Sclerosis tuberosa and pregnancy
Tuberózna skleróza a gravidita
Ciele:
Cieľom práce je podať aktuálny, komplexný a ucelený prehľad poznatkov o tuberóznej skleróze a typických komplikáciách tejto chorobnej jednotky spájaných s graviditou. Typ štúdie: Komplexný review. Pracovisko: 2. gynekologicko-pôrodnícka klinika LF UK a UNB, Univerzita Komenského Bratislava, prednosta prof. MUDr. Karol Holomáň, CSc. Metodika: Komplexná analýza syndómu, systematický rešerš vedeckej databázy MEDLINE a Slovenskej lekárskej knižnice. Dôvodom realizácie komplexnej prehľadovej práce bola naša klinická skúsenosť a manažment jednej z najzávažnejších a život ohrozujúcich komplikácií tuberóznej sklerózy v gravidite – akútneho retroperitoneálneho krvácania tehotnej ženy. Záver: Tuberózna skleróza v gravidite môže zapríčiniť hoci zriedkavé, no potenciálne závažné, až život ohrozujúce komplikácie najmä v gravidite. Komplikácie v gravidite je nutné striktne dispenzarizovať a monitorovať a v akútnych stavoch je nutné neodkladne rozhodnúť o promptnom radikálnom manažmente pacientky. Kľúčové slová: m. Bourneville-Pringle, sclerosis tuberosa, tuberózna skleróza, fakomatóza, gravidita, angiomyolipóm, retroperitoneálne krvácanie
Authors:
M. Gábor 1; V. Ferianec 1; I. Mečiarová 2; Peter Papcun 1; K. Holomáň 1
Authors place of work:
Department of pathology Ružinov, Alpha medical patológia, s. r. o., Bratislava, Slovak Republic, doc. MUDr. F. Ondriáš, CSc.
2; nd Department of Obstetrics and Gynaecology, University Hospital Bratislava, Comenius University, Bratislava, Slovak Republic, prof. MUDr. K. Holomáň, CSc.
12
Published in the journal:
Ceska Gynekol 2014; 79(3): 186-189
Summary
Objective:
To perform a review of Tuberous sclerosis complex and its complications during the pregnancy from up to date scientific literature. Design: Complex systematic review of the literature. Setting: 2nd Department of Obstetrics and Gynaecology, University Hospital Bratislava, Comenius University, Bratislava, Slovak Republic. Methods: Complex analysis of the syndrome, systematic search of MEDLINE and Slovak Medical Library. The reason to create a complex review of this syndrome was our clinical experience with one of the most acute lifethreatening condition of this syndrome – acute retroperitoneal haemorrhage in the pregnancy. Conclusion: Tuberous sclerosis can cause a rare, but potentially lifethreatening complications, especially during the pregnancy. These should be carefully dispesarized and in complicated cases acute radical management should be considered. Keywords: m. Bourneville-Pringle, sclerosis tuberosa, tuberous sclerosis, phacomatosis, pregnancy, angiomyolipoma, retroperitoneal haemorrhage
SCLEROSIS TUBEROSA SYNDROME
Tuberous sclerosis (TS, synonym Epiloia seu Bourneville-Pringle disease) is a neurocutaneous syndrome and the second most frequent phacomatosis (gr. “phacos“ means birthmark).
It was described by Désiré-Magloire Bourneville for the first time in 1880. TS is a hereditary disease affecting ectodermal tissues. In childhood it has a slow progression with typical growth of benign tumours called hamarthomas in different anatomical locations. It is a rare disease with a prevalence in the population 1:10 000 and incidence 1:6000, occuring almost identically in all races, ethnic groups and both genders [6, 13, 27].
GENETICS, CLINICAL MANIFESTATIONS, DIAGNOSTICS AND THERAPY
From a genetic point of view, this is a tumoursupressor disease with variable expresivity, high penetrance and autosomal dominant inheritance. Two different genes whose mutations can cause this syndrome have been identified – TSC1 and TSC2. Both genes belong to the tumoursupressors gene group, which regulates proliferation of the cells. “De novo“ mutations are very frequent (up to 80 percent) and clinical manifestation is usually more serious [11, 18]. The clinical signs and symptoms depend on organ manifestation. Potentially, TS can affect every tissue in the body. Most frequent manifestations are hamarthomas in the skin, brain, kidneys, lungs, heart, endocrine glands, bones and the retina.[6,18] Primary diagnosis is usually made by pediatricians and neurologists in childhood. TS can vary from “only“ cosmetic skin defects, to severe organ damage.[13, 25]. The most important diagnostic criteria are cerebral lesions causing epileptic seizures, mental retardation, cerebral palsy and psychiatric disorders, skin lesions include facial angiofibromas called adenoma sebaceum, subungual and periungual fibromas called “pringle tumours“, rough spots of Schagren “pig-elephant“ skin, etc. Other common organ presentations are cardiac rhabdomyomas, retinal hamarthomas, renal angiomyolipomas, hamarthomatous rectal polyps, etc. Malignant change of these tumours is very rare [3, 8, 10]. The leading imaging modalities in diagnostics of TS lesions are computed tomography, magnetic resonance imaging and ultrasonography. Additional examinations by dermatologist, ophthalmologist and psychiatrist are useful [1, 2, 18, 27]. Some kidney tumours were incidentally diagnosed also during standard ultrasound examination in the pregnancy [19]. Final diagnosis is based on DNA analysis of the TSC1 or TSC2 gene mutations, clinically on main signs according to actual classification. Reliable methods used in diagnostics of mutations are PCR, quantitative PCR and gene sequencing. Useful modalities in the diagnosis of TS are described in table 1.
Causal therapy of TS is not yet available and treatment is only symptomatic. Tiberio et al. in 2011 described a case of significant regression of a cardiac rhabdomyoma after receiving Everolimus, an mTOR inhibitor (mammalian target of Repamycine inhibitor). This finding suggested a possible novel therapy for patients with clinically significant cardiac rhabdomyomas [26].
For subependymal giant-cell astrocytomas in patients with the TS the standard treatment is the neurosurgical resection. In the Kruegers study (2010) the Everolimus therapy was associated with marked reduction in the volume of subependymal giant-cell astrocytomas and seizure frequency and may be a potential alternative to neurosurgical resection in some cases, though long-term studies are more needed [17].
Dispensarisation of the patient is necessary. The prognosis depends on the localisation of the lesions. Slow progression, especially alteration of the cognitive functions, often leads to terminal state in early adulthood. Prognosis quad vitam for incomplete forms of the syndrome is better [18].
PRENATAL DIAGNOSTICS
Prenatal screening of TS is recommended if positive family history of TSC gene mutations has been identified [23]. The most frequent ultrasound marker of TS affected fetus is the presence of cardiac rhabdomyoma [15]. This benign tumour with poor prognosis is usually recognized after the 29th week of gestation by fetal ultrasound examination, especially fetal echocardiography. Despite its benign dignity, extensive tumours affecting cardiac outflow tracts can cause haemodynamic alteration of the fetus. Tumours totally involving outflow tracts and extensively expanding pericardium have been described. These severe cases are often related to fetal hydrops and intrauterine death in the second trimester is common [15, 29]. After primary in utero diagnosis of the left outflow tract obstruction, it is necessary to provide postpartal emergent surgical intervention [9, 20]. Prenatal diagnosis is recommended for fetuses in the high risk group – a positive family history or the presence of cardiac rhabdomyoma. The leading procedure is amniocentesis or chorionic villus sampling [7]. For a detailed image of cardiac lesions fetal magnetic resonance may be also beneficial. Prognosis and management should be consulted with pediatricians and cardiac surgeons. Fortunately, cardiac rhabdomyomas usually slowly regresses in the first year of life. Possible ultrasound markers of TS are also cerebral cortical tubers and cerebral astrocytomas. Unfortunately, these tumours do not tend to regress, on the contrary, there is progression in their growth and count [21, 30].
TUBEROUS SCLEROSIS IN THE PREGNANCY AND TYPICAL ACUTE COMPLICATIONS
In the management of early pregnancy, it is necessary to consider the influence of administred anticonvulsive drugs. Spontaneous abortion and fetal demise are very frequent. Except general complications of TS, the lifethreatening complication associated with pregnancy is retroperitoneal haemorrhage (figure 1). The high risk of retroperitoneal haemorrhage is associated with renal angiomyolipomas. Frequently the tumours can be very big, in the literature tumours weighing 5700 g or more have been described [22]. Physiological haemodynamic changes in pregnancy induce this complication, which threaten the patient mostly in the third trimester. Vaginal delivery is also considered as a risk factor [22]. In a retrospective study of these tumours and their associated complications in the period between 1952 and 2004, 72 cases were described. 58 cases were complicated in average gestational age at 27th week [16].
In the surgical management of this complication, the total nephrectomy in 79 percent of cases was indicated [16], rarely polar nephrectomy or selective arterial embolisation were performed [16]. If possible, also a conservative management with strict monitoring can be applied. Another possibility to solve the complication is to perform the therapeutical selective arterial embolisation of the tumour vessels. In the cases of multiple angiomyolipomas, repeated early prophylactic embolisations are also suitable. If tumour embolisation does not tend to prevent or to stop the bleeding, radical surgery is indicated, after the 28th week with simultaneous caesarean section (SC) [12]. As a mode of delivery SC is recommended [12]. In the case of bilateral tumour masses, it is possible to succeed with nephron-sparing tumorectomy [5, 24]. Giant bilateral renal masses without signs of bleeding should be managed without radical surgical intervention, prophylactic embolisation and strict follow-up management is indicated [14]. Ferianec et al. in 2013 reported an unique acute complication of TS. He described severe retroperitoneal haemorrhage of the 30-year-old primigravida in the first trimester of a multiple pregnancy. The complication was presented after spontaneous rupture of renal angiomyolipoma caused by TS. The authors reported that acute renal lifethreatening complication of TS is not only typical for 2nd or 3rd trimester and the coincidence with multiple pregnancy can lead to its very early onset in the early pregnancy [4].
Martin Gábor, MD
University Hospital Bratislava
Ružinovská 6
826 06 Bratislava
Slovak Republic
e-mail: martingabormd@gmail.com
Zdroje
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Štítky
Paediatric gynaecology Gynaecology and obstetrics Reproduction medicineČlánok vyšiel v časopise
Czech Gynaecology
2014 Číslo 3
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