N-glycosylation of CD4+ T cell changes with the development in Graves' disease and is sensitive to methimazole treatment

Graves' disease (GD) is one of the most common autoimmune disorders. Helper T (Th) cells, whose surface receptors are rich in glycans, are involved in the GD pathomechanism. N-glycosylation is altered during autoimmunity and can be modulated by pharmacotherapy. We hypothesized that changes in T...

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Published in	Biochimica et biophysica acta. General subjects Vol. 1869; no. 8; p. 130824
Main Authors	Trzos, Sara, Szewczyk, Marta, Link-Lenczowski, Paweł, Sokołowski, Grzegorz, Trofimiuk-Müldner, Małgorzata, Bocian, Katarzyna, Pocheć, Ewa
Format	Journal Article
Language	English
Published	Netherlands Elsevier B.V 01.07.2025
Subjects	Adult Antithyroid Agents - pharmacology Antithyroid Agents - therapeutic use Autoimmunity CD4+ T cells CD4-Positive T-Lymphocytes - drug effects CD4-Positive T-Lymphocytes - immunology CD4-Positive T-Lymphocytes - metabolism Female Glycosylation - drug effects Glycosyltransferases Graves Disease - drug therapy Graves Disease - immunology Graves Disease - metabolism Graves Disease - pathology Graves' disease Humans Male Methimazole Methimazole - pharmacology Methimazole - therapeutic use Middle Aged N-glycosylation Polysaccharides - metabolism Autoimmunity Methimazole CD4+ T cells Graves' disease N-glycosylation Glycosyltransferases CD4(+) T cells
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Abstract	Graves' disease (GD) is one of the most common autoimmune disorders. Helper T (Th) cells, whose surface receptors are rich in glycans, are involved in the GD pathomechanism. N-glycosylation is altered during autoimmunity and can be modulated by pharmacotherapy. We hypothesized that changes in Th glycosylation accompany GD, and the glycome of these cells is sensitive to methimazole therapy. The study group consisted of patients with Graves' disease before (GD) and after (GD/T) restoring euthyroidism as a result of methimazole therapy. In the control group, healthy donors were recruited. Th cells were isolated from PBMCs and sorted into a subpopulation of CD4+CD25− cells and those expressing the CD25 late activation marker (CD4+CD25+). MALDI-Tof MS was used for analysis of N-linked glycans, and the expression of glycosyltransferases was determined by RT-qPCR. The N-glycosylation profile of CD4+ cell subpopulations differed in the ratio of the complex-to-oligomannose N-glycans in GD. Complex N-glycans are partially replaced by oligomannose forms, and their structure is shortened by agalactosylation in CD4+CD25− cells from GD. The rearrangement of N-glycans in CD4+CD25+ cells has the opposite direction, namely the ratio is shifted towards complex structures in GD. The changes in the N-glycan profile were reflected partly in MGAT5 and FUT8 expression. Methimazole to some extent normalized the glycosyltransferase levels and affected the N-linked glycans profile. Our study shows N-glycosylation changes in CD4+ T cells in GD development and methimazole therapy for the first time. Further studies are needed to determine the functional aspect of the identified glycosylation changes in thyroid autoimmunity. [Display omitted] •N-glycan structure of CD4+ T CD25− and CD25+ cells is differently rebuilt during GD.•Oligomannose N-glycans are preferred in CD4+CD25− cells in GD.•Complex-type N-gycans are more abundant in CD4+CD25+ cells in GD development.•Methimazole partially reverses N-glycosylation changes in CD4+ T cells.•Reduced FUT8 expression is reflected in the lower level of fucosylated N-glycans.
AbstractList	Graves' disease (GD) is one of the most common autoimmune disorders. Helper T (Th) cells, whose surface receptors are rich in glycans, are involved in the GD pathomechanism. N-glycosylation is altered during autoimmunity and can be modulated by pharmacotherapy. We hypothesized that changes in Th glycosylation accompany GD, and the glycome of these cells is sensitive to methimazole therapy. The study group consisted of patients with Graves' disease before (GD) and after (GD/T) restoring euthyroidism as a result of methimazole therapy. In the control group, healthy donors were recruited. Th cells were isolated from PBMCs and sorted into a subpopulation of CD4+CD25- cells and those expressing the CD25 late activation marker (CD4+CD25+). MALDI-Tof MS was used for analysis of N-linked glycans, and the expression of glycosyltransferases was determined by RT-qPCR. The N-glycosylation profile of CD4+ cell subpopulations differed in the ratio of the complex-to-oligomannose N-glycans in GD. Complex N-glycans are partially replaced by oligomannose forms, and their structure is shortened by agalactosylation in CD4+CD25- cells from GD. The rearrangement of N-glycans in CD4+CD25+ cells has the opposite direction, namely the ratio is shifted towards complex structures in GD. The changes in the N-glycan profile were reflected partly in MGAT5 and FUT8 expression. Methimazole to some extent normalized the glycosyltransferase levels and affected the N-linked glycans profile. Our study shows N-glycosylation changes in CD4+ T cells in GD development and methimazole therapy for the first time. Further studies are needed to determine the functional aspect of the identified glycosylation changes in thyroid autoimmunity.Graves' disease (GD) is one of the most common autoimmune disorders. Helper T (Th) cells, whose surface receptors are rich in glycans, are involved in the GD pathomechanism. N-glycosylation is altered during autoimmunity and can be modulated by pharmacotherapy. We hypothesized that changes in Th glycosylation accompany GD, and the glycome of these cells is sensitive to methimazole therapy. The study group consisted of patients with Graves' disease before (GD) and after (GD/T) restoring euthyroidism as a result of methimazole therapy. In the control group, healthy donors were recruited. Th cells were isolated from PBMCs and sorted into a subpopulation of CD4+CD25- cells and those expressing the CD25 late activation marker (CD4+CD25+). MALDI-Tof MS was used for analysis of N-linked glycans, and the expression of glycosyltransferases was determined by RT-qPCR. The N-glycosylation profile of CD4+ cell subpopulations differed in the ratio of the complex-to-oligomannose N-glycans in GD. Complex N-glycans are partially replaced by oligomannose forms, and their structure is shortened by agalactosylation in CD4+CD25- cells from GD. The rearrangement of N-glycans in CD4+CD25+ cells has the opposite direction, namely the ratio is shifted towards complex structures in GD. The changes in the N-glycan profile were reflected partly in MGAT5 and FUT8 expression. Methimazole to some extent normalized the glycosyltransferase levels and affected the N-linked glycans profile. Our study shows N-glycosylation changes in CD4+ T cells in GD development and methimazole therapy for the first time. Further studies are needed to determine the functional aspect of the identified glycosylation changes in thyroid autoimmunity. Graves' disease (GD) is one of the most common autoimmune disorders. Helper T (Th) cells, whose surface receptors are rich in glycans, are involved in the GD pathomechanism. N-glycosylation is altered during autoimmunity and can be modulated by pharmacotherapy. We hypothesized that changes in Th glycosylation accompany GD, and the glycome of these cells is sensitive to methimazole therapy. The study group consisted of patients with Graves' disease before (GD) and after (GD/T) restoring euthyroidism as a result of methimazole therapy. In the control group, healthy donors were recruited. Th cells were isolated from PBMCs and sorted into a subpopulation of CD4+CD25− cells and those expressing the CD25 late activation marker (CD4+CD25+). MALDI-Tof MS was used for analysis of N-linked glycans, and the expression of glycosyltransferases was determined by RT-qPCR. The N-glycosylation profile of CD4+ cell subpopulations differed in the ratio of the complex-to-oligomannose N-glycans in GD. Complex N-glycans are partially replaced by oligomannose forms, and their structure is shortened by agalactosylation in CD4+CD25− cells from GD. The rearrangement of N-glycans in CD4+CD25+ cells has the opposite direction, namely the ratio is shifted towards complex structures in GD. The changes in the N-glycan profile were reflected partly in MGAT5 and FUT8 expression. Methimazole to some extent normalized the glycosyltransferase levels and affected the N-linked glycans profile. Our study shows N-glycosylation changes in CD4+ T cells in GD development and methimazole therapy for the first time. Further studies are needed to determine the functional aspect of the identified glycosylation changes in thyroid autoimmunity. [Display omitted] •N-glycan structure of CD4+ T CD25− and CD25+ cells is differently rebuilt during GD.•Oligomannose N-glycans are preferred in CD4+CD25− cells in GD.•Complex-type N-gycans are more abundant in CD4+CD25+ cells in GD development.•Methimazole partially reverses N-glycosylation changes in CD4+ T cells.•Reduced FUT8 expression is reflected in the lower level of fucosylated N-glycans. Graves' disease (GD) is one of the most common autoimmune disorders. Helper T (Th) cells, whose surface receptors are rich in glycans, are involved in the GD pathomechanism. N-glycosylation is altered during autoimmunity and can be modulated by pharmacotherapy. We hypothesized that changes in Th glycosylation accompany GD, and the glycome of these cells is sensitive to methimazole therapy. The study group consisted of patients with Graves' disease before (GD) and after (GD/T) restoring euthyroidism as a result of methimazole therapy. In the control group, healthy donors were recruited. Th cells were isolated from PBMCs and sorted into a subpopulation of CD4 CD25 cells and those expressing the CD25 late activation marker (CD4 CD25 ). MALDI-Tof MS was used for analysis of N-linked glycans, and the expression of glycosyltransferases was determined by RT-qPCR. The N-glycosylation profile of CD4 cell subpopulations differed in the ratio of the complex-to-oligomannose N-glycans in GD. Complex N-glycans are partially replaced by oligomannose forms, and their structure is shortened by agalactosylation in CD4 CD25 cells from GD. The rearrangement of N-glycans in CD4 CD25 cells has the opposite direction, namely the ratio is shifted towards complex structures in GD. The changes in the N-glycan profile were reflected partly in MGAT5 and FUT8 expression. Methimazole to some extent normalized the glycosyltransferase levels and affected the N-linked glycans profile. Our study shows N-glycosylation changes in CD4 T cells in GD development and methimazole therapy for the first time. Further studies are needed to determine the functional aspect of the identified glycosylation changes in thyroid autoimmunity.
ArticleNumber	130824
Author	Trofimiuk-Müldner, Małgorzata Link-Lenczowski, Paweł Bocian, Katarzyna Pocheć, Ewa Trzos, Sara Szewczyk, Marta Sokołowski, Grzegorz
Author_xml	– sequence: 1 givenname: Sara surname: Trzos fullname: Trzos, Sara email: sara.trzos@doctoral.uj.edu.pl organization: Department of Glycoconjugate Biochemistry, Institute of Zoology and Biomedical Research, Faculty of Biology, Jagiellonian University, Gronostajowa 9, 30-387 Krakow, Poland – sequence: 2 givenname: Marta surname: Szewczyk fullname: Szewczyk, Marta email: marta2.szewczyk@uj.edu.pl organization: Department of Glycoconjugate Biochemistry, Institute of Zoology and Biomedical Research, Faculty of Biology, Jagiellonian University, Gronostajowa 9, 30-387 Krakow, Poland – sequence: 3 givenname: Paweł surname: Link-Lenczowski fullname: Link-Lenczowski, Paweł email: p.link-lenczowski@uj.edu.pl organization: Department of Medical Physiology, Faculty of Health Sciences, Jagiellonian University Medical College, Michalowskiego 12, 31-126 Krakow, Poland – sequence: 4 givenname: Grzegorz surname: Sokołowski fullname: Sokołowski, Grzegorz email: g.sokolowski@uj.edu.pl organization: Department of Endocrinology, Faculty of Medicine, Jagiellonian University Medical College, Jakubowskiego 2, 30-688 Krakow, Poland – sequence: 5 givenname: Małgorzata surname: Trofimiuk-Müldner fullname: Trofimiuk-Müldner, Małgorzata email: malgorzata.trofimiuk@uj.edu.pl organization: Department of Endocrinology, Faculty of Medicine, Jagiellonian University Medical College, Jakubowskiego 2, 30-688 Krakow, Poland – sequence: 6 givenname: Katarzyna surname: Bocian fullname: Bocian, Katarzyna email: k.bocian@uw.edu.pl organization: Department of Immunology, Institute of Experimental Zoology, Faculty of Biology, University of Warsaw, Miecznikowa 1, 02-096 Warsaw, Poland – sequence: 7 givenname: Ewa surname: Pocheć fullname: Pocheć, Ewa email: ewa.pochec@uj.edu.pl organization: Department of Glycoconjugate Biochemistry, Institute of Zoology and Biomedical Research, Faculty of Biology, Jagiellonian University, Gronostajowa 9, 30-387 Krakow, Poland
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Keywords	Autoimmunity Methimazole CD4+ T cells Graves' disease N-glycosylation Glycosyltransferases CD4(+) T cells
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Snippet	Graves' disease (GD) is one of the most common autoimmune disorders. Helper T (Th) cells, whose surface receptors are rich in glycans, are involved in the GD...
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SubjectTerms	Adult Antithyroid Agents - pharmacology Antithyroid Agents - therapeutic use Autoimmunity CD4+ T cells CD4-Positive T-Lymphocytes - drug effects CD4-Positive T-Lymphocytes - immunology CD4-Positive T-Lymphocytes - metabolism Female Glycosylation - drug effects Glycosyltransferases Graves Disease - drug therapy Graves Disease - immunology Graves Disease - metabolism Graves Disease - pathology Graves' disease Humans Male Methimazole Methimazole - pharmacology Methimazole - therapeutic use Middle Aged N-glycosylation Polysaccharides - metabolism
Title	N-glycosylation of CD4+ T cell changes with the development in Graves' disease and is sensitive to methimazole treatment
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