Urinary Incontinence Clinical Trial
Official title:
Transurethral Autologous Myoblast Injection for Treatment of Urinary Incontinence in Children With Bladder Exstrophy
Muscle precursor cells constantly regenerate striated muscles, and include the quiescent
satellite cells located beneath the basal lamina of skeletal myofibers, which are
responsible for repair of the terminally differentiated striated muscle tissue.
Transurethral implantation of autologous myoblasts may represent an improved alternative to
synthetic bulking agents, with the unique ability to compensate for the deficient muscle
fibers in the urethral sphincter. Clinical studies of cell therapy based treatment of
sphincter insufficiency, using muscle derived stem cell transplantation was carried out in
patients with stress incontinence revealed and confirmed the ability of cell therapy to
improve the structure and contractile function of the sphincter. In this study autologous
heterotopic myoblasts will be transurethrally injected in patients with bladder extrophy
epispadias complex who remained incontinent after staged bladder reconstruction and bladder
neck reconstruction.
The aim of this study is to investigate the potential therapeutic effects of autologous
myoblast injection for the treatment of children presenting with urinary incontinence after
modern staged repair and bladder neck reconstruction of extrophy-epispadias complex as well
as studying the safety, efficacy and durability of the procedure, and health related quality
of life.
Achieving urinary continence in patients with bladder extrophy epispadias complex remains a
challenging urological goal. Children with bladder extrophy epispadias complex generally
undergo many surgical procedures for the treatment of sphincteric incompetence, including
bladder neck reconstruction, slings and bulking agent injection. The key point in most of
these procedures is to enhance urethral resistance, leading to some degree of bladder outlet
obstruction. However, the reported 7% to 85% continence rates in these patients may not
exactly represent those children who achieve volitional voiding through the urethra, but may
also include the ones with bladder augmentation and urinary diversion. Endoscopic injection
of bulking agent has emerged as a therapeutic approach in the treatment of urinary
incontinence (UI). this procedure seems to be economical, with shorter hospitalization and
fewer major complications. On the other hand, degradation, migration, reabsorption,
overbulking, bladder outlet obstruction and hypersensitivity are frequently reported
complications of bulking agents.
The ideal substance for periurethral injection should be durable, non immunogenic,
nonmigratory and efficacious. So, transurethral implantation of autologous myoblasts may
represent an improved alternative to synthetic bulking agents, with the unique ability to
compensate for the deficient muscle fibers in the urethral sphincter. Patients with
incontinence usually have decreased resting tone and contractility of the rhabdosphincter.
In patients with bladder extrophy epispadias complex the perineal structures are dislocated
laterally, and the internal and external urethral sphincters are deficient. Muscle precursor
cells constantly regenerate striated muscles, and include the quiescent satellite cells
located beneath the basal lamina of skeletal myofibers, which are responsible for repair of
the terminally differentiated striated muscle tissue. After injury or in response to
intensive physical exercise satellite cells proliferate and differentiate into myoblasts,
which ultimately fuse to form new myofibers capable of muscle contraction. Considering the
limited capacity of the rhabdosphincter for regeneration, the idea of urethral sphincter
repair in patients with bladder extrophy epispadias COMPLEX via transurethral injection of
autologous myoblasts has been suggested. The technical availability of these cells, as well
as immunological acceptance and survival, makes them appropriate for this purpose. Satellite
cells are committed cell lineage with restricted plasticity and do not multiply beyond the
required repair needs. This property confers an acceptable measure of safety for clinical
applications. The first clinical study of cell therapy based treatment of sphincter
insufficiency, using muscle derived stem cell transplantation was carried out in patients
with stress incontinence revealed and confirmed the ability of cell therapy to improve the
structure and contractile function of the sphincter.
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Endpoint Classification: Safety/Efficacy Study, Intervention Model: Single Group Assignment, Masking: Open Label, Primary Purpose: Treatment
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