Margaux Kuijlaars scite author profile

Margaux Kuijlaars

4Publications

7Citation Statements Received

132Citation Statements Given

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130

Affiliations

University of Glasgow

Publications

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Autoimmune polyendocrine syndrome in a standard poodle with concurrent non‐endocrine immune‐mediated diseases

Kuijlaars

Yool

Ridyard

2021

Vet Record Case Reports

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A 6-year-old female neutered standard poodle was referred with a 4-week history of rapidly progressive weight loss, muscle atrophy, hyporexia, hind limb weakness and lethargy. In the preceding 3-month period, the dog had been diagnosed with both keratoconjunctivitis sicca (KCS) and hypoadrenocorticism. Clinical deterioration had occurred despite treatment for hypoadrenocorticism. Following referral, the dog was diagnosed with concurrent hypothyroidism, exocrine pancreatic insufficiency (EPI) and suspected generalised myositis. Treatment with hormone replacement therapy, pancreatic enzyme supplementation and immunosuppressive doses of prednisolone and mycophenolate resulted in marked clinical improvement. This case describes a rapidly progressive, presumed autoimmune, polyglandular endocrinopathy in a dog with concurrent non-endocrine autoimmune diseases.

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Development and progression of proteinuria in dogs treated with masitinib for neoplasia: 28 cases (2010‐2019)

Kuijlaars

Helm

McBrearty

2021

J of Small Animal Practice

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Objectives To describe the incidence, severity and progression of proteinuria over the first 6 months of masitinib treatment in tumour‐bearing dogs without pre‐existing proteinuria. To describe the effect of treatment on urine protein:creatinine and renal parameters in patients with pre‐existing proteinuria. Materials and Methods Records were reviewed from patients receiving masitinib for neoplasms between June 1, 2010, and May 5, 2019. Patients without pre‐treatment and at least one urine protein:creatinine after ≥7 days treatment were excluded. Signalment, tumours and concurrent diseases, treatments, haematology, biochemistry and urinalysis results before, during and after treatment for up to 202 days were collected. Patient visits were grouped into six timepoints for analysis. Results Twenty‐eight dogs were included. Eighteen percent of dogs non‐proteinuric at baseline (four of 22) developed proteinuria during treatment, all within 1 month of treatment initiation. One dog developed hypoalbuminaemia, none developed oedema or ascites, azotaemia or were euthanased/died due to proteinuria. Masitinib was immediately discontinued in both dogs in which urine protein:creatinine greater than 2.0 was detected and in both, proteinuria improved. Six dogs with pre‐treatment proteinuria were treated with masitinib, significant worsening of proteinuria did not occur. Neither azotaemia nor severe hypoalbuminaemia occurred. Clinical Significance Proteinuria, when it occurs, tends to develop within 1 month of masitinib commencement and may progress rapidly. Weekly proteinuria monitoring should be considered for the first month and a urine protein:creatinine greater than 0.5 should prompt reassessment within 1 week. Masitinib treatment can be considered in patients with pre‐treatment proteinuria and does not inevitably cause worsening of proteinuria.

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The occurrence of proteinuria in dogs treated with masitinib

Kuijlaars¹,

McBrearty²,

Helm³

2017

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RESULTSMedian age at presentation was 7 years, with 8 males and 7 females. No breed predisposition was highlighted. 9/15 were multi-centric and 4/15 intestinal/mesenteric lymphoma. WHO stage III, IV and IV were reported in 8/15, 5/15 and 2/15 dogs respectively. 6 dogs were sub-stage a and 9 sub-stage b. B-cell and T-cell lymphomas were identified in 2/5 and 3/5 dogs respectively. GPS of 0, 1 and 2 were documented in 3/15, 8/15 and 4/15 dogs. MST for dogs with a mGPS of 0 was 277 days (range 210-1672), mGPS of 1, 164 days (range 76-1491) and mGPS of 2, 7 days (1-64 days). Kaplan-Meier analysis revealed dogs with mGPS of 2 had significantly shorter MSTs than dogs with mGPS 0 or 1. Dogs with an mGPS of 0 had significantly longer MST than dogs with GPS of 1 or 2.

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Evaluation of a point-of-care coagulation analyser in dogs by comparison with central diagnostic laboratory methods

Kuijlaars¹,

Ramsey²

2017

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