Pericyte structure and distribution in the cerebral cortex revealed by high-resolution imaging of transgenic mice

Hartmann, David A.; Underly, Robert G.; Grant, Roger I.; Watson, Ashley N.; Lindner, Volkhard; Shih, Andy Y.

doi:10.1117/1.nph.2.4.041402

Cited by 266 publications

(322 citation statements)

References 41 publications

Supporting

Mentioning

293

Contrasting

Unclassified

Order By: Relevance

“…As in past studies, we observed a heterogeneity of mural cell types, ranging from ring-shaped smooth muscle cells on arterioles to pericytes with varying degrees of vessel coverage on pre-capillary arterioles and capillaries (Grant et al, 2017; Hartmann et al, 2015). In this study, we focused on pericytes adorning the mid-capillary regions (Figure 1C).…”

Section: Resultssupporting

confidence: 81%

“…Recent high-resolution optical imaging studies have shown that brain capillary pericytes are organized as a cellular chain along the capillary bed (Hartmann et al, 2015; Hill et al, 2015). Each pericyte extends thin, elongated processes from distinct ovoid cell bodies to contact and communicate with multiple underlying endothelial cells (Allt and Lawrenson, 2001).…”

Section: Introductionmentioning

confidence: 99%

See 1 more Smart Citation

Dynamic Remodeling of Pericytes In Vivo Maintains Capillary Coverage in the Adult Mouse Brain

et al. 2018

Self Cite

View full text Add to dashboard Cite

SUMMARY Direct contact and communication between pericytes and endothelial cells is critical for maintenance of cerebrovascular stability and blood-brain barrier function. Capillary pericytes have thin processes that reach hundreds of micrometers along the capillary bed. The processes of adjacent pericytes come in close proximity but do not overlap, yielding a cellular chain with discrete territories occupied by individual pericytes. Little is known about whether this pericyte chain is structurally dynamic in the adult brain. Using in vivo two-photon imaging in adult mouse cortex, we show that while pericyte somata were immobile, the tips of their processes underwent extensions and/or retractions over days. The selective ablation of single pericytes provoked exuberant extension of processes from neighboring pericytes to contact uncovered regions of the endothelium. Uncovered capillary regions had normal barrier function, but were dilated until pericyte contact was regained. Pericyte structural plasticity may be critical for cerebrovascular health and warrants detailed investigation.

show abstract

Section: Resultssupporting

confidence: 81%

Section: Introductionmentioning

confidence: 99%

Dynamic Remodeling of Pericytes In Vivo Maintains Capillary Coverage in the Adult Mouse Brain

et al. 2018

Self Cite

View full text Add to dashboard Cite

show abstract

“…Confocal images were obtained with a Zeiss LSM 880 imaging system under a 63× water-immersion objective. Cerebral capillaries, precapillary arterioles, and postcapillary venules were identified according to features established in earlier publications (5,43,44) and briefly as follows: (i) αSMA-negative vessels with a vascular lumen diameter < 10 μm were identified as capillaries; (ii) αSMA-positive vessels terminating before αSMA-negative capillaries were identified as precapillary arterioles; and (iii) αSMA-negative vessels with a vascular lumen diameter 10-20 μm were identified as postcapillary venules.…”

Section: Methodsmentioning

confidence: 99%

CD146 coordinates brain endothelial cell–pericyte communication for blood–brain barrier development

Chen

Luo

Hui

et al. 2017

Proc. Natl. Acad. Sci. U.S.A.

162

140

View full text Add to dashboard Cite

The blood-brain barrier (BBB) establishes a protective interface between the central neuronal system and peripheral blood circulation and is crucial for homeostasis of the CNS. BBB formation starts when the endothelial cells (ECs) invade the CNS and pericytes are recruited to the nascent vessels during embryogenesis. Despite the essential function of pericyte-EC interaction during BBB development, the molecular mechanisms coordinating the pericyte-EC behavior and communication remain incompletely understood. Here, we report a single cell receptor, CD146, that presents dynamic expression patterns in the cerebrovasculature at the stages of BBB induction and maturation, coordinates the interplay of ECs and pericytes, and orchestrates BBB development spatiotemporally. In mouse brain, CD146 is first expressed in the cerebrovascular ECs of immature capillaries without pericyte coverage; with increased coverage of pericytes, CD146 could only be detected in pericytes, but not in cerebrovascular ECs. Specific deletion of Cd146 in mice ECs resulted in reduced brain endothelial claudin-5 expression and BBB breakdown. By analyzing mice with specific deletion of Cd146 in pericytes, which have defects in pericyte coverage and BBB integrity, we demonstrate that CD146 functions as a coreceptor of PDGF receptor-β to mediate pericyte recruitment to cerebrovascular ECs. Moreover, we found that the attached pericytes in turn downregulate endothelial CD146 by secreting TGF-β1 to promote further BBB maturation. These results reveal that the dynamic expression of CD146 controls the behavior of ECs and pericytes, thereby coordinating the formation of a mature and stable BBB.lood-brain barrier (BBB) development is a sequential and well-orchestrated process that commences when brain endothelial cells (ECs; BECs) invade the embryonic neuroectoderm from the surrounding vascular plexus and induce BBB properties by establishing paracellular tight junctions (TJs) (1). Endothelial TJs are formed by a complex of transmembrane proteins, including claudins and occludin, as well as cytoplasmic adaptors such as zonula occludens protein 1 (ZO-1), thus creating a highresistance paracellular barrier to molecules and ions (2). Compelling evidence shows that claudin-5 plays a key role in the induction of BBB properties, and specific loss of claudin-5 in mice results in a more leaky BBB (3-5). Following the establishment of the TJs, the BECs of nascent vessels recruit pericytes to the endothelial walls, which improve the barrier function of BECs by stabilizing TJs and decreasing transcytosis, and are crucial for maturation of the BBB (6). Importantly, pericytes suppress the expression of leukocyte adhesion molecules (LAMs) in BECs to reduce the invasion of immune cells into the CNS, therefore regulating CNS immune surveillance, a critical feature of the mature BBB (6, 7). Thus, as a dynamic interface with a range of interrelated functions, the BBB results from extremely effective TJs, pericyte recruitment, and regulation of leukocyte extravasation, there...

show abstract

“…Recent studies of the cortical angioarchitecture in mice expressing fluorescent proteins under control of the NG2 and PDGFRβ promoters have identified several pericyte subpopulations including VSMC-pericyte hybrid on pre-capillary arterioles, thin strand helical mid-capillary pericyte, and mesh pericyte with a stellate morphology on post-capillary arterioles and venules 19,20 . Future single-cell RNA-seq and proteomic studies as used successfully to characterize subpopulations of cortical progenitor cells 23 and drug resistant tumor cells 24 , may also contribute to better understanding of different pericyte subtypes.…”

Section: Pericytes: Characterization Function and Dysfunctionmentioning

confidence: 99%

Pericytes of the neurovascular unit: key functions and signaling pathways

Ayyadurai²,

2016

View full text Add to dashboard Cite

Pericytes are vascular mural cells embedded in the basement membrane of blood microvessels. They extend their processes along capillaries, pre-capillary arterioles, and post-capillary venules. The central nervous system (CNS) pericytes are uniquely positioned within the neurovascular unit between endothelial cells, astrocytes, and neurons. They integrate, coordinate, and process signals from their neighboring cells to generate diverse functional responses that are critical for CNS functions in health and disease including regulation of the blood-brain barrier permeability, angiogenesis, clearance of toxic metabolites, capillary hemodynamic responses, neuroinflammation, and stem cell activity. Here, we examine the key signaling pathways between pericytes and their neighboring endothelial cells, astrocytes, and neurons that control neurovascular functions. We also review the role of pericytes in different CNS disorders including rare monogenic diseases and complex neurological disorders such as Alzheimer's disease and brain tumors. Finally, we discuss directions for future studies.

show abstract

Pericyte structure and distribution in the cerebral cortex revealed by high-resolution imaging of transgenic mice

Cited by 266 publications

References 41 publications

Dynamic Remodeling of Pericytes In Vivo Maintains Capillary Coverage in the Adult Mouse Brain

Dynamic Remodeling of Pericytes In Vivo Maintains Capillary Coverage in the Adult Mouse Brain

CD146 coordinates brain endothelial cell–pericyte communication for blood–brain barrier development

Pericytes of the neurovascular unit: key functions and signaling pathways

Contact Info

Product

Resources

About