Lingual microcystic lymphatic malformations (LMLMs) are rare congenital vascular malformations, presenting as clusters of cysts filled with lymph fluid or blood. They are responsible for a heavy burden even with small well-limited lesions because of oozing, bleeding, infections, or even speech, chewing or breathing impairment. Pain and aesthetic prejudice are also frequently reported. The natural history of LMLMs is progressive worsening. LMLMs complex management requires multidisciplinary care in specialised centres, and the "wait-and-see" approach is frequently used. In complicated lymphatic malformations, whatever the location, treatment with oral sirolimus, an mTOR (mammalian Target of Rapamycin) inhibitor, is often used. Topical sirolimus is a known effective treatment for some cutaneous conditions such as angiofibromas in tuberous sclerosis. Topical applications of sirolimus on the buccal mucosae have been reported in erosive lichen planus and oral pemphigus vulgaris with good tolerance and none to slight detectable blood sirolimus concentrations. The objective of this study is to evaluate the efficacy and safety of a 1mg/mL sirolimus solution applied once daily on mild to moderate lingual microcystic lymphatic malformation in children and adults after 4, 8, 12, 16, 20 and 24 weeks of treatment as compared to usual care (no treatment).
This is a randomized, open-labelled, multicenter pilot study using an individually randomized stepped wedge design over a 24 weeks period to evaluate topical application of 1 mg/mL sirolimus solution, 0.5 mL to 1 mL according to the size of the lesion, once daily, on lingual microcystic lymphatic malformation that do not require systemic treatment, the experimental intervention versus usual care (no treatment), the control condition. In this design, subjects are included in a cohort where at a randomized time (W0, W4, W8 or W12), they switch from an observational period to the interventional period. All subjects will be followed for 24 weeks
Study Type
INTERVENTIONAL
Allocation
RANDOMIZED
Purpose
TREATMENT
Masking
SINGLE
Enrollment
12
0.5 mL to 1 mL according to the size of the lesion, once daily, on lingual microcystic lymphatic malformation
Univsersity of TOURS _ Service de Dermatologie
Tours, Indre et Loire, France
Hospital NECKER -AP-HP - Dermatology
Paris, France
Change in Physical Global Assessment (PGA) after topical application of Sirolimus for 12 weeks
The primary outcome will consist in the evaluation of global severity of the LMLM using PGA (Physical Global Assessment) 0 to 5 score, by three independent blinded experts, on monthly standardized photographs. A 1-point improvement versus baseline in PGA scale would already have a clinical relevance. Our primary analysis will focus on change in PGA after topical application of Sirolimus for 12 weeks
Time frame: 12 weeks
Investigator-assessed PGA
Investigator-assessed PGA (Physical Global Assessment)
Time frame: at weeks 0, 4, 8, 12, 16, 20 and 24
Assessment by the patient regarding severity of oozing, bleeding, sialorrhea, eating impairment, taste modification, aesthetic impairment, pain and global discomfort,
Assessment by the patient regarding severity of oozing, bleeding, sialorrhea, eating impairment, taste modification, aesthetic impairment, pain and global discomfort, each using a numeric scale from 0 to 10 (0: clear, 10: very severe), at weeks 0, 4, 8, 12, 16, 20 and 24
Time frame: at weeks 0, 4, 8, 12, 16, 20 and 24.
Global evolution assessed by the patient
Global evolution assessed by the patient from -10 to 10 (-10 = severe worsening, 0 = no change, 10 = complete recovery), at weeks 4, 8, 12, 16, 20 and 24.
Time frame: at weeks 4, 8, 12, 16, 20 and 24.
Global Quality of life assessment
(DLQI or children's DLQI for minors aged 5 to 16), at baseline, time of switch to treatment and week 24.
Time frame: at baseline, at time of switch to the intervention (either week 0, week 4, week 8 or week 12) and week 24.
Measurements of the lesion
by the investigator, at baseline, time of switch to treatment and week 24.
Time frame: at baseline, at time of switch to the intervention (either week 0, week 4, week 8 or week 12) and week 24.
Time to obtain optimal results
i.e. time from switch to treatment to time reaching the minimal PGA score
Time frame: up to 24 weeks
Assessment of tolerance of topical sirolimus:
record of local side effects at each visit after the patient has crossed over to the intervention, up to 24 weeks
Time frame: from the switch to intervention up to the end of the study, i.e a maximum of 24 weeks.
General side effects
Follow-up of general side effects
Time frame: rom the switch to intervention up to the end of the study, i.e a maximum of 24 weeks.
Assessment of sirolimus blood passage
by measuring residual sirolimus blood concentration: after 4 weeks of treatment, then 8 weeks, then every 8 weeks until week 24
Time frame: after 4 weeks of treatment, then 8 weeks, then every 8 weeks until week 24
Evaluation of biological safety
Number of participants with at least one biological abnormality treatment-related adverse events as assessed by CTCAE v4.0
Time frame: after 8,16 and up to 24 weeks
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