Your search keyword '"Fenn JS"' showing total 3 results

1. Biochemical assessment of adequate levothyroxine replacement in primary hypothyroidism differs with different TSH assays: potential clinical implications.

Author

Kalaria TR, Sanders A, Ford C, Buch H, Fenn JS, Ashby HL, Mohammed P, and Gama RM

Subjects

Female, Humans, Laboratories, Middle Aged, Reference Values, Thyrotropin, Hypothyroidism diagnosis, Hypothyroidism drug therapy, Thyroxine therapeutic use

Abstract

Aim: Thyroid stimulating hormone (TSH) assays provided by Abbott Laboratories and Roche Diagnostics are used by approximately 75% of laboratories in the UK. We assessed the potential impact of Abbott and Roche TSH assay differences on the biochemical assessment of levothyroxine replacement in primary hypothyroidism., Method: Samples from 100 consecutive primary care patients (83 women, median age 64 years, IQR 51-73 years) with primary hypothyroidism on adequate levothyroxine based on an Abbott Architect TSH in the reference range were analysed for TSH on Roche cobas within 24 hours. The Abbott and Roche TSH results were compared. Over 1 year, TSH results from patients in primary care from the laboratories with Abbott and Roche methods were compared., Results: The median (IQR) Roche TSH (2.5 (1.3-3.6) mIU/L) was 30%±10% higher (p<0.001) than Abbott TSH (1.9 (1.1-2.6) mIU/L). Although all Abbott TSH results were in the Abbott specific reference range, 14 patients (14%) had Roche TSH results above the Roche specific reference range. In the 1 year gather, Roche TSH (1.9 (1.3-2.9) mIU/L, n=103 932) results were higher (p<0.001) than Abbott TSH (1.5 (1.0-2.2) mIU/L, n=1 10 544) results. The TSH results were above their assay-specific upper reference limit in 10.7% of Roche results and 4.2% of Abbott results., Conclusion: Biochemical assessment of levothyroxine replacement may be dependent on the type of TSH assay. Laboratorians and clinicians should be aware that the lack of harmonisation between TSH methods and their assay-specific reference ranges may potentially lead to different patient management decisions. We suggest lot verification in laboratories should include processes to identify cumulative drift in assay performance., Competing Interests: Competing interests: None declared., (© Author(s) (or their employer(s)) 2022. No commercial re-use. See rights and permissions. Published by BMJ.)

Published

2022

2. Hypophosphatasia.

Author

Fenn JS, Lorde N, Ward JM, and Borovickova I

Subjects

Alkaline Phosphatase blood, Alkaline Phosphatase genetics, Alkaline Phosphatase therapeutic use, Calcium, Dietary adverse effects, Calcium-Regulating Hormones and Agents therapeutic use, Enzyme Replacement Therapy, Genetic Predisposition to Disease, Humans, Hypophosphatasia epidemiology, Hypophosphatasia genetics, Hypophosphatasia therapy, Immunoglobulin G therapeutic use, Mutation, Phenotype, Prognosis, Recombinant Fusion Proteins therapeutic use, Tooth Demineralization epidemiology, Tooth Demineralization genetics, Tooth Demineralization physiopathology, Tooth Demineralization therapy, Hypophosphatasia physiopathology, Odontogenesis genetics, Osteogenesis genetics, Tooth Demineralization congenital

Abstract

Hypophosphatasia (HPP) is a group of inherited disorders characterised by the impaired mineralisation of bones and/or teeth and low serum alkaline phosphatase (ALP) activity. It is caused by a mutation in the ALPL gene encoding the tissue-non-specific isoenzyme of ALP (TNSALP) resulting in a loss of function. The disease is highly heterogenous in its clinical expression ranging from stillbirth without mineralised bone to the mild form of late adult onset with symptoms and signs such as musculoskeletal pain, arthropathy, lower-extremity fractures, premature loss of teeth or an incidental finding of reduced serum ALP activity. A classification based on the age at diagnosis and the presence or absence of bone symptoms was historically used: perinatal, prenatal benign, infantile, childhood, adult and odontohypophosphatasia. These subtypes are known to have overlapping signs and complications. Three forms of HPP distinguishable by their genetic characteristics have been described: severe, moderate and mild. Severe forms of HPP (perinatal and infantile severe) are recessively inherited, whereas moderate HPP may be dominantly or recessively inherited. The biochemical hallmark of HPP is persistently low serum ALP for age and increase in natural substrates of TNSALP, pyridoxal 5'-phosphate and phosphoethanolamine supported by radiological findings. The diagnosis is confirmed by ALPL sequencing. A multidisciplinary team of experts is essential for the effective management. Calcium restriction is recommended in infants/children to manage hypercalcaemia. A targeted enzyme replacement therapy for HPP has become available and correct diagnosis is crucial to allow early treatment., Competing Interests: Competing interests: None declared., (© Author(s) (or their employer(s)) 2021. No commercial re-use. See rights and permissions. Published by BMJ.)

Published

2021

3. Structural Basis of Glycerophosphodiester Recognition by the Mycobacterium tuberculosis Substrate-Binding Protein UgpB.

Author

Fenn JS, Nepravishta R, Guy CS, Harrison J, Angulo J, Cameron AD, and Fullam E

Subjects

ATP-Binding Cassette Transporters chemistry, Bacterial Proteins chemistry, Binding Sites, Carrier Proteins chemistry, Carrier Proteins metabolism, Escherichia coli chemistry, Escherichia coli Proteins chemistry, Escherichia coli Proteins metabolism, Protein Binding, Protein Domains, Substrate Specificity, ATP-Binding Cassette Transporters metabolism, Bacterial Proteins metabolism, Glycerylphosphorylcholine metabolism, Mycobacterium tuberculosis chemistry

Abstract

Mycobacterium tuberculosis ( Mtb ) is the causative agent of tuberculosis (TB) and has evolved an incredible ability to survive latently within the human host for decades. The Mtb pathogen encodes for a low number of ATP-binding cassette (ABC) importers for the acquisition of carbohydrates that may reflect the nutrient poor environment within the host macrophages. Mtb UgpB (Rv2833c) is the substrate binding domain of the UgpABCE transporter that recognizes glycerophosphocholine (GPC), indicating that this transporter has a role in recycling glycerophospholipid metabolites. By using a combination of saturation transfer difference (STD) NMR and X-ray crystallography, we report the structural analysis of Mtb UgpB complexed with GPC and have identified that Mtb UgpB not only recognizes GPC but is also promiscuous for a broad range of glycerophosphodiesters. Complementary biochemical analyses and site-directed mutagenesis precisely define the molecular basis and specificity of glycerophosphodiester recognition. Our results provide critical insights into the structural and functional role of the Mtb UgpB transporter and reveal that the specificity of this ABC-transporter is not limited to GPC, therefore optimizing the ability of Mtb to scavenge scarce nutrients and essential glycerophospholipid metabolites via a single transporter during intracellular infection.

Published

2019