Menstrual cycle distribution of uterine natural killer cells is altered in heavy menstrual bleeding
•Reduced numbers of uNK cells in late secretory endometrium of women with HMB.•uNK cells are phenotypically altered in endometrium of women with HMB.•Other leukocyte populations are not altered. Heavy menstrual bleeding (HMB) affects 30% of women of reproductive age and significantly interferes with...
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Published in | Journal of reproductive immunology Vol. 112; pp. 88 - 94 |
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Main Authors | , , , , |
Format | Journal Article |
Language | English |
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Elsevier Ireland Ltd
01.11.2015
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Online Access | Get full text |
ISSN | 0165-0378 1872-7603 1872-7603 |
DOI | 10.1016/j.jri.2015.09.001 |
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Abstract | •Reduced numbers of uNK cells in late secretory endometrium of women with HMB.•uNK cells are phenotypically altered in endometrium of women with HMB.•Other leukocyte populations are not altered.
Heavy menstrual bleeding (HMB) affects 30% of women of reproductive age and significantly interferes with quality of life. Altered endometrial vascular maturation has been reported in HMB and recurrent miscarriage, the latter associated with increased uterine natural killer (uNK) cell numbers. This study compared endometrial leukocyte populations in controls and women with HMB. Formalin-fixed paraffin-embedded endometrial biopsies from controls (without endometrial pathology) and HMB were immunostained for CD14 (macrophages), CD56 (uNK cells), CD83 (dendritic cells), FOXP3 (regulatory T cells/Tregs), CD3 and CD8 (T cells). Leukocyte numbers were analysed as a percentage of total stromal cells in five randomly selected fields of view in the stratum functionalis of each sample. In control women across the menstrual cycle, 2–8% of total stromal cells were CD3+ cells, 2–4% were CD8+ T cells and 6–8% were CD14+ macrophages. Compared with controls, CD3+ cells were reduced during the mid-secretory phase (4%, P<0.01) and increased in the late secretory phase (12%, P=0.01) in HMB. CD83+ dendritic cells and FOXP3+ Tregs were scarce throughout the menstrual cycle in both groups. In controls, 2% of stromal cells in proliferative endometrium were CD56+ uNK cells, increasing to 17% during the late secretory phase. In HMB, CD56+ uNK cells were increased in the proliferative (5%, P<0.01) and early secretory (4%, P<0.02) phases, but reduced (10%, P<0.01) in the late secretory phase. This study demonstrates dysregulation of uNK cells in HMB, the functional consequence of which may have an impact on endometrial vascular development and/or endometrial preparation for menstruation. |
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AbstractList | Highlights • Reduced numbers of uNK cells in late secretory endometrium of women with HMB. • uNK cells are phenotypically altered in endometrium of women with HMB. • Other leukocyte populations are not altered. Heavy menstrual bleeding (HMB) affects 30% of women of reproductive age and significantly interferes with quality of life. Altered endometrial vascular maturation has been reported in HMB and recurrent miscarriage, the latter associated with increased uterine natural killer (uNK) cell numbers. This study compared endometrial leukocyte populations in controls and women with HMB. Formalin-fixed paraffin-embedded endometrial biopsies from controls (without endometrial pathology) and HMB were immunostained for CD14 (macrophages), CD56 (uNK cells), CD83 (dendritic cells), FOXP3 (regulatory T cells/Tregs), CD3 and CD8 (T cells). Leukocyte numbers were analysed as a percentage of total stromal cells in five randomly selected fields of view in the stratum functionalis of each sample. In control women across the menstrual cycle, 2-8% of total stromal cells were CD3+ cells, 2-4% were CD8+ T cells and 6-8% were CD14+ macrophages. Compared with controls, CD3+ cells were reduced during the mid-secretory phase (4%, P <0.01) and increased in the late secretory phase (12%, P =0.01) in HMB. CD83+ dendritic cells and FOXP3+ Tregs were scarce throughout the menstrual cycle in both groups. In controls, 2% of stromal cells in proliferative endometrium were CD56+ uNK cells, increasing to 17% during the late secretory phase. In HMB, CD56+ uNK cells were increased in the proliferative (5%, P <0.01) and early secretory (4%, P <0.02) phases, but reduced (10%, P <0.01) in the late secretory phase. This study demonstrates dysregulation of uNK cells in HMB, the functional consequence of which may have an impact on endometrial vascular development and/or endometrial preparation for menstruation. Heavy menstrual bleeding (HMB) affects 30% of women of reproductive age and significantly interferes with quality of life. Altered endometrial vascular maturation has been reported in HMB and recurrent miscarriage, the latter associated with increased uterine natural killer (uNK) cell numbers. This study compared endometrial leukocyte populations in controls and women with HMB. Formalin-fixed paraffin-embedded endometrial biopsies from controls (without endometrial pathology) and HMB were immunostained for CD14 (macrophages), CD56 (uNK cells), CD83 (dendritic cells), FOXP3 (regulatory T cells/Tregs), CD3 and CD8 (T cells). Leukocyte numbers were analysed as a percentage of total stromal cells in five randomly selected fields of view in the stratum functionalis of each sample. In control women across the menstrual cycle, 2-8% of total stromal cells were CD3(+) cells, 2-4% were CD8(+) T cells and 6-8% were CD14(+) macrophages. Compared with controls, CD3(+) cells were reduced during the mid-secretory phase (4%, P<0.01) and increased in the late secretory phase (12%, P=0.01) in HMB. CD83(+) dendritic cells and FOXP3(+) Tregs were scarce throughout the menstrual cycle in both groups. In controls, 2% of stromal cells in proliferative endometrium were CD56(+) uNK cells, increasing to 17% during the late secretory phase. In HMB, CD56(+) uNK cells were increased in the proliferative (5%, P<0.01) and early secretory (4%, P<0.02) phases, but reduced (10%, P<0.01) in the late secretory phase. This study demonstrates dysregulation of uNK cells in HMB, the functional consequence of which may have an impact on endometrial vascular development and/or endometrial preparation for menstruation.Heavy menstrual bleeding (HMB) affects 30% of women of reproductive age and significantly interferes with quality of life. Altered endometrial vascular maturation has been reported in HMB and recurrent miscarriage, the latter associated with increased uterine natural killer (uNK) cell numbers. This study compared endometrial leukocyte populations in controls and women with HMB. Formalin-fixed paraffin-embedded endometrial biopsies from controls (without endometrial pathology) and HMB were immunostained for CD14 (macrophages), CD56 (uNK cells), CD83 (dendritic cells), FOXP3 (regulatory T cells/Tregs), CD3 and CD8 (T cells). Leukocyte numbers were analysed as a percentage of total stromal cells in five randomly selected fields of view in the stratum functionalis of each sample. In control women across the menstrual cycle, 2-8% of total stromal cells were CD3(+) cells, 2-4% were CD8(+) T cells and 6-8% were CD14(+) macrophages. Compared with controls, CD3(+) cells were reduced during the mid-secretory phase (4%, P<0.01) and increased in the late secretory phase (12%, P=0.01) in HMB. CD83(+) dendritic cells and FOXP3(+) Tregs were scarce throughout the menstrual cycle in both groups. In controls, 2% of stromal cells in proliferative endometrium were CD56(+) uNK cells, increasing to 17% during the late secretory phase. In HMB, CD56(+) uNK cells were increased in the proliferative (5%, P<0.01) and early secretory (4%, P<0.02) phases, but reduced (10%, P<0.01) in the late secretory phase. This study demonstrates dysregulation of uNK cells in HMB, the functional consequence of which may have an impact on endometrial vascular development and/or endometrial preparation for menstruation. •Reduced numbers of uNK cells in late secretory endometrium of women with HMB.•uNK cells are phenotypically altered in endometrium of women with HMB.•Other leukocyte populations are not altered. Heavy menstrual bleeding (HMB) affects 30% of women of reproductive age and significantly interferes with quality of life. Altered endometrial vascular maturation has been reported in HMB and recurrent miscarriage, the latter associated with increased uterine natural killer (uNK) cell numbers. This study compared endometrial leukocyte populations in controls and women with HMB. Formalin-fixed paraffin-embedded endometrial biopsies from controls (without endometrial pathology) and HMB were immunostained for CD14 (macrophages), CD56 (uNK cells), CD83 (dendritic cells), FOXP3 (regulatory T cells/Tregs), CD3 and CD8 (T cells). Leukocyte numbers were analysed as a percentage of total stromal cells in five randomly selected fields of view in the stratum functionalis of each sample. In control women across the menstrual cycle, 2–8% of total stromal cells were CD3+ cells, 2–4% were CD8+ T cells and 6–8% were CD14+ macrophages. Compared with controls, CD3+ cells were reduced during the mid-secretory phase (4%, P<0.01) and increased in the late secretory phase (12%, P=0.01) in HMB. CD83+ dendritic cells and FOXP3+ Tregs were scarce throughout the menstrual cycle in both groups. In controls, 2% of stromal cells in proliferative endometrium were CD56+ uNK cells, increasing to 17% during the late secretory phase. In HMB, CD56+ uNK cells were increased in the proliferative (5%, P<0.01) and early secretory (4%, P<0.02) phases, but reduced (10%, P<0.01) in the late secretory phase. This study demonstrates dysregulation of uNK cells in HMB, the functional consequence of which may have an impact on endometrial vascular development and/or endometrial preparation for menstruation. |
Author | Bulmer, Judith N. Innes, Barbara A. Lash, Gendie E. Hapangama, Dharani K. Biswas Shivhare, Sourima |
Author_xml | – sequence: 1 givenname: Sourima surname: Biswas Shivhare fullname: Biswas Shivhare, Sourima organization: Reproductive and Vascular Biology Group, Institute of Cellular Medicine, Newcastle University, Newcastle upon Tyne NE2 4HH, UK – sequence: 2 givenname: Judith N. surname: Bulmer fullname: Bulmer, Judith N. organization: Reproductive and Vascular Biology Group, Institute of Cellular Medicine, Newcastle University, Newcastle upon Tyne NE2 4HH, UK – sequence: 3 givenname: Barbara A. surname: Innes fullname: Innes, Barbara A. organization: Reproductive and Vascular Biology Group, Institute of Cellular Medicine, Newcastle University, Newcastle upon Tyne NE2 4HH, UK – sequence: 4 givenname: Dharani K. surname: Hapangama fullname: Hapangama, Dharani K. organization: Department of Women’s and Children’s Health, Institute of Translational Medicine, University of Liverpool, Liverpool Women’s Hospital, Crown Street, Liverpool L8 7SS, UK – sequence: 5 givenname: Gendie E. surname: Lash fullname: Lash, Gendie E. email: gendie.lash@hotmail.com organization: Reproductive and Vascular Biology Group, Institute of Cellular Medicine, Newcastle University, Newcastle upon Tyne NE2 4HH, UK |
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Keywords | Heavy menstrual bleeding Leukocytes Uterine natural killer cells Endometrium |
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Snippet | •Reduced numbers of uNK cells in late secretory endometrium of women with HMB.•uNK cells are phenotypically altered in endometrium of women with HMB.•Other... Highlights • Reduced numbers of uNK cells in late secretory endometrium of women with HMB. • uNK cells are phenotypically altered in endometrium of women with... Heavy menstrual bleeding (HMB) affects 30% of women of reproductive age and significantly interferes with quality of life. Altered endometrial vascular... |
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SubjectTerms | Adult Antigens, CD - immunology CD8-Positive T-Lymphocytes - immunology CD8-Positive T-Lymphocytes - pathology Endometrium Endometrium - immunology Endometrium - pathology Female Heavy menstrual bleeding Humans Killer Cells, Natural - immunology Killer Cells, Natural - pathology Leukocytes Macrophages - immunology Macrophages - pathology Menorrhagia - immunology Menorrhagia - pathology Menstrual Cycle - immunology Middle Aged Obstetrics and Gynecology T-Lymphocytes, Regulatory - immunology T-Lymphocytes, Regulatory - pathology Uterine natural killer cells |
Title | Menstrual cycle distribution of uterine natural killer cells is altered in heavy menstrual bleeding |
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