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Eur J Pediatr Surg 2011; 21(2): 134-136
DOI: 10.1055/s-0030-1261883
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© Georg Thieme Verlag KG Stuttgart · New York

Bleomycin Sclerotherapy for Extensive Lympho-Venous Malformation. A Retrospective Analysis of A Patient's Death

S. Kantorowicz1 , K. Kobylarz2 , P. Wojciechowski1
  • 1Jagioellonian University, Pediatric Surgery,Kraków, Poland
  • 2Jagioellonian University, Pediatric Anesthesiology, Kraków, Poland
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Publication History

Publication Date:
28 July 2010 (online)

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Introduction

Lympho-venous malformations (LVM) in children may be localized everywhere in a child's body as limited or extensive malformations, including a few anatomical regions representing errors in vascular and lymphatic development. LVM are classified as combined malformations [1]. A radical surgical excision of the malformation reported to be the best treatment, however in extensive LVM complete resection of the malformation is impossible. Incomplete resection of the malformation leads to recurrence and over-resection leads to tissue and organ damage [2] [3] [4]. Thus, the search for a non-surgical form of treatment for LVM continues. Direct injection sclerotherapy has been proposed with few side-effects, but the effectiveness of direct sclerotherapy was poor.

Yura and co-workers in 1997 reported good results with bleomycin sclerotherapy of lymphatic malformations (LM) after unsuccessful surgical treatment [5]. Other centers have been skeptical of this treatment due to the unclear therapeutic mechanism of bleomycin and high risk of post therapeutic pulmonary complications [6] [7].

An early toxic effect on pulmonary tissue was observed in 10% of all oncologic patients who received i. v. bleomycin therapy and presented with fever, dry cough, dyspnea at rest and cyanosis. Permanent damage to pulmonary tissue causing pulmonary fibrosis after bleomycin therapy was described as occurring some weeks or even months after treatment. In patients who underwent bleomycin therapy, spirometric restrictive changes were described. Vital capacity (VC), total lung capacity (TLC) and diffusion lung capacity for carbon monoxide (DLCO) have been shown to decrease. A DLCO below 40% of initial values is a simple contraindication to bleomycin therapy. Early as well as late pulmonary toxicity of bleomycin with progressive pulmonary fibrosis causes death in 1–2% of patients [8] [9].

A combined treatment of a patient with extensive LVM who died at the age of 20 years is presented.

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Correspondence

Dr. Piotr Wojciechowski

Jagiellonian University

Pediatric Surgery

Wielicka 265

PL-60-663 Kraków

Poland

Phone: +48 60 2634 722

Fax: +48 12 6581 325

Email: piwojr@vp.pl

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