Your search keyword '"Bogomolovas, J."' showing total 7 results

1. Titin antibodies in 'seronegative' myasthenia gravis - A new role for an old antigen

Author

Stergiou, C., Lazaridis, K., Zouvelou, V., Tzartos, J., Mantegazza, R., Antozzi, C., Andreetta, F., Evoli Stampanoni-B, Amelia, Deymeer, F., Saruhan Direskeneli, G., Durmus, H., Brenner, T., Vaknin, A., Berrih Aknin, S., Behin, A., Sharshar, T., De Baets, M., Losen, M., Martinez Martinez, P., Kleopa, K. A., Zamba Papanicolaou, E., Kyriakides, T., Kostera Pruszczyk, A., Szczudlik, P., Szyluk, B., Lavrnic, D., Basta, I., Peric, S., Tallaksen, C., Maniaol, A., Gilhus, N. E., Casasnovas Pons, C., Pitha, J., Jakubíkova, M., Hanisch, F., Bogomolovas, J., Labeit, D., Labeit, S., Tzartos, S. J., Evoli, Amelia (ORCID:0000-0003-0282-8787), Stergiou, C., Lazaridis, K., Zouvelou, V., Tzartos, J., Mantegazza, R., Antozzi, C., Andreetta, F., Evoli Stampanoni-B, Amelia, Deymeer, F., Saruhan Direskeneli, G., Durmus, H., Brenner, T., Vaknin, A., Berrih Aknin, S., Behin, A., Sharshar, T., De Baets, M., Losen, M., Martinez Martinez, P., Kleopa, K. A., Zamba Papanicolaou, E., Kyriakides, T., Kostera Pruszczyk, A., Szczudlik, P., Szyluk, B., Lavrnic, D., Basta, I., Peric, S., Tallaksen, C., Maniaol, A., Gilhus, N. E., Casasnovas Pons, C., Pitha, J., Jakubíkova, M., Hanisch, F., Bogomolovas, J., Labeit, D., Labeit, S., Tzartos, S. J., and Evoli, Amelia (ORCID:0000-0003-0282-8787)

Abstract

Myasthenia gravis (MG) is an autoimmune disease caused by antibodies targeting the neuromuscular junction of skeletal muscles. Triple-seronegative MG (tSN-MG, without detectable AChR, MuSK and LRP4 antibodies), which accounts for ~ 10% of MG patients, presents a serious gap in MG diagnosis and complicates differential diagnosis of similar disorders. Several AChR antibody positive patients (AChR-MG) also have antibodies against titin, usually detected by ELISA. We have developed a very sensitive radioimmunoprecipitation assay (RIPA) for titin antibodies, by which many previously negative samples were found positive, including several from tSN-MG patients. The validity of the RIPA results was confirmed by western blots. Using this RIPA we screened 667 MG sera from 13 countries; as expected, AChR-MG patients had the highest frequency of titin antibodies (40.9%), while MuSK-MG and LRP4-MG patients were positive in 14.6% and 16.4% respectively. Most importantly, 13.4% (50/372) of the tSN-MG patients were also titin antibody positive. None of the 121 healthy controls or the 90 myopathy patients, and only 3.6% (7/193) of other neurological disease patients were positive. We thus propose that the present titin antibody RIPA is a useful tool for serological MG diagnosis of tSN patients.

Published

2016

2. Molecular basis for the fold organization and sarcomeric targeting of the muscle atrogin MuRF1

Author

Franke, B., Gasch, A., Rodriguez, D., Chami, M., Khan, M.M., Rudolf, R., Bibby, J., Hanashima, A., Bogomolovas, J., Castelmur, E. von, Rigden, D.J., Uson, I., Labeit, S., Mayans, O., Franke, B., Gasch, A., Rodriguez, D., Chami, M., Khan, M.M., Rudolf, R., Bibby, J., Hanashima, A., Bogomolovas, J., Castelmur, E. von, Rigden, D.J., Uson, I., Labeit, S., and Mayans, O.

Abstract

Contains fulltext : 137461.pdf (publisher's version ) (Open Access), MuRF1 is an E3 ubiquitin ligase central to muscle catabolism. It belongs to the TRIM protein family characterized by a tripartite fold of RING, B-box and coiled-coil (CC) motifs, followed by variable C-terminal domains. The CC motif is hypothesized to be responsible for domain organization in the fold as well as for high-order assembly into functional entities. But data on CC from this family that can clarify the structural significance of this motif are scarce. We have characterized the helical region from MuRF1 and show that, contrary to expectations, its CC domain assembles unproductively, being the B2- and COS-boxes in the fold (respectively flanking the CC) that promote a native quaternary structure. In particular, the C-terminal COS-box seemingly forms an alpha-hairpin that packs against the CC, influencing its dimerization. This shows that a C-terminal variable domain can be tightly integrated within the conserved TRIM fold to modulate its structure and function. Furthermore, data from transfected muscle show that in MuRF1 the COS-box mediates the in vivo targeting of sarcoskeletal structures and points to the pharmacological relevance of the COS domain for treating MuRF1-mediated muscle atrophy.

Published

2014

3. Molecular basis for the fold organization and sarcomeric targeting of the muscle atrogin MuRF1

Author

Franke, B., Gasch, A., Rodriguez, D., Chami, M., Khan, M.M., Rudolf, R., Bibby, J., Hanashima, A., Bogomolovas, J., Castelmur, E. von, Rigden, D.J., Uson, I., Labeit, S., Mayans, O., Franke, B., Gasch, A., Rodriguez, D., Chami, M., Khan, M.M., Rudolf, R., Bibby, J., Hanashima, A., Bogomolovas, J., Castelmur, E. von, Rigden, D.J., Uson, I., Labeit, S., and Mayans, O.

Abstract

Contains fulltext : 137461.pdf (publisher's version ) (Open Access), MuRF1 is an E3 ubiquitin ligase central to muscle catabolism. It belongs to the TRIM protein family characterized by a tripartite fold of RING, B-box and coiled-coil (CC) motifs, followed by variable C-terminal domains. The CC motif is hypothesized to be responsible for domain organization in the fold as well as for high-order assembly into functional entities. But data on CC from this family that can clarify the structural significance of this motif are scarce. We have characterized the helical region from MuRF1 and show that, contrary to expectations, its CC domain assembles unproductively, being the B2- and COS-boxes in the fold (respectively flanking the CC) that promote a native quaternary structure. In particular, the C-terminal COS-box seemingly forms an alpha-hairpin that packs against the CC, influencing its dimerization. This shows that a C-terminal variable domain can be tightly integrated within the conserved TRIM fold to modulate its structure and function. Furthermore, data from transfected muscle show that in MuRF1 the COS-box mediates the in vivo targeting of sarcoskeletal structures and points to the pharmacological relevance of the COS domain for treating MuRF1-mediated muscle atrophy.

Published

2014

4. Molecular basis for the fold organization and sarcomeric targeting of the muscle atrogin MuRF1

Author

Franke, B., Gasch, A., Rodriguez, D., Chami, M., Khan, M.M., Rudolf, R., Bibby, J., Hanashima, A., Bogomolovas, J., Castelmur, E. von, Rigden, D.J., Uson, I., Labeit, S., Mayans, O., Franke, B., Gasch, A., Rodriguez, D., Chami, M., Khan, M.M., Rudolf, R., Bibby, J., Hanashima, A., Bogomolovas, J., Castelmur, E. von, Rigden, D.J., Uson, I., Labeit, S., and Mayans, O.

Abstract

Contains fulltext : 137461.pdf (publisher's version ) (Open Access), MuRF1 is an E3 ubiquitin ligase central to muscle catabolism. It belongs to the TRIM protein family characterized by a tripartite fold of RING, B-box and coiled-coil (CC) motifs, followed by variable C-terminal domains. The CC motif is hypothesized to be responsible for domain organization in the fold as well as for high-order assembly into functional entities. But data on CC from this family that can clarify the structural significance of this motif are scarce. We have characterized the helical region from MuRF1 and show that, contrary to expectations, its CC domain assembles unproductively, being the B2- and COS-boxes in the fold (respectively flanking the CC) that promote a native quaternary structure. In particular, the C-terminal COS-box seemingly forms an alpha-hairpin that packs against the CC, influencing its dimerization. This shows that a C-terminal variable domain can be tightly integrated within the conserved TRIM fold to modulate its structure and function. Furthermore, data from transfected muscle show that in MuRF1 the COS-box mediates the in vivo targeting of sarcoskeletal structures and points to the pharmacological relevance of the COS domain for treating MuRF1-mediated muscle atrophy.

Published

2014

5. Identification of an N-terminal inhibitory extension as the primary mechanosensory regulator of twitchin kinase

Author

von Castelmur, E., Strumpfer, J., Franke, B., Bogomolovas, J., Barbieri, S., Qadota, H., Konarev, P.V., Svergun, D.I., Labeit, S., Benian, G.M., Schulten, K., Mayans, O., von Castelmur, E., Strumpfer, J., Franke, B., Bogomolovas, J., Barbieri, S., Qadota, H., Konarev, P.V., Svergun, D.I., Labeit, S., Benian, G.M., Schulten, K., and Mayans, O.

Abstract

Item does not contain fulltext, Titin-like kinases are an important class of cytoskeletal kinases that intervene in the response of muscle to mechanical stimulation, being central to myofibril homeostasis and development. These kinases exist in autoinhibited states and, allegedly, become activated during muscle activity by the elastic unfolding of a C-terminal regulatory segment (CRD). However, this mechano-activation model remains controversial. Here we explore the structural, catalytic, and tensile properties of the multidomain kinase region of Caenorhabditis elegans twitchin (Fn(31)-Nlinker-kinase-CRD-Ig(26)) using X-ray crystallography, small angle X-ray scattering, molecular dynamics simulations, and catalytic assays. This work uncovers the existence of an inhibitory segment that flanks the kinase N-terminally (N-linker) and that acts synergistically with the canonical CRD tail to silence catalysis. The N-linker region has high mechanical lability and acts as the primary stretch-sensor in twitchin kinase, while the CRD is poorly responsive to pulling forces. This poor response suggests that the CRD is not a generic mechanosensor in this kinase family. Instead, the CRD is shown here to be permissive to catalysis and might protect the kinase active site against mechanical damage. Thus, we put forward a regulatory model where kinase inhibition results from the combined action of both N- and C-terminal tails, but only the N-terminal extension undergoes mechanical removal, thereby affording partial activation. Further, we compare invertebrate and vertebrate titin-like kinases and identify variations in the regulatory segments that suggest a mechanical speciation of these kinase classes.

Published

2012

6. Identification of an N-terminal inhibitory extension as the primary mechanosensory regulator of twitchin kinase

Author

von Castelmur, E., Strumpfer, J., Franke, B., Bogomolovas, J., Barbieri, S., Qadota, H., Konarev, P.V., Svergun, D.I., Labeit, S., Benian, G.M., Schulten, K., Mayans, O., von Castelmur, E., Strumpfer, J., Franke, B., Bogomolovas, J., Barbieri, S., Qadota, H., Konarev, P.V., Svergun, D.I., Labeit, S., Benian, G.M., Schulten, K., and Mayans, O.

Abstract

Item does not contain fulltext, Titin-like kinases are an important class of cytoskeletal kinases that intervene in the response of muscle to mechanical stimulation, being central to myofibril homeostasis and development. These kinases exist in autoinhibited states and, allegedly, become activated during muscle activity by the elastic unfolding of a C-terminal regulatory segment (CRD). However, this mechano-activation model remains controversial. Here we explore the structural, catalytic, and tensile properties of the multidomain kinase region of Caenorhabditis elegans twitchin (Fn(31)-Nlinker-kinase-CRD-Ig(26)) using X-ray crystallography, small angle X-ray scattering, molecular dynamics simulations, and catalytic assays. This work uncovers the existence of an inhibitory segment that flanks the kinase N-terminally (N-linker) and that acts synergistically with the canonical CRD tail to silence catalysis. The N-linker region has high mechanical lability and acts as the primary stretch-sensor in twitchin kinase, while the CRD is poorly responsive to pulling forces. This poor response suggests that the CRD is not a generic mechanosensor in this kinase family. Instead, the CRD is shown here to be permissive to catalysis and might protect the kinase active site against mechanical damage. Thus, we put forward a regulatory model where kinase inhibition results from the combined action of both N- and C-terminal tails, but only the N-terminal extension undergoes mechanical removal, thereby affording partial activation. Further, we compare invertebrate and vertebrate titin-like kinases and identify variations in the regulatory segments that suggest a mechanical speciation of these kinase classes.

Published

2012

7. Identification of an N-terminal inhibitory extension as the primary mechanosensory regulator of twitchin kinase

Author

von Castelmur, E., Strumpfer, J., Franke, B., Bogomolovas, J., Barbieri, S., Qadota, H., Konarev, P.V., Svergun, D.I., Labeit, S., Benian, G.M., Schulten, K., Mayans, O., von Castelmur, E., Strumpfer, J., Franke, B., Bogomolovas, J., Barbieri, S., Qadota, H., Konarev, P.V., Svergun, D.I., Labeit, S., Benian, G.M., Schulten, K., and Mayans, O.

Abstract

Item does not contain fulltext, Titin-like kinases are an important class of cytoskeletal kinases that intervene in the response of muscle to mechanical stimulation, being central to myofibril homeostasis and development. These kinases exist in autoinhibited states and, allegedly, become activated during muscle activity by the elastic unfolding of a C-terminal regulatory segment (CRD). However, this mechano-activation model remains controversial. Here we explore the structural, catalytic, and tensile properties of the multidomain kinase region of Caenorhabditis elegans twitchin (Fn(31)-Nlinker-kinase-CRD-Ig(26)) using X-ray crystallography, small angle X-ray scattering, molecular dynamics simulations, and catalytic assays. This work uncovers the existence of an inhibitory segment that flanks the kinase N-terminally (N-linker) and that acts synergistically with the canonical CRD tail to silence catalysis. The N-linker region has high mechanical lability and acts as the primary stretch-sensor in twitchin kinase, while the CRD is poorly responsive to pulling forces. This poor response suggests that the CRD is not a generic mechanosensor in this kinase family. Instead, the CRD is shown here to be permissive to catalysis and might protect the kinase active site against mechanical damage. Thus, we put forward a regulatory model where kinase inhibition results from the combined action of both N- and C-terminal tails, but only the N-terminal extension undergoes mechanical removal, thereby affording partial activation. Further, we compare invertebrate and vertebrate titin-like kinases and identify variations in the regulatory segments that suggest a mechanical speciation of these kinase classes.

Published

2012