnostic Lab Test List

Please contact the department for sample specifications before shipping. To view the lab form and all tests, please open the Lab Test Form.