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Klf4 has an unexpected protective role in perivascular cells within the microvasculature.

ABSTRACT: Recent smooth muscle cell (SMC) lineage-tracing studies have revealed that SMCs undergo remarkable changes in phenotype during development of atherosclerosis. Of major interest, we demonstrated that Kruppel-like factor 4 (KLF4) in SMCs is detrimental for overall lesion pathogenesis, in that SMC-specific conditional knockout of the KLF4 gene ( Klf4) resulted in smaller, more-stable lesions that exhibited marked reductions in the numbers of SMC-derived macrophage- and mesenchymal stem cell-like cells. However, since the clinical consequences of atherosclerosis typically occur well after our reproductive years, we sought to identify beneficial KLF4-dependent SMC functions that were likely to be evolutionarily conserved. We tested the hypothesis that KLF4-dependent SMC transitions play an important role in the tissue injury-repair process. Using SMC-specific lineage-tracing mice positive and negative for simultaneous SMC-specific conditional knockout of Klf4, we demonstrate that SMCs in the remodeling heart after ischemia-reperfusion injury (IRI) express KLF4 and transition to a KLF4-dependent macrophage-like state and a KLF4-independent myofibroblast-like state. Moreover, heart failure after IRI was exacerbated in SMC Klf4 knockout mice. Surprisingly, we observed a significant cardiac dilation in SMC Klf4 knockout mice before IRI as well as a reduction in peripheral resistance. KLF4 chromatin immunoprecipitation-sequencing analysis on mesenteric vascular beds identified potential baseline SMC KLF4 target genes in numerous pathways, including PDGF and FGF. Moreover, microvascular tissue beds in SMC Klf4 knockout mice had gaps in lineage-traced SMC coverage along the resistance arteries and exhibited increased permeability. Together, these results provide novel evidence that Klf4 has a critical maintenance role within microvascular SMCs: it is required for normal SMC function and coverage of resistance arteries. NEW & NOTEWORTHY We report novel evidence that the Kruppel-like factor 4 gene ( Klf4) has a critical maintenance role within microvascular smooth muscle cells (SMCs). SMC-specific Klf4 knockout at baseline resulted in a loss of lineage-traced SMC coverage of resistance arteries, dilation of resistance arteries, increased blood flow, and cardiac dilation.

SUBMITTER: Haskins RM

PROVIDER: S-EPMC6139624 | biostudies-literature | 2018 Aug

REPOSITORIES: biostudies-literature

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Klf4 has an unexpected protective role in perivascular cells within the microvasculature.

Haskins Ryan M RM Nguyen Anh T AT Alencar Gabriel F GF Billaud Marie M Kelly-Goss Molly R MR Good Miranda E ME Bottermann Katharina K Klibanov Alexander L AL French Brent A BA Harris Thurl E TE Peirce Shayn M SM Isakson Brant E BE Owens Gary K GK

American journal of physiology. Heart and circulatory physiology 20180406 2

Recent smooth muscle cell (SMC) lineage-tracing studies have revealed that SMCs undergo remarkable changes in phenotype during development of atherosclerosis. Of major interest, we demonstrated that Kruppel-like factor 4 (KLF4) in SMCs is detrimental for overall lesion pathogenesis, in that SMC-specific conditional knockout of the KLF4 gene ( Klf4) resulted in smaller, more-stable lesions that exhibited marked reductions in the numbers of SMC-derived macrophage- and mesenchymal stem cell-like ce ...[more]

PMID: 29631369

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Project description:Recent smooth muscle cell (SMC) lineage tracing studies have demonstrated that SMCs undergo remarkable changes in phenotype during development of atherosclerosis, including loss of typical SMC markers such as ACTA2 and Klf4 dependent activation of multiple markers of macrophages and mesenchymal stem cells. Of major interest, we showed Klf4 in SMC is critical for overall lesion pathogenesis as SMC-specific conditional knockout (KO) of Klf4 resulted in smaller, more stable lesions that exhibited marked reductions in the numbers of SMC-derived macrophage-like and mesenchymal stem cell like cells. Herein we tested the hypothesis that Klf4 dependent SMC transitions are beneficial following myocardial infarction (MI). Utilizing SMC-specific lineage tracing mice +/- simultaneous SMC-specific conditional KO of Klf4, we demonstrate that SMCs express Klf4 and transition to a Klf4 dependent macrophage-like state as well as a Klf4 independent myofibroblast-like state. SMC specific, conditional KO of Klf4 resulted in marked exacerbation of heart failure following MI. Surprisingly, significant cardiac dilation was seen in SMC-Klf4 KO mice prior to MI. This cardiac dilation was accompanied by a reduction in peripheral resistance, as evidenced by a reduction in blood pressure, an increase in blood flow, and a larger passive diameter of mesenteric resistance arteries as measured by pressure myography. Klf4 ChIP-Seq analysis on the mesenteric resistance arteries identified potential Klf4 target genes in SMC at baseline in pathways including PDGF and FGF signaling previously shown to be important for perivascular cell investment. Interestingly, examination of microvascular tissue beds revealed gaps in lineage traced SMC coverage along the resistance arteries. Taken together, these results provide novel evidence that Klf4 has a critical maintenance role within microvascular SMCs, including being required for normal SMC coverage of resistance arteries as well as their function.

Project description:Mycobacterium tuberculosis (Mtb), the causative agent of tuberculosis (TB), infects one third of the world's population. Among these infections, clinical isolates belonging to the W-Beijing appear to be emerging, representing about 50% of Mtb isolates in East Asia, and about 13% of all Mtb isolates worldwide. In animal models, infection with W-Beijing strain, Mtb HN878, is considered "hypervirulent" as it results in increased mortality and causes exacerbated immunopathology in infected animals. We had previously shown the Interleukin (IL) -17 pathway is dispensable for primary immunity against infection with the lab adapted Mtb H37Rv strain. However, it is not known whether IL-17 has any role to play in protective immunity against infection with clinical Mtb isolates. We report here that lab adapted Mtb strains, such as H37Rv, or less virulent Mtb clinical isolates, such as Mtb CDC1551, do not require IL-17 for protective immunity against infection while infection with Mtb HN878 requires IL-17 for early protective immunity. Unexpectedly, Mtb HN878 induces robust production of IL-1β through a TLR-2-dependent mechanism, which supports potent IL-17 responses. We also show that the role for IL-17 in mediating protective immunity against Mtb HN878 is through IL-17 Receptor signaling in non-hematopoietic cells, mediating the induction of the chemokine, CXCL-13, which is required for localization of T cells within lung lymphoid follicles. Correct T cell localization within lymphoid follicles in the lung is required for maximal macrophage activation and Mtb control. Since IL-17 has a critical role in vaccine-induced immunity against TB, our results have far reaching implications for the design of vaccines and therapies to prevent and treat emerging Mtb strains. In addition, our data changes the existing paradigm that IL-17 is dispensable for primary immunity against Mtb infection, and instead suggests a differential role for IL-17 in early protective immunity against emerging Mtb strains.

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Klf4 has an unexpected protective role in perivascular cells within the microvasculature.

Publications

Klf4 has an unexpected protective role in perivascular cells within the microvasculature.

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