Your search

Reset search

In authors or contributors

"Herbst, K. L."

Topic

Review

Results 5 resources

Abstracts

Herbst, K. L. (2020). Insights on the Pathophysiology, Diagnosis and Treatment of Lipedema. Today’s Wound Clinic. https://www.todayswoundclinic.com/articles/insights-pathophysiology-diagnosis-and-treatment-lipedema

Lipedema can cause chronic pain and increases patients’ risk for conditions such as lymphedema and venous disease. This author explores how lipedema affects the body, why its effects are disproportionate in the lower body, and how to diagnose and manage the condition.

View for free on www.todayswoundclinic.com
Beltran, K., & Herbst, K. L. (2017). Differentiating lipedema and Dercum’s disease. International Journal of Obesity (2005), 41(2), 240–245. https://doi.org/10.1038/ijo.2016.205

BACKGROUND: People with lipedema or Dercum's disease (DD) can have a similar distribution of excess painful nodular subcutaneous adipose tissue (SAT), making them difficult to differentiate. METHODS: Case series of 94 patients with DD, 160 with lipedema and 18 with both diagnoses (Lip+DD) from a single clinic in an academic medical center to improve identification and differentiation of these disorders by comparison of clinical findings, prevalence of type 2 diabetes (DM2), hypermobility by the Beighton score and assessment of a marker of inflammation, Total complement activity (CH50). RESULTS: Differences between groups were by Student's t-test with α of 0.05. The Lipedema Group had significantly greater weight, body mass index (BMI), gynoid distributed nodular SAT and fibrotic and heavy tissue than the DD Group. Hypermobility was significantly higher in the Lipedema (58±0.5%) than DD Group (23±0.4%; P<0.0001). DM2 was significantly greater in the DD (16±0.2%; P=0.0007) than the Lipedema Group (6±0.2%). Average pain by an analog scale was significantly higher in the DD (6±2.5%) than the Lipedema Group (4±2.1%; P<0.0001). Fatigue and swelling were common in both groups. Easy bruising was more common in the Lipedema Group, whereas abdominal pain, shortness of breath, fibromyalgia, migraines and lipomas were more prevalent in the DD Group. The percentage of patients with elevated CH50 was significantly positive in both groups. CONCLUSIONS: The significantly lower prevalence of DM2 in people with lipedema compared with DD may be due to the greater amount of gynoid fat known to be protective against metabolic disorders. The high percentage of hypermobility in lipedema patients indicates that it may be a comorbid condition. The location of fat, high average daily pain, presence of lipomas and comorbid painful disorders in DD patients may help differentiate from lipedema.

View on www.nature.com
Bonetti, G., Dhuli, K., Kaftalli, J., Micheletti, C., Donato, K., Michelini, S., Ricci, M., Cestari, M., Fulcheri, E., Michelini, S., Herbst, K. L., Marceddu, G., & Bertelli, M. (2023). Characterization of somatic mutations in the pathogenesis of lipedema. La Clinica Terapeutica, 174(Suppl 2(6)), 249–255. https://doi.org/10.7417/CT.2023.2495

BACKGROUND: Lipedema, a complex and enigmatic adipose tissue disorder, remains poorly understood despite its significant impact on the patients' quality of life. Genetic investigations have uncovered potential contributors to its pathogenesis, including somatic mutations, which are nonheritable genetic alterations that can play a pivotal role in the development of this disease. AIM: This review aims to elucidate the role of somatic mutations in the etiology of lipedema by examining their implications in adipose tissue biology, inflammation, and metabolic dysfunction. RESULTS: Studies focusing on leukocyte clones, genetic alterations like TET2 and DNMT3A, and the intricate interplay between adipose tissue and other organs have shed light on the underlying mechanisms driving lipedema. From the study of the scientific literature, mutations to genes correlated to three main pathways could be involved in the somatic development of lipedema: genes related to mitochondrial activity, genes related to localized disorders of subcutaneous adipose tissue, and genes of leukocyte clones. CONCLUSIONS: The insights gained from these diverse studies converge to highlight the complex genetic underpinnings of lipedema and offer potential avenues for therapeutic interventions targeting somatic mutations to alleviate the burden of this condition on affected individuals.

View for free on clinicaterapeutica.it
Paolacci, S., Precone, V., Acquaviva, F., Chiurazzi, P., Fulcheri, E., Pinelli, M., Buffelli, F., Michelini, S., Herbst, K. L., Unfer, V., Bertelli, M., & GeneOb Project. (2019). Genetics of lipedema: new perspectives on genetic research and molecular diagnoses. European Review for Medical and Pharmacological Sciences, 23(13), 5581–5594. https://doi.org/10.26355/eurrev_201907_18292

OBJECTIVE: The aim of this qualitative review is to provide an update on the current understanding of the genetic determinants of lipedema and to develop a genetic test to differentiate lipedema from other diagnoses. MATERIALS AND METHODS: An electronic search was conducted in MEDLINE, PubMed, and Scopus for articles published in English up to March 2019. Lipedema and similar disorders included in the differential diagnosis of lipedema were searched in the clinical synopsis section of OMIM, in GeneCards, Orphanet, and MalaCards. RESULTS: The search identified several genetic factors related to the onset of lipedema and highlighted the utility of developing genetic diagnostic testing to help differentiate lipedema from other diagnoses. CONCLUSIONS: No genetic tests or guidelines for molecular diagnosis of lipedema are currently available, despite the fact that genetic testing is fundamental for the differential diagnosis of lipedema against Mendelian genetic obesity, primary lymphedema, and lipodystrophies.

View for free on www.europeanreview.org
Kiani, A. K., Mor, M., Bernini, A., Fulcheri, E., Michelini, S., Herbst, K. L., Buffelli, F., Belgrado, J.-P., Kaftalli, J., Stuppia, L., Dautaj, A., Dhuli, K., Guda, T., Manara, E., Maltese, P. E., Michelini, S., Chiurazzi, P., Paolacci, S., Ceccarini, M. R., … Bertelli, M. (2021). Steroid-converting enzymes in human adipose tissues and fat deposition with a focus on AKR1C enzymes. European Review for Medical and Pharmacological Sciences, 25(1 Suppl), 23–32. https://doi.org/10.26355/eurrev_202112_27330

Adipocytes express various enzymes, such as aldo-keto reductases (AKR1C), 11β-hydroxysteroid dehydrogenase (11β-HSD), aromatase, 5α-reductases, 3β-HSD, and 17β-HSDs involved in steroid hormone metabolism in adipose tissues. Increased activity of AKR1C enzymes and their expression in mature adipocytes might indicate the association of these enzymes with subcutaneous adipose tissue deposition. The inactivation of androgens by AKR1C enzymes increases adipogenesis and fat mass, particularly subcutaneous fat. AKR1C also causes reduction of estrone, a weak estrogen, to produce 17β-estradiol, a potent estrogen and, in addition, it plays a role in progesterone metabolism. Functional impairments of adipose tissue and imbalance of steroid biosynthesis could lead to metabolic disturbances. In this review, we will focus on the enzymes involved in steroid metabolism and fat tissue deposition.

View for free on www.europeanreview.org

Custom feed

Last update from database: 4/2/25, 8:13 AM (UTC)

Your search

Results 5 resources

Explore

Topic

Resource type

Publication year

Publication

Online resource