4.4 Article

Perivascular macrophages produce type I collagen around cerebral small vessels under prolonged hypertension in rats

Journal

HISTOCHEMISTRY AND CELL BIOLOGY
Volume 155, Issue 4, Pages 503-512

Publisher

SPRINGER
DOI: 10.1007/s00418-020-01948-9

Keywords

Cerebral arteriolosclerosis; Hypertension; Perivascular macrophages; Type I collagen

Funding

  1. Jichi Medical University Young Investigator Award
  2. Jichi Medical University School of Medicine

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Hypertension leads to structural remodeling of cerebral blood vessels, involving fibrosis and type I collagen production, with perivascular macrophages (PVMs) found to be involved in collagen production near cerebral small vessels in rats. This highlights the potential role of PVMs in vascular fibrosis under hypertensive conditions.
Hypertension leads to structural remodeling of cerebral blood vessels, which has been implicated in the pathophysiology of cerebrovascular diseases. The remodeling and progression of arteriolosclerosis under hypertension involve fibrosis along with the production of type I collagen around cerebral arterioles. However, the source and regulatory mechanisms of this collagen production remain elusive. In this study, we examined if perivascular macrophages (PVMs) are involved in collagen production around cerebral small vessels in hypertensive SHRSP/Izm rats. Immunoreactivity for type I collagen around cerebral small vessels in 12-week-old hypertensive rats tended to higher than those in 4-week-old hypertensive and 12-week-old control rats. In ultrastructural analyses using transmission electron microscopy, the substantial deposition of collagen fibers could be observed in the intercellular spaces around PVMs near the arterioles of rats with prolonged hypertension. In situ hybridization analyses revealed that cells positive for mRNA of Col1a1, which comprises type I collagen, were observed near cerebral small vessels. The Col1a1-positive cells around cerebral small vessels were colocalized with immunoreactivity for CD206, a marker for PVMs, but not with those for glial fibrillary acidic protein or desmin, markers for other perivascular cells such as astrocytes and vascular smooth muscle cells. These results demonstrated that enhanced production of type I collagen is observed around cerebral small vessels in rats with prolonged hypertension and Col1a1 is expressed by PVMs, and support the concept that PVMs are involved in collagen production and vascular fibrosis under hypertensive conditions.

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