Your search keyword '"Tzong Hae Lee"' showing total 3 results

1. Male microchimerism in peripheral blood leukocytes from women with multiple sclerosis

Author

Tzong-Hae Lee, Lisa F. Barcellos, William Reed, Evan M. Bloch, Stephen Shiboski, Leilani Montalvo, and Brian Custer

Subjects

Autoimmune disease, Pregnancy, Fetus, business.industry, Multiple sclerosis, Microchimerism, medicine.disease, Biochemistry, Genetics and Molecular Biology (miscellaneous), Biochemistry, Immune tolerance, Male pregnancy, Immunology, Genetics, medicine, Etiology, business, Molecular Biology

Abstract

Background: Fetal microchimerism (F-MC), the persistence of fetal cells in the mother, is frequently encountered following pregnancy. The high prevalence of F-MC in autoimmune disease prompts consideration of the role for immune tolerance and regulation. This study examines the association between F-MC and multiple sclerosis (MS), an autoimmune disorder, of undetermined etiology. Study Design and Methods: Seventy-three female subjects were assigned to 3 groups according to disease status and pregnancy history: (1) MS positive (+) women with a history of one male pregnancy before symptom onset (n=27); (2) MS negative (-) female siblings of MS+ women with a history of one male pregnancy (n=22); and (3) MS+ women that reported never having been pregnant (n=24). Ten micrograms of genomic DNA obtained from peripheral blood leukocytes of each subject were analyzed for F-MC using allele-specific real-time PCR targeting the SR-Y sequence on the Y-chromosome. MC classification was dichotomous (positive vs. negativ...

Published

2011

2. Male microchimerism in peripheral blood leukocytes from women with multiple sclerosis

Author

Evan M, Bloch, William F, Reed, Tzong-Hae, Lee, Leilani, Montalvo, Stephen, Shiboski, Brian, Custer, and Lisa F, Barcellos

Subjects

Research Paper

Abstract

Fetal microchimerism (F-MC), the persistence of fetal cells in the mother, is frequently encountered following pregnancy. The high prevalence of F-MC in autoimmune disease prompts consideration of the role for immune tolerance and regulation. This study examines the association between F-MC and multiple sclerosis (MS), an autoimmune disorder, of undetermined etiology.21 out of 51 MS-positive subjects (41%) were classified as positive for F-MC; 4 of 22 (18%) of MS-negative sibling controls, were also positive for MC (p = 0.066). Unanticipated F-MC in controls lead to re-evaluation using 30 female singleton cord blood units (CBUs) as a biological control. Four CBUs were low-level positive.Seventy-three female subjects were assigned to three groups according to disease status and pregnancy history: (1) MS positive (+) women with a history of one male pregnancy before symptom onset (n = 27); (2) MS negative (-) female siblings of MS(+) women with a history of one male pregnancy (n = 22); and (3) MS(+) women that reported never having been pregnant (n = 24). Ten micrograms of genomic DNA obtained from peripheral blood leukocytes of each subject were analyzed for F-MC using allele-specific real-time PCR targeting the SR-Y sequence on the Y-chromosome. MC classification was dichotomous (positive vs. negative) based on PCR results.The association between F-MC and MS warrants further study to define this relationship. F-MC in women self-reporting as nulligravid, supports previous findings that a significant proportion of pregnancies go undetected. This lead to re-validation of a Y-chromosome based assay for F-MC detection.

Published

2010

3. Analysis of maternal microchimerism in rhesus monkeys (Macaca mulatta) using real-time quantitative PCR amplification of MHC polymorphisms.

Author

Bakkour, Sonia, Baker, Chris A. R., Tarantal, Alice F., Li Wen, Busch, Michael P., Tzong-Hae Lee, and Mccune, Joseph M.

Subjects

CHIMERISM, RHESUS monkeys, ANIMAL young, POLYMERASE chain reaction, CELL analysis

Abstract

Although pregnancy-associated microchimerism is known to exist in humans, its clinical significance remains unclear. Fetal microchimerism has been documented in rhesus monkeys, but the trafficking and persistence of maternal cells in the monkey fetus and infant have not been fully explored. To investigate the frequency of maternal microchimerism in the rhesus monkey (Macaca mulatta), a real-time polymerase chain reaction (PCR) strategy was developed and validated to target polymorphic major histocompatibility complex (MHC) gene sequences. Informative PCR assays were identified for 19 of 25 dams and their respective offspring. analyses were performed on tissues (thymus, liver, spleen, lymph nodes, and bone marrow) and peripheral blood mononuclear cells (PBMCs) collected prenatally and postnatally in a subset of animals. Seven of 19 monkeys had detectable maternal microchimerism in at least one compartment (range: 0.001-1.9% chimeric cells). In tissues, maternal microchimerism was found in 2 of 7 fetuses and 3 of 12 juveniles (1-1.5 years of age), and most of the animals that were positive had microchimeric cells in more than one tissue. Maternal microchimerism was detected in PBMCs from all (4 of 4) fetuses. These observations suggest that maternal microchimerism occurs in the rhesus monkey fetus and can be detected in tissues in a subset of offspring after birth. [ABSTRACT FROM AUTHOR]

Published

2014