Desmin: molecular interactions and putative functions of the muscle intermediate filament protein

Costa, Márcio Henrique Sá Netto; Escaleira, Roberta C.; Cataldo, Anne M.; Oliveira, Francisco Meirelles Bastos de; Mermelstein, Cláudia

doi:10.1590/s0100-879x2004001200007

Cited by 121 publications

(96 citation statements)

References 62 publications

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“…Along with the molecular link between R120G-and G6PD-mediated GSH production, HSPB1 was upregulated at the transcriptional and translational levels. Mitochondria, by far the most vital organelle for energy production and redox adaptation (56,120), are organized spatially at the A and I bands of the sarcomere, thereby providing proximity of ATP production to the proximal contractile apparatus (28,84). Independently, Maloyan and coworkers demonstrated severely compromised mitochondrial function and disrupted mitochondrial organization of mouse R120G compared with HSPB5 WT littermates, suggesting that the mutant R120G expression might disrupt ROS production during progressive heart failure (80).…”

Section: Brewer Et Almentioning

confidence: 99%

Reductive Stress Linked to Small HSPs, G6PD, and Nrf2 Pathways in Heart Disease

Brewer

Mustafi

Murray

et al. 2013

Antioxidants & Redox Signaling

109

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Significance: Aerobic organisms must exist between the dueling biological metabolic processes for energy and respiration and the obligatory generation of reactive oxygen species (ROS) whose deleterious consequences can reduce survival. Wide fluctuations in harmful ROS generation are circumvented by endogenous countermeasures (i.e., enzymatic and nonenzymatic antioxidants systems) whose capacity decline with aging and are enhanced by disease states. Recent Advances: Substantial efforts on the cellular and molecular underpinnings of oxidative stress has been complemented recently by the discovery that reductive stress similarly predisposes to inheritable cardiomyopathy, firmly establishing that the biological extremes of the redox spectrum play essential roles in disease pathogenesis. Critical Issues: Because antioxidants by nutritional or pharmacological supplement to prevent or mitigate disease states have been largely disappointing, we hypothesize that lack of efficacy of antioxidants might be related to adverse outcomes in responders at the reductive end of the redox spectrum. As emerging concepts, such as reductive, as opposed, oxidative stress are further explored, there is an urgent and critical gap for biochemical phenotyping to guide the targeted clinical applications of therapeutic interventions. Future Directions: New approaches are vitally needed for characterizing redox states with the long-term goal to noninvasively assess distinct clinical states (e.g., presymptomatic, end-stage) with the diagnostic accuracy to guide personalized medicine.

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Section: Brewer Et Almentioning

confidence: 99%

Reductive Stress Linked to Small HSPs, G6PD, and Nrf2 Pathways in Heart Disease

Brewer

Mustafi

Murray

et al. 2013

Antioxidants & Redox Signaling

109

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“…23 and is present in higher amounts during embryogenesis. This suggests that there may be some interaction between the two in determining muscle cell differentiation 13 . This also suggests that 10(67%) of the samples were obtained from relatively advanced sarcoma lesions.…”

Section: Discussionmentioning

confidence: 99%

“…It is a 52 kD protein that is a subunit of intermediate filaments in skeletal muscle tissue, smooth muscle tissue, and cardiac muscle tissue. Its presence in vascular smooth muscle is variable 13 . The muscle cell matures only if desmin is present.…”

Section: Introductionmentioning

confidence: 99%

“…Vimentin is present in higher amounts during embryogenesis while desmin is present in higher amounts after differentiation. This suggests that there may be some interaction between the two in determining muscle cell differentiation 13 . Desmin is detected in rhabdomyosarcoma of all subtypes, benign smooth muscle tumours, benign skeletal muscle tumours and leiomyosarcoma (50%) 14 .…”

Section: Introductionmentioning

confidence: 99%

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Immunohistochemistry and antigenic expression of four proteins in Kaposi Sarcoma

Egbujo

Adisa

Egbujo

et al. 2013

Int J of Biomed & Adv Res

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Introduction: Kaposi sarcoma poses problems in histological diagnosis because of its broad morphologic variants and similarity to many vasoproliferative lesions. Establishing diagnosis on the basis of tumour marker alone (especially a single result) is fraught with associated pitfalls because of the problem of non- specificity.

Method: Fifteen(15) Kaposi sarcoma biopsies from seven(7) men and eight(8) women were used to find out the gene expression of vimentin, desmin, smooth muscle actin(SMA), S-100 and neuron specific enolase(NSE) in Kaposi sarcoma, Haematoxylin and eosin(H&E) method was used to confirm the diagnosis of Kaposi sarcoma in archival processed biopsies. Subsequently, Immunohistochemistry(IHC) was carried out to find out the expression of the antibodies listed.

Results: Vimentin and SMA were found to be most reactive. Neuron specific enolase were mildly reactive while the rest were non-reactive.

Conclusion: Only vimentin and SMA offer significant reactivity in the diagnosis of Kaposi sarcoma and are useful in undifferentiated neoplasms.

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“…Cells were grown in 2 mL of medium (minimum essential medium with the addition of 10% horse serum, 0.05% chick embryo extract, 1% L-glutamine and 1% penicillin-streptomycin) under humidified 5% CO 2 atmosphere at 37°C. The percentage of myoblasts in these cell cultures was calculated by the double labeling of 24-h cultures with both DAPI (nuclear staining) and anti-desmin antibodies (applied herein to define a muscle-specific marker) [4] and subsequently counting the number of desmin-positive cells out of the total number of cells in the field. A rabbit polyclonal antibody against desmin (Sigma) was used.…”

Section: Primary Chick Myogenic Cell Culturesmentioning

confidence: 99%

Knockdown of Lmo7 inhibits chick myogenesis

et al. 2016

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Edited by Dietmar MansteinThe multifunctional protein Lmo7 has been implicated in some aspects of myogenesis in mammals. Here we studied the distribution and expression of Lmo7 and the effects of Lmo7 knockdown in primary cultures of chick skeletal muscle cells. Lmo7 was localized within the nuclei of myoblasts and at the perinuclear region of myotubes. Knockdown of Lmo7 using siRNA specific to chick reduces the number and width of myotubes and the number of MyoD positive-myoblasts. Both Wnt3a enriched medium and Bio, activators of the Wnt/beta-catenin pathway, could rescue the effects of the Lmo7 knockdown suggesting a crosstalk between the Wnt/beta-catenin and Lmo7-mediated signaling pathways. Our data shows a role of Lmo7 during the initial events of chick skeletal myogenesis, particularly in myoblast survival.

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Desmin: molecular interactions and putative functions of the muscle intermediate filament protein

Cited by 121 publications

References 62 publications

Reductive Stress Linked to Small HSPs, G6PD, and Nrf2 Pathways in Heart Disease

Reductive Stress Linked to Small HSPs, G6PD, and Nrf2 Pathways in Heart Disease

Immunohistochemistry and antigenic expression of four proteins in Kaposi Sarcoma

Knockdown of Lmo7 inhibits chick myogenesis

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