Breast Cancer Clinical Trial
Official title:
Evaluation of the Effect of Pasireotide LAR Administration in the Lymphocele Prevention After Axillary Node Dissection for Breast Cancer
The principal morbidity following axillary node dissection within the scope of breast cancer
surgery is the post-operative development of lymphocele. According to the literature,
incidence can vary from 4 to 89% depending on the type of surgery, whether or not a drain is
inserted or a compression dressing applied and the time at which the drain is removed… In
our experience, the incidence is 40% [IGR (Gustave Roussy Institute) data focusing on 70
patients between November 2008 and February 2009]
Encouraging results in terms of reducing postoperative lymphoceles as well as drainage
duration and volume using Octreotide have been recorded in two recent studies. A new
molecule developed by Novartis Laboratories, namely pasireotide, is a somatostatin analog
possessing strong affinity for several somatostatin receptors (30 to 40 times greater for
sst1 and sst5, 5 times greater for sst3 and equivalent for sst2)
The purpose of this trial is to assess the efficacy of a pre-surgical injection of
pasireotide LAR in reducing the postoperative incidence of symptomatic lymphoceles following
axillary node dissection.
The secondary objectives are to assess the efficacy of prolonged release pasireotide on the
duration of postoperative drainage, the daily drainage volume, the total drainage volume,
the number of repeated lymphocele aspirations and the volume, the total volume of lymph
aspirated, the incidence of postoperative febrile episodes, the length of hospital stay, and
the length of time to onset of adjuvant chemotherapy. It is also to assess the safety of
prolonged release pasireotide.
The primary objective of this study is to assess the efficacy of a preoperative prolonged
release pasireotide injection in the reduction in the incidence of symptomatic,
postoperative axillary lymphoceles following mastectomy-axillary node dissection.
Octreotide, a somatostatin analog, has demonstrated its efficacy in the medical management
of postoperative gastro-intestinal and pancreatic fistulae. Two recent studies have shown
its value in reducing lymphoceles following axillary node dissection performed as part of
breast cancer surgery.
The principal morbidity following axillary node dissection within the scope of breast cancer
surgery is the postoperative development of lymphocele following the removal of an axillary
drain. This may be a source of pain, repeated aspiration, infection and delayed local
healing.
Pasireotide, a somatostatin analog under evaluation and possessing a high affinity for
somatostatine receptors (30 to 40 times greater for sst1 and sst5 receptors, 5 times greater
for sst3 and equivalent for sst2) is an attractive molecule in this indication.
Based on the encouraging results published with octreotide and the greater effects
anticipated with pasireotide, the investigators want to assess the benefit of preoperative
administration of pasireotide in reducing the incidence of axillary lymphoceles following
mastectomy - axillary node dissection.
Somatostatin is a hormone that is widely distributed in the nervous and gastropancreatic
system responsible for a variety of pharmacological and physiological effects. It can
inhibit gastrointestinal endocrine and exocrine secretion and has an anti-inflammatory
action (1). The direct effect of somatostatin on lymphatic flow has only been observed on
the gastrointestinal tract.
Several series report the use of octreotide in the treatment of chylous ascites or in the
management of thoracic duct injury (2). Although its mechanism of action has not been
studied in depth, it probably acts by inhibiting splanchnic blood flow and limiting the
absorption of triglycerides.
Somatostatin receptors have been demonstrated in lymphatic tissues, including those not
associated with the intestinal tract. It is therefore probable that the inhibitory action of
somatostatin on gastrointestinal lymphatic flow may also apply elsewhere in the body, and to
the lymphatic system in particular.
Somatostatin might therefore decrease lymphatic flow following essentially axillary
lymphadenectomy.
A new molecule, pasireotide, is currently in clinical development. This molecule is a
somatostatin analog possessing an affinity 30 to 40 times greater for sst1 and sst5
receptors, 5 times greater for sst3 and comparable for sst2 than octreotide. It could
therefore have a greater effect than octreotide.
The gradual release form must be injected intramuscularly prior to surgery. An effective
plateau concentration is obtained after 10 days regardless of the selected dosage (20, 40,
or 60 mg).
In addition to the many articles in the literature detailing the beneficial effects of
octreotide on gastrointestinal and pancreatic fistulae and on regression of chylous ascites
and chylothorax, a few articles have attempted to highlight its effect on postoperative
lymphoceles.
Firstly, two articles have highlighted the positive effect of somatostatin analogs in
reducing drainage volume and the incidence of lymphoceles following axillary node dissection
in breast cancer:
Another more recent article by Mahmoud et al. (5) showed the same beneficial effects on the
mean daily drainage volume (104 vs 145 ml, p=0.0001), the total duration of drainage (12.7
vs 25 days, p=0.0001) and the need for postoperative aspiration of lymphoceles (90 vs 40%,
p=0.0001).
In 2006, in a different field (that of renal transplantation), an article by Capocasale et
al.Pasireotide is an injectable somatostatin analog. Like natural somatostatin and known
analogs, its pharmaceutical efficacy depends on its binding to somatostatin receptors. There
are five of these (sst 1 to 5); they are expressed in various bodily tissues under normal
physiological conditions. Somatostatin analogs activate these receptors, which in turn
reduce cell activity and inhibits hormone synthesis. (7). Octreotide and lanreotide, which
are currently used, have a strong affinity for the sst2 receptor and moderate affinity, if
any, for the other types. Pasireotide possesses greater affinity than octreotide for certain
somatostatin receptors: 30 times greater for sst1, 5 times greater for sst3 and 40 times
greater for sst5. It possesses equivalent affinity for sst2 and none (like octreotide) for
sst4.
In the literature, the incidence of axillary lymphoceles following surgery for breast cancer
varies considerably: a recent meta-analysis of 66 studies revealed an incidence of 4 to 89 %
depending on whether or not drainage was being carried out, the type of surgery
(conservative or not), the time at which the drain was removed and whether or not a
compression dressing was applied.
In our experience, the incidence at Hôpital Tenon is 40%. This percentage has been
corroborated by Gustave Roussy Institute data, which recorded an incidence of 39.3% in out
of 70 patients who underwent surgery between November 2008 and February 2009.
Several teams have reported their use of Sandostatin® or other somatostatin analogs in the
management of patients suffering from inoperable peritoneal carcinoma (9-12). This treatment
was used as supportive therapy and reduced the incidence of symptoms associated with an
obstructive syndrome. It fact, it can reduce gastrointestinal secretions. Some authors have
even suggested that somatostatin analogs possess an anti-tumor effect (9). Octreotide is
recommended by AFSSAPS in the treatment of palliative care patients presenting with
intestinal occlusion in peritoneal carcinoma. Since a Marketing Authorization (MA) has been
granted for the use of somatostatin analogs in patients presenting with a gastrointestinal
endocrine tumor, the use of pasireotide does not raise any specific ethical issue.
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