Microenvironmental Regulation by Fibrillin-1

Sengle, Gerhard; Tsutsui, Ko; Keene, Douglas R.; Tufa, Sara F.; Carlson, Eric; Charbonneau, Noé L.; Ono, Robert N.; Sasaki, Takako; Wirtz, Mary K.; Samples, John R.; Fessler, Liselotte I.; Fessler, John H.; Sekiguchi, Kiyotoshi; Hayflick, Susan J.; Sakai, Lynn Y.

doi:10.1371/journal.pgen.1002425

Cited by 128 publications

(195 citation statements)

References 37 publications

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“…6 Although Weill-Marchesani patients are opposite to Marfan patients in outward appearance, the syndromes share a common molecular mechanism, which is defective fibrillin-1 microfibrils. 33,73,77 Further supporting a role for ADAMTS10 in microfibril function, co-localization of ADAMTS10 and fibrillin-1 has been shown by immunohistochemistry of human skin 33,73 and ADAMTS10 has been shown to promote microfibril formation in cell culture. 73 Specific and high-affinity binding of ADAMTS10 to fibrillin-1 has been demonstrated by affinity blotting assays, affinity pull-down assays, and surface plasmon resonance.…”

mentioning

confidence: 80%

“…28 While important, integrin activation with LAP does not apply to TGFb2 activation because it does not have an RGD domain in its LAP, unlike the other TGFbs. A critical role for microfibrils in TGFb activation is suggested by a number of diseases that have chronic activation of TGFb signaling associated with mutations in fibrillin-1 or other microfibril-related diseases, including Marfan syndrome, [29][30][31][32] Weill-Marchesani syndrome, 33 acromicric dysplasia, 34 geleophysic dysplasia, 34,35 congenital scleroderma, 36 and cutis laxa. 37,38 …”

Section: Microfibrils Control Location and Activation Of Tgfbmentioning

confidence: 99%

“…73 Specific and high-affinity binding of ADAMTS10 to fibrillin-1 has been demonstrated by affinity blotting assays, affinity pull-down assays, and surface plasmon resonance. 33,73 The binding site on fibrillin-1 for ADAMTS10 overlaps with the binding site for other ADAMTS proteins, 33 suggesting competition for the fibrillin-1 binding site or complex formation with other microfibril-associated proteins.…”

mentioning

confidence: 99%

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The Microfibril Hypothesis of Glaucoma: Implications for Treatment of Elevated Intraocular Pressure

Kuchtey

2014

Journal of Ocular Pharmacology and Therapeutics

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Microfibrils are macromolecular aggregates located in the extracellular matrix of both elastic and nonelastic tissues that have essential functions in formation of elastic fibers and control of signaling through the transforming growth factor beta (TGFb) family of cytokines. Elevation of systemic TGFb and chronic activation of TGFb signal transduction are associated with diseases caused by mutations in microfibril-associated genes, including FBN1. A role for microfibrils in glaucoma is suggested by identification of risk alleles in LOXL1 for exfoliation glaucoma and mutations in LTBP2 for primary congenital glaucoma, both of which are microfibrilassociated genes.

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mentioning

confidence: 80%

Section: Microfibrils Control Location and Activation Of Tgfbmentioning

confidence: 99%

mentioning

confidence: 99%

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The Microfibril Hypothesis of Glaucoma: Implications for Treatment of Elevated Intraocular Pressure

Kuchtey

2014

Journal of Ocular Pharmacology and Therapeutics

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“…Several arguments are in favor of a role of ADAMTS17 in growth regulation (for summary, see Table 3), including: (1) significant association with height in population GWAS; 1 (2) a short child with a similar terminal deletion in the DECIPHER database; (3) significant association with size in a GWAS in the domestic dog; 29 (4) human mutations in ADAMTS17 causing the acromelic chondrodysplasia Weill-Marchesani-like syndrome (OMIM #277600 and #608328); [30][31][32][33] and (5) association of members of the ADAMTSL/ADAMTS family with the modulation of fibrillin-1 function. 31,33 Unfortunately, expression of the rodent homolog of ADAMTS17 could not be investigated, because the gene was not represented on the microarrays used. Besides ADAMTS17, this deletion contains three other genes, ALDH1A3, LRRK1 and CHSY1, that might be implicated in short stature.…”

Section: Discussionmentioning

confidence: 99%

“…39 Case II.17, described previously, 12 carries a duplication of 3p12.3 containing part of ROBO2, encoding a receptor for SLIT2 and probably SLIT1, thought to function in axon guidance and cell migration. 40 Case II.21, born SGA, length À3.7 SDS and head circumference À3.1 SDS presented with clinodactily, a protruded [30][31][32][33] Associated with fibrillin-1 function. 31,33 Aldh1a3 and Lrrk1 higher expressed in murine GP; Chsy1 highly expressed in HZ and downregulated with age.…”

Section: Discussionmentioning

confidence: 99%

Copy number variants in patients with short stature

et al. 2013

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Retracted: Long non‐coding RNA PGM5‐AS1 promotes epithelial‐mesenchymal transition, invasion and metastasis of osteosarcoma cells by impairing miR‐140‐5p‐mediated FBN1 inhibition

Liu

Gao

et al. 2020

Molecular Oncology

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Osteosarcoma is an uncommon tumor occurring in bone, accompanied by elevated incidence and reduced rate of healing. Epithelial-to-mesenchymal transition (EMT) serves as a conceptual paradigm to explain the invasion and metastasis of osteosarcoma and other cancers. Hence, developing effective therapeutic strategy to treat the EMT of osteosarcoma is essential. Here, we identified the molecular mechanism of long noncoding RNA (lncRNA) PGM5-AS1 in EMT and progression of osteosarcoma. Microarray-based analysis was employed to screen the osteosarcoma-related differentially expressed lncRNAs. The levels of PGM5-AS1 as well as microRNA-140-5p (miR-140-5p) and fibrillin-1 (FBN1) in osteosarcoma tissues and cells were determined. Dual-luciferase reporter gene assay, RNA pull-down assay, and RNA immunoprecipitation assay were conducted to validate the relationship among PGM5-AS1, miR-140-5p, and FBN1. Expression of PGM5-AS1, miR-140-5p, and FBN1 was altered by overexpression, shRNA, mimic, or inhibitors in order to investigate how they regulated migration, invasion, and EMT of osteosarcoma cells in vitro. Loss-and gain-of-function approaches were employed in nude mice to detect their roles in tumorigenesis in vivo. Osteosarcoma tissues and cells exhibited low expression of miR-140-5p, but high expression of PGM5-AS1 and FBN1. PGM5-AS1 competitively bound to miR-140-5p to upregulate FBN1. Furthermore, hindering PGM5-AS1 and FBN1 or overexpressing miR-140-5p dampened migration, invasion, and EMT of osteosarcoma cells in vitro. Furthermore, silencing PGM5-AS1 or FBN1, or overexpressing miR-140-5p markedly inhibited tumorigenesis in nude mice in vivo. Taken together, PGM5-AS1 depletion causes FBN1 reduction to retard osteosarcoma processes by negatively modulating miR-140-5p.

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Microenvironmental Regulation by Fibrillin-1

Cited by 128 publications

References 37 publications

The Microfibril Hypothesis of Glaucoma: Implications for Treatment of Elevated Intraocular Pressure

The Microfibril Hypothesis of Glaucoma: Implications for Treatment of Elevated Intraocular Pressure

Copy number variants in patients with short stature

Retracted: Long non‐coding RNA PGM5‐AS1 promotes epithelial‐mesenchymal transition, invasion and metastasis of osteosarcoma cells by impairing miR‐140‐5p‐mediated FBN1 inhibition

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