Your search keyword '"Economides, Aris N"' showing total 3 results

1. Anti-ACVRI antibodies exacerbate heterotopic ossification in fibrodysplasia ossificans progressive (FOP) by activating FOP-mutant ACVR1

Author

Aykul, Senem, Huang, Lily, Wang, Lili, Das, Nanditha M., Reisman, Sandra, Ray, Yonaton, Zhang, Qian, Rothman, Nyanza, Nannuru, Kalyan C., Brydges, Vishal KamaSusannah, Troncone, Luca, Johnsen, Laura, Yu, Paul B., Fazio, Sergio, Lees-Shepard, John, Schutz, Kevin, Murphy, Andrew J., Economides, Aris N., Idone, Vincent, and Hatsell, Sarah J.

Subjects

Autoantibodies -- Physiological aspects -- Health aspects -- Genetic aspects, Connective tissue diseases -- Development and progression -- Genetic aspects, Growth factor receptors -- Genetic aspects -- Physiological aspects, Health care industry

Abstract

Fibrodysplasia ossificans progressiva (FOP) is a rare genetic disorder whose most debilitating pathology is progressive and cumulative heterotopic ossification (HO) of skeletal muscles, ligaments, tendons, and fascia. FOP is caused by mutations in the type I BMP receptor gene ACVR1, which enable ACVR1 to utilize its natural antagonist, activin A, as an agonistic ligand. The physiological relevance of this property is underscored by the fact that HO in FOP is exquisitely dependent on activation of FOP-mutant ACVR1 by activin A, an effect countered by inhibition of anti-activin A via monoclonal antibody treatment. Hence, we surmised that anti-ACVR1 antibodies that block activation of ACVR1 by ligands should also inhibit HO in FOP and provide an additional therapeutic option for this condition. Therefore, we generated anti-ACVR1 monoclonal antibodies that block ACVR1's activation by its ligands. Surprisingly, in vivo, these anti-ACVR1 antibodies stimulated HO and activated signaling of FOP-mutant ACVR1. This property was restricted to FOPmutant ACVR1 and resulted from anti-ACVR1 antibody-mediated dimerization of ACVR1. Conversely, wild-type ACVR1 was inhibited by anti-ACVR1 antibodies. These results uncover an additional property of FOP-mutant ACVR1 and indicate that anti-ACVR1 antibodies should not be considered as therapeutics for FOP., Introduction Fibrodysplasia ossificans progressiva (FOP) (OMIM #135100) is a rare, autosomal dominant disorder characterized by congenital skeletal dysplasias and progressive and cumulative heterotopic ossification (HO) of skeletal muscles, tendons, ligaments, [...]

Published

2022

2. A lymphatic defect causes ocular hypertension and glaucoma in mice

Author

Thomson, Benjamin R., Heinen, Stefan, Jeansson, Marie, Ghosh, Asish K., Fatima, Anees, Sung, Hoon-Ki, Onay, Tuncer, Chen, Hui, Yamaguchi, Shinji, Economides, Aris N., Flenniken, Ann, Gale, Nicholas W., Hong, Young-Kwon, Fawzi, Amani, Liu, Xiaorong, Kume, Tsutomu, and Quaggin, Susan E.

Subjects

Eye diseases -- Development and progression -- Genetic aspects, Lymphatic diseases -- Complications and side effects -- Genetic aspects, Cellular signal transduction -- Genetic aspects, Health care industry

Abstract

Glaucoma is a leading cause of blindness, afflicting more than 60 million people worldwide. Increased intraocular pressure (IOP) due to impaired aqueous humor drainage is a major risk factor for the development of glaucoma. Here, we demonstrated that genetic disruption of the angiopoietin/TIE2 (ANGPT/TIE2) signaling pathway results in high IOP, buphthalmos, and classic features of glaucoma, including retinal ganglion degeneration and vision loss. Eyes from mice with induced deletion of Angptl and Angpt2 (A1A2[Flox.sup.WB] mice) lacked drainage pathways in the corneal limbus, including Schlemm's canal and lymphatic capillaries, which share expression of the PROX1, VEGFR3, and FOXC family of transcription factors. VEGFR3 and FOXCs have been linked to lymphatic disorders in patients, and FOXC1 has been linked to glaucoma. In contrast to blood endothelium, in which ANGPT2 is an antagonist of ANGPT1, we have shown that both ligands cooperate to regulate TIE2 in the lymphatic network of the eye. While A1A2[Flox.sup.WB] mice developed high IOP and glaucoma, expression of ANGPT1 or ANGPT2 alone was sufficient for ocular drainage. Furthermore, we demonstrated that loss of FOXC2 from lymphatics results in TIE2 downregulation, suggesting a mechanism for ocular defects in patients with FOXC mutations. These data reveal a pathogenetic and molecular basis for glaucoma and demonstrate the importance of angiopoietin ligand cooperation in the lymphatic endothelium., Introduction The angiopoietin/TIE2 (ANGPT/TIE2) signaling pathway is a major regulator of vascular development, and altered expression of ANGPT ligands or activity of the TIE2 receptor is linked to a variety [...]

Published

2014

3. Loss of the BMP antagonist USAG-1 ameliorates disease in a mouse model of the progressive hereditary kidney disease Alport syndrome

Author

Tanaka, Mari, Asada, Misako, Higashi, Atsuko Y., Nakamura, Jin, Oguchi, Akiko, Tomita, Mayumi, Yamada, Sachiko, Asada, Nariaki, Takase, Masayuki, Okuda, Tomohiko, Kawachi, Hiroshi, Economides, Aris N., Robertson, Elizabeth, Takahashi, Satoru, Sakurai, Takeshi, Goldschmeding, Roel, Muso, Eri, Fukatsu, Atsushi, Kita, Toru, and Yanagita, Motoko

Subjects

Animal models in research -- Usage -- Genetic aspects -- Physiological aspects -- Research, Bone morphogenetic proteins -- Physiological aspects -- Genetic aspects -- Research -- Usage, Alport's syndrome -- Risk factors -- Genetic aspects -- Research, Health care industry

Abstract

The glomerular basement membrane (GBM) is a key component of the filtering unit in the kidney. Mutations involving any of the collagen IV genes (COL4A3, COL4A4, and COL4A5) affect GBM assembly and cause Alport syndrome, a progressive hereditary kidney disease with no definitive therapy. Previously, we have demonstrated that the bone morphogenetic protein (BMP) antagonist uterine sensitization-associated gene-1 (USAG-1) negatively regulates the renoprotective action of BMP-7 in a mouse model of tubular injury during acute renal failure. Here, we investigated the role of USAG-1 in renal function in [Col4a3.sup.[-/-]] mice, which model Alport syndrome. Ablation of Usag1 in [Col4a3.sup.[-/-]]mice led to substantial attenuation of disease progression, normalization of GBM ultrastructure, preservation of renal function, and extension of life span. Immunohistochemical analysis revealed that USAG-1 and BMP-7 colocalized in the macula densa in the distal tubules, lying in direct contact with glomerular mesangial cells. Furthermore, in cultured mesangial cells, BMP-7 attenuated and USAG-1 enhanced the expression of MMP-12, a protease that may contribute to GBM degradation. These data suggest that the pathogenetic role of USAG-1 in [Col4a3.sup.[-/-]] mice might involve crosstalk between kidney tubules and the glomerulus and that inhibition of USAG-1 may be a promising therapeutic approach for the treatment of Alport syndrome., Introduction The renal glomerular basement membrane (GBM) contributes importantly to maintenance of the structural integrity of the glomerular capillaries (1), (2). Type IV collagen is the major component of the [...]

Published

2010