Marlies de Graaf scite author profile

The selective activation of a relatively non-toxic prodrug by an enzyme present only in the tumour should enhance the drug concentration at the tumour site and result in a better anti-tumour effect and a reduction in systemic toxicity as compared to conventional chemotherapy. beta-Glucuronidase is such an enzyme. It is normally expressed in the lysosomes of cells. In larger tumours, however, high levels of the enzyme are present in necrotic areas. Several glucuronide prodrugs have been synthesised that can be activated by beta-glucuronidase. They are relatively non-toxic due to their hydrophilic nature, which prevents them from entering cells and thus from contact with lysosomal beta-glucuronidase. The main problem of glucuronide prodrugs for clinical use is their fast renal clearance. Special attention should be paid to the development of new less hydrophilic prodrugs with slower clearance, as this would result in a prolonged exposure to beta-glucuronidase at the site of the tumour and a reduction of the amount of prodrug needed. A number of interesting anthracyclin-based glucuronide prodrugs have been synthesised and have shown favourable therapeutic effects compared to treatment with the parent drug. The tumoural levels of beta-glucuronidase can even be enhanced by two-step approaches, in which exogenous enzyme is targeted to the tumour by an antibody (ADEPT) or by the gene encoding the enzyme in transduced tumour cells (GDEPT). The ADEPT and GDEPT approaches in combination with glucuronide prodrugs have shown enhanced efficacy in experimental tumour models. Further improvement of ADEPT and GDEPT is warranted to optimise the tumour uptake and retention of antibody-enzyme fusion proteins and the efficiency and safety of current gene delivery methods. In conclusion, it is clear that glucuronide prodrugs hold promise for future use in the treatment of cancer in patients as monotherapy. Enhancement of the therapeutic effects of glucuronide prodrugs, also in patients with small tumour lesions, may possibly be achieved by techniques that target beta-glucuronidase specifically to the site of the tumour.

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Treatment of infantile haemangiomas with atenolol: Comparison with a historical propranolol group

Graaf

Raphaël

Breugem

et al. 2013

Journal of Plastic, Reconstructive & Aesthetic Surgery

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Hypoglycemia as a Result of Propranolol During Treatment of Infantile Hemangioma: A Case Report

Breur

Graaf

Breugem

et al. 2011

Pediatric Dermatology

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Propranolol is a new and promising treatment for hemangiomas of infancy. We report of a patient in whom steroid maintenance therapy is successfully tapered after introduction of propranolol. This patient, however, developed symptomatic hypoglycemic events presumably because of a concurrent deficiency of epinephrine and cortisol as a direct result of both beta-blockage by propranolol and adrenal insufficiency as a result of prednisone use. Extreme care should be taken in patients treated with both propranolol and prednisone as they are at increased risk of hypoglycemia.

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Atenolol: A promising alternative to propranolol for the treatment of hemangiomas

Raphaël

Graaf

Breugem

et al. 2011

Journal of the American Academy of Dermatology

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Ocular surface disease is common in moderate‐to‐severe atopic dermatitis patients

Achten

Bakker

Luijk

et al. 2022

Clin Experimental Allergy

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Marlies de Graaf

Adverse effects of propranolol when used in the treatment of hemangiomas: A case series of 28 infants

Activation of cardiac and smooth muscle-specific genes in primary human cells after forced expression of human myocardin

Long-term follow-up and treatment outcomes of conjunctivitis during dupilumab treatment in patients with moderate-to-severe atopic dermatitis

Beta-Glucuronidase-Mediated Drug Release

Treatment of infantile haemangiomas with atenolol: Comparison with a historical propranolol group

Hypoglycemia as a Result of Propranolol During Treatment of Infantile Hemangioma: A Case Report

Atenolol: A promising alternative to propranolol for the treatment of hemangiomas

Ocular surface disease is common in moderate‐to‐severe atopic dermatitis patients

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