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2157-P: Tyrosine Hydroxylase-Containing Cells in the Human Fetal Pancreas

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Tyrosine hydroxylase (TH) - the specific marker of the catecholamine synthesizing cells, has been detected in the pancreatic endocrine, acinar and ductal cells in some mammals. In the developing mouse pancreas, TH+ cells are often contained glucagon and shared some features that are characteristics for differentiated endocrine cells. As it was shown in experimental studies on mice, a non-neural catecholaminergic pathway appears to modulate pancreatic endocrine precursor and insulin producing cell neogenesis. Our aim was to evaluate whether TH+ cells are present in the developing human pancreas. We have analyzed pancreatic autopsies from 34 human fetuses (10-37 gestational weeks (g.w.)) using double immunofluorescent labeling with antibodies to TH and either insulin or glucagon. Rare TH+ cells were found in the pancreas of all fetuses from 10th to 21th g.w., which were not detected later in development. At early stages (10-12 g.w.), such cells were located among the epithelial cells of primitive ducts, often in close proximity to the endocrine cell clusters, or were associated with the TH+ nerve bundles. In the pancreas of fetuses from 14th to 21th g.w., TH+ cells were observed in the nerve bundles, nerve ganglia and in the neuro-inular complexes type 1 (endocrine cells integrated with the neurons and nerve fibers). Some of the TH+ cells simultaneously contained glucagon. However, the majority of the TH+ cells were negative for insulin or glucagon. Thus, we first detected TH+ cells in the human fetal pancreas. These cells may be differentiating endocrine cells, because some of the TH+ cells were located in the ductal epithelium and rarely contained glucagon. Similarly with mice, non-neural catecholamines may be involved in the endocrine cells differentiation during human pancreas development. Disclosure Y. Krivova: None. A. Proshchina: None. D. Otlyga: None. O. Leonova: None. V. Popenko: None. V. Barabanov: None. S. Saveliev: None. Funding Russian Foundation for Basic Research (18-015-00146)
Title: 2157-P: Tyrosine Hydroxylase-Containing Cells in the Human Fetal Pancreas
Description:
Tyrosine hydroxylase (TH) - the specific marker of the catecholamine synthesizing cells, has been detected in the pancreatic endocrine, acinar and ductal cells in some mammals.
In the developing mouse pancreas, TH+ cells are often contained glucagon and shared some features that are characteristics for differentiated endocrine cells.
As it was shown in experimental studies on mice, a non-neural catecholaminergic pathway appears to modulate pancreatic endocrine precursor and insulin producing cell neogenesis.
Our aim was to evaluate whether TH+ cells are present in the developing human pancreas.
We have analyzed pancreatic autopsies from 34 human fetuses (10-37 gestational weeks (g.
w.
)) using double immunofluorescent labeling with antibodies to TH and either insulin or glucagon.
Rare TH+ cells were found in the pancreas of all fetuses from 10th to 21th g.
w.
, which were not detected later in development.
At early stages (10-12 g.
w.
), such cells were located among the epithelial cells of primitive ducts, often in close proximity to the endocrine cell clusters, or were associated with the TH+ nerve bundles.
In the pancreas of fetuses from 14th to 21th g.
w.
, TH+ cells were observed in the nerve bundles, nerve ganglia and in the neuro-inular complexes type 1 (endocrine cells integrated with the neurons and nerve fibers).
Some of the TH+ cells simultaneously contained glucagon.
However, the majority of the TH+ cells were negative for insulin or glucagon.
Thus, we first detected TH+ cells in the human fetal pancreas.
These cells may be differentiating endocrine cells, because some of the TH+ cells were located in the ductal epithelium and rarely contained glucagon.
Similarly with mice, non-neural catecholamines may be involved in the endocrine cells differentiation during human pancreas development.
Disclosure Y.
Krivova: None.
A.
Proshchina: None.
D.
Otlyga: None.
O.
Leonova: None.
V.
Popenko: None.
V.
Barabanov: None.
S.
Saveliev: None.
Funding Russian Foundation for Basic Research (18-015-00146).

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