Your search keyword '"Brenner, Rolf E."' showing total 6 results

1. Interleukin-1β and cathepsin D modulate formation of the terminal complement complex in cultured human disc tissue.

Author

Teixeira, Graciosa Q., Yong, Zhiyao, Kuhn, Amelie, Riegger, Jana, Goncalves, Raquel M., Ruf, Michael, Mauer, Uwe M., Huber-Lang, Markus, Ignatius, Anita, Brenner, Rolf E., and Neidlinger-Wilke, Cornelia

Subjects

ADOLESCENT idiopathic scoliosis, TISSUE culture, COMPLEMENT activation, NUCLEUS pulposus, CD55 antigen

Abstract

Purpose: Formation of terminal complement complex (TCC), a downstream complement system activation product inducing inflammatory processes and cell lysis, has been identified in degenerated discs. However, it remains unclear which molecular factors regulate complement activation during disc degeneration (DD). This study investigated a possible involvement of the pro-inflammatory cytokine interleukin-1β (IL-1β) and the lysosomal protease cathepsin D (CTSD). Methods: Disc biopsies were collected from patients suffering from DD (n = 43) and adolescent idiopathic scoliosis (AIS, n = 13). Standardized tissue punches and isolated cells from nucleus pulposus (NP), annulus fibrosus (AF) and endplate (EP) were stimulated with 5% human serum (HS) alone or in combination with IL-1β, CTSD or zymosan. TCC formation and modulation by the complement regulatory proteins CD46, CD55 and CD59 were analysed. Results: In DD tissue cultures, IL-1β stimulation decreased the percentage of TCC + cells in AF and EP (P < 0.05), whereas CTSD stimulation significantly increased TCC deposition in NP (P < 0.01) and zymosan in EP (P < 0.05). Overall, the expression of CD46, CD55 and CD59 significantly increased in all isolated cells during culture (P < 0.05). Moreover, cellular TCC deposition was HS concentration dependent but unaffected by IL-1β, CTSD or zymosan. Conclusion: These results suggest a functional relevance of IL-1β and CTSD in modulating TCC formation in DD, with differences between tissue regions. Although strong TCC deposition may represent a degeneration-associated event, IL-1β may inhibit it. In contrast, TCC formation was shown to be triggered by CTSD, indicating a multifunctional involvement in disc pathophysiology. [ABSTRACT FROM AUTHOR]

Published

2021

2. Terminal complement complex formation is associated with intervertebral disc degeneration.

Author

Teixeira, Graciosa Q., Yong, Zhiyao, Goncalves, Raquel M., Kuhn, Amelie, Riegger, Jana, Brisby, Helena, Barreto Henriksson, Helena, Ruf, Michael, Nerlich, Andreas, Mauer, Uwe M., Ignatius, Anita, Brenner, Rolf E., and Neidlinger-Wilke, Cornelia

Subjects

ADOLESCENT idiopathic scoliosis, INTERVERTEBRAL disk, ECULIZUMAB, SOCIAL degeneration, T helper cells, NUCLEUS pulposus, LYSIS

Abstract

Purpose: The complement system is a crucial part of innate immunity. Recent work demonstrated an unexpected contribution to tissue homeostasis and degeneration. This study investigated for the first time, in human disc tissues, the deposition profile of the complement activation product terminal complement complex (TCC), an inflammatory trigger and inducer of cell lysis, and its inhibitor CD59, and their correlation with the degree of disc degeneration (DD). Methods: Disc biopsies were collected from patients diagnosed with DD (n = 39, age 63 ± 12) and adolescent idiopathic scoliosis (AIS, n = 10, age 17 ± 4) and compared with discs from healthy Young (n = 11, age 7 ± 7) and Elder (n = 10, age 65 ± 15) donors. Immunohistochemical detection of TCC and CD59 in nucleus pulposus (NP), annulus fibrosus (AF) and endplate (EP) was correlated with age, Pfirrmann grade and Modic changes. Results: Higher percentage of TCC+ cells was detected in the NP and EP of DD compared to Elder (P < 0.05), and in the EP of Young versus Elder (P < 0.001). In DD, TCC deposition was positively correlated with Pfirrmann grade, but not with Modic changes, whereas for Young donors, a negative correlation was found with age, indicating TCC's involvement not only in DD, but also in early stages of skeletal development. Higher CD59 positivity was found in AIS and DD groups compared to Young (P < 0.05), and it was negatively correlated with the age of the patients. Conclusion: TCC deposition positively correlated with the degree of disc degeneration. A functional relevance of TCC may exist in DD, representing a potential target for new therapeutics. [ABSTRACT FROM AUTHOR]

Published

2021

3. Role of Complement on Broken Surfaces After Trauma.

Author

Huber-Lang, Markus, Ignatius, Anita, and Brenner, Rolf E.

Published

2015

4. Classic, atypically severe and neonatal Marfan syndrome: twelve mutations and genotype–phenotype correlations in FBN1 exons 24–40.

Author

Tiecke, Frank, Katzke, Stefanie, Booms, Patrick, Robinson, Peter N, Neumann, Luitgard, Godfrey, Maurice, Mathews, Kurt R, Scheuner, Maren, Hinkel, Georg Klaus, Brenner, Rolf E, Hövels-Gürich, Hedwig H, Hagemeier, Christian, Fuchs, Josefine, Skovby, Flemming, and Rosenberg, Thomas

Subjects

MARFAN syndrome, GENETIC mutation, EXONS (Genetics)

Abstract

Mutations in the gene for fibrillin-1 (FBN1) cause Marfan syndrome, an autosomal dominant disorder of connective tissue with prominent manifestations in the skeletal, ocular, and cardiovascular system. There is a remarkable degree of clinical variability both within and between families with Marfan syndrome as well as in individuals with related disorders of connective tissue caused by FBN1 mutations and collectively termed type-1 fibrillinopathies. The so-called neonatal region in FBN1 exons 24-32 comprises one of the few generally accepted genotype-phenotype correlations described to date. In this work, we report 12 FBN1 mutations identified by temperature-gradient gel electrophoresis screening of exons 24-40 in 127 individuals with Marfan syndrome or related disorders. The data reported here, together with other published reports, document a significant clustering of mutations in exons 24-32. Although all reported mutations associated with neonatal Marfan syndrome and the majority of point mutations associated with atypically severe presentations have been found in exons 24-32, mutations associated with classic Marfan syndrome occur in this region as well. It is not possible to predict whether a given mutation in exons 24-32 will be associated with classic, atypically severe, or neonatal Marfan syndrome. [ABSTRACT FROM AUTHOR]

Published

2001

5. Five years' trajectories of functionality and pain in patients after hip or knee replacement and association with long-term patient survival.

Author

Repky, Stefan, Büchele, Gisela, Günther, Klaus-Peter, Huch, Klaus, Brenner, Hermann, Stürmer, Til, Beyersmann, Jan, Brenner, Rolf E., and Rothenbacher, Dietrich

Subjects

OSTEOARTHRITIS, ARTHROPLASTY, PAIN, MORTALITY, PATIENTS

Abstract

To describe the 5 years' trajectories in functionality and pain of patients with hip or knee osteoarthritis and arthroplasty and analyze the association of these with long-term patients survival. Patients with OA receiving total hip or knee arthroplasty were recruited and completed two sets of standardized questionnaires for functionality and pain 6, 12, and 60 months postoperatively. Multivariate mixed models were conducted to assess trajectories over time and the resulting improvement per month during the last time period was included in a landmark-model to estimate adjusted hazard ratios for mortality. In total 809 patients with joint replacement were included (mean age 65.0 years, 62.2% female), 407 patients died (median follow-up 18.4 years). Both instruments of functionality and pain showed extensive improvement during the first 6 months. Baseline and change in functionality (both p < 0.001) and pain (p = 0.02) during the first 6 months were associated with mortality. Better values in functionality corresponded with improved survival whereas the association with the pain scores was inverse. In patients with hip and knee OA, an explicit improvement in function is seen within the first 6 months after arthroplasty. In addition, especially the functionality scores at baseline as well as their improvement showed an association with long-term patient survival. [ABSTRACT FROM AUTHOR]

Published

2020

6. Evidence of necroptosis in osteoarthritic disease: investigation of blunt mechanical impact as possible trigger in regulated necrosis.

Author

Riegger, Jana and Brenner, Rolf E.

Published

2019