THE ROLE OF PREGNANCY-SPECIFIC GLYCOPROTEIN IN REGULATION OF MOLECULAR GENETIC DIFFERENTIATION MECHANISMS OF IMMUNE MEMORY T CELLS

THE ROLE OF PREGNANCY-SPECIFIC GLYCOPROTEIN IN REGULATION OF MOLECULAR GENETIC DIFFERENTIATION MECHANISMS OF IMMUNE MEMORY T CELLS

The role of pregnancy-specific β1-glycoprotein (PSG) in the regulation of molecular genetic factors determining the functional activity of naїve T cells and T cells of immune memory in vitro was studied. Human PSG was isolated with a proprietary immuno-purification method using a biospecific sorbent...

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Autores principales: M. B. Rayev, L. S. Litvinova, K. A. Yurova, O. G. Khaziakhmatova, V. P. Timganova, M. S. Bochkova, P. V. Khramtsov, S. A. Zamorina
Formato: article
Lenguaje:RU
Publicado: SPb RAACI 2019
Materias:
psg
immune memory
naїve t cells
memory t cells
alternative splicing
ptprc gene
cd45ra
cd45r0
cd25
cd28
il-2
Immunologic diseases. Allergy
RC581-607
Acceso en línea:https://doaj.org/article/ad25fae09c3146448f77eede22b8cadf
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spelling oai:doaj.org-article:ad25fae09c3146448f77eede22b8cadf2021-11-18T08:03:48ZTHE ROLE OF PREGNANCY-SPECIFIC GLYCOPROTEIN IN REGULATION OF MOLECULAR GENETIC DIFFERENTIATION MECHANISMS OF IMMUNE MEMORY T CELLS1563-06252313-741X10.15789/1563-0625-2019-1-49-58https://doaj.org/article/ad25fae09c3146448f77eede22b8cadf2019-01-01T00:00:00Zhttps://www.mimmun.ru/mimmun/article/view/1698https://doaj.org/toc/1563-0625https://doaj.org/toc/2313-741XThe role of pregnancy-specific β1-glycoprotein (PSG) in the regulation of molecular genetic factors determining the functional activity of naїve T cells and T cells of immune memory in vitro was studied. Human PSG was isolated with a proprietary immuno-purification method using a biospecific sorbent followed by removing of immunoglobulin contamination with a HiTrapTM Protein G HP column. Physiological concentrations of PSG were used in the experiments. They corresponded to PSG levels in the peripheral blood of pregnant woman: 1, 10 and 100 μg/ml (I, II, III trimester, respectively). The objects of study were monocultures of naїve T cells (CD45RA+) and memory T cells (CD45R0+), obtained by immunomagnetic separation from the peripheral blood of women of reproductive age.It was established that at the level of naїve T cells (CD45RA+) PSG inhibited the expression of CD28 (1, 10, 100 μg/ml) and CD25 (100 μg/ml), without affecting the interleukin-2 (IL-2) production by these cells. At the same time, PSG in all concentrations studied suppressed the expression of CD25 at the immune memory T-cell (CD45R0+) surface but increased the IL-2 production. Expression of U2af1l4, Gfi1, hnRNPLL genes regulating the alternative splicing of the Ptprc gene encoding CD45 was also evaluated. It was found, that PSG reduced the expression of the Gfi1 (1, 10, 100 μg/ml), hnRNPLL (10, 100 μg/ml) genes, but increased the expression of the U2af1l4 gene (1, 10, 100 μg/ml) in the naїve T cells. It was shown that at the immune memory T-cells’ level the effects were similar, with PSG rendering them in all concentrations used. The revealed changes in the mRNA transcription of U2af1l4, Gfi1 and hnRNPLL genes in the studied T cell subsets may lead to the inhibition of CD45 “mature” isoform formation – CD45R0.Thus, PSG reduces the functional activity of naїve T cells and immune memory T cells associated with the expression of costimulation/activation molecules CD25 and CD28 and is involved in the regulation of Ptprc gene alternative splicing, which determines the ratio of CD45 molecule variants. Apparently, using these mechanisms, PSG regulates the functional activity of the memory T cell circulating pool, which is potentially capable of carrying out antigen-specific cytotoxic reactions against fetal antigens in vivo. In general, the data obtained broadens the notion of the PSG role in the regulation of molecular-genetic mechanisms of naїve T cells and immune memory T cells differentiation.M. B. RayevL. S. LitvinovaK. A. YurovaO. G. KhaziakhmatovaV. P. TimganovaM. S. BochkovaP. V. KhramtsovS. A. ZamorinaSPb RAACIarticlepsgimmune memorynaїve t cellsmemory t cellsalternative splicingptprc genecd45racd45r0cd25cd28il-2Immunologic diseases. AllergyRC581-607RUMedicinskaâ Immunologiâ, Vol 21, Iss 1, Pp 49-58 (2019)
institution DOAJ
collection DOAJ
language RU
topic psg
immune memory
naїve t cells
memory t cells
alternative splicing
ptprc gene
cd45ra
cd45r0
cd25
cd28
il-2
Immunologic diseases. Allergy
RC581-607
spellingShingle psg
immune memory
naїve t cells
memory t cells
alternative splicing
ptprc gene
cd45ra
cd45r0
cd25
cd28
il-2
Immunologic diseases. Allergy
RC581-607
M. B. Rayev
L. S. Litvinova
K. A. Yurova
O. G. Khaziakhmatova
V. P. Timganova
M. S. Bochkova
P. V. Khramtsov
S. A. Zamorina
THE ROLE OF PREGNANCY-SPECIFIC GLYCOPROTEIN IN REGULATION OF MOLECULAR GENETIC DIFFERENTIATION MECHANISMS OF IMMUNE MEMORY T CELLS
description The role of pregnancy-specific β1-glycoprotein (PSG) in the regulation of molecular genetic factors determining the functional activity of naїve T cells and T cells of immune memory in vitro was studied. Human PSG was isolated with a proprietary immuno-purification method using a biospecific sorbent followed by removing of immunoglobulin contamination with a HiTrapTM Protein G HP column. Physiological concentrations of PSG were used in the experiments. They corresponded to PSG levels in the peripheral blood of pregnant woman: 1, 10 and 100 μg/ml (I, II, III trimester, respectively). The objects of study were monocultures of naїve T cells (CD45RA+) and memory T cells (CD45R0+), obtained by immunomagnetic separation from the peripheral blood of women of reproductive age.It was established that at the level of naїve T cells (CD45RA+) PSG inhibited the expression of CD28 (1, 10, 100 μg/ml) and CD25 (100 μg/ml), without affecting the interleukin-2 (IL-2) production by these cells. At the same time, PSG in all concentrations studied suppressed the expression of CD25 at the immune memory T-cell (CD45R0+) surface but increased the IL-2 production. Expression of U2af1l4, Gfi1, hnRNPLL genes regulating the alternative splicing of the Ptprc gene encoding CD45 was also evaluated. It was found, that PSG reduced the expression of the Gfi1 (1, 10, 100 μg/ml), hnRNPLL (10, 100 μg/ml) genes, but increased the expression of the U2af1l4 gene (1, 10, 100 μg/ml) in the naїve T cells. It was shown that at the immune memory T-cells’ level the effects were similar, with PSG rendering them in all concentrations used. The revealed changes in the mRNA transcription of U2af1l4, Gfi1 and hnRNPLL genes in the studied T cell subsets may lead to the inhibition of CD45 “mature” isoform formation – CD45R0.Thus, PSG reduces the functional activity of naїve T cells and immune memory T cells associated with the expression of costimulation/activation molecules CD25 and CD28 and is involved in the regulation of Ptprc gene alternative splicing, which determines the ratio of CD45 molecule variants. Apparently, using these mechanisms, PSG regulates the functional activity of the memory T cell circulating pool, which is potentially capable of carrying out antigen-specific cytotoxic reactions against fetal antigens in vivo. In general, the data obtained broadens the notion of the PSG role in the regulation of molecular-genetic mechanisms of naїve T cells and immune memory T cells differentiation.
format article
author M. B. Rayev
L. S. Litvinova
K. A. Yurova
O. G. Khaziakhmatova
V. P. Timganova
M. S. Bochkova
P. V. Khramtsov
S. A. Zamorina
author_facet M. B. Rayev
L. S. Litvinova
K. A. Yurova
O. G. Khaziakhmatova
V. P. Timganova
M. S. Bochkova
P. V. Khramtsov
S. A. Zamorina
author_sort M. B. Rayev
title THE ROLE OF PREGNANCY-SPECIFIC GLYCOPROTEIN IN REGULATION OF MOLECULAR GENETIC DIFFERENTIATION MECHANISMS OF IMMUNE MEMORY T CELLS
title_short THE ROLE OF PREGNANCY-SPECIFIC GLYCOPROTEIN IN REGULATION OF MOLECULAR GENETIC DIFFERENTIATION MECHANISMS OF IMMUNE MEMORY T CELLS
title_full THE ROLE OF PREGNANCY-SPECIFIC GLYCOPROTEIN IN REGULATION OF MOLECULAR GENETIC DIFFERENTIATION MECHANISMS OF IMMUNE MEMORY T CELLS
title_fullStr THE ROLE OF PREGNANCY-SPECIFIC GLYCOPROTEIN IN REGULATION OF MOLECULAR GENETIC DIFFERENTIATION MECHANISMS OF IMMUNE MEMORY T CELLS
title_full_unstemmed THE ROLE OF PREGNANCY-SPECIFIC GLYCOPROTEIN IN REGULATION OF MOLECULAR GENETIC DIFFERENTIATION MECHANISMS OF IMMUNE MEMORY T CELLS
title_sort role of pregnancy-specific glycoprotein in regulation of molecular genetic differentiation mechanisms of immune memory t cells
publisher SPb RAACI
publishDate 2019
url https://doaj.org/article/ad25fae09c3146448f77eede22b8cadf
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