Case Report: Moyamoya Disease: A Case Report in a 10 Years Old Sudanese Girl Volume 54- Issue 1

Amjed Abdu¹, Thowiba Mohammed², Mustafa Ahmed³, Basharia Abdalla⁴ and Sufian Khalid^5*

• ¹Assistant Professor, Department of Pediatrics, Faculty of Medicine, Nile Valley University, Sudan
• ²Houseman ship at ATBRA TEACHING HOSPITAL, River Nile state, Sudan
• ³Teaching Assistant, Department of skills lab and problem based learning, Faculty of Medicine, Ahfad University for Women, Sudan
• ⁴Houseman ship at ATBRA TEACHING HOSPITAL, Sudan
• ⁵Professor of Internal medicine, Faculty of Medicine, Nile Valley University, Sudan

Received: December 01, 2023; Published: December 14, 2023

*Corresponding author: Sufian Khalid Mohammed Noor, Professor of Internal medicine, Faculty of Medicine, Nile Valley University, Sudan

DOI: 10.26717/BJSTR.2023.54.008509

Abstract PDF

Background: Moyamoya disease (MMD) is a rare pathology caused by a progressive unilateral or bilateral stenosis of the terminal portion of the internal carotid artery, leading to the development of collateral vessels.

Case presentation: We report a rare case of a10 years old girl, presented with sudden onset of left side weakness not associated with headache or vomiting. The diagnosis of MMD was established when the cerebral angiogram revealed moderate proximal right MCA stenosis together with aplastic A1. The left ICA showed T occlusion at bifurcation with very strong collaterals.

Conclusion: This case highlights the importance of considering moyamoya disease to be one of the classic etiologies of acute ischemic strokes in children from North Africa. It also emphasizes the rare presentation among the African population and the use of neurovascular imaging techniques to facilitate diagnosis of moyamoya disease.

Abbreviations: MAD: Moyamoya Disease; AIS: Acute Ischemic Stroke; DSA: Digital Subtraction Angiogram

Moyamoya disease is a chronic, progressive occlusion of the circle of Willis arteries that leads to the development of characteristic collateral vessels evidence by imaging, particularly cerebral angiography [1]. The disorder initially involves the intracranial portion of the internal carotid arteries and progresses to involve the middle, anterior and posterior cerebral arteries. Collateral vascular network developed due to compensatory dilatation of lenticulostriate and thalamostriate arteries. Angiographic study of these collateral vascular network give rise to characteristics appearance such as a pu of cigarette smoke. e Japanese term “MOYAMOYA” means “some thing hazy like a pu of cigarette smok [2,3]. Moyamoya disease was first described in Japan by Takeuchi and Shimizu in 1957. Ough e disease is most common in Japan, many subsequent cases have been reported elsewhere Asia, Europe and North America. In 1988 the Japanese Ministry of Health and Welfare defined primary MMD as an idiopathic bilateral stenosis of arteries of the circle of Willis with collateral vascular networks, demonstrated on angiography. Recent studies indicate that the amount of collateral vessels at the base of the skull serve as markers of disease severity and degree of progression [4]. The gold standard in the current diagnosis of Moyamoya disease is cerebral angiography. As it is an invasive exam, we can use other methods such as angiotomography and MR angiography, which are non-invasive exams. Currently, there is no specific treatment to prevent the progression of Moyamoya disease. However, the procedure predilection for patients with ischemic and hemorrhagic strokes is surgical revascularization (extracranial-intracranial bypass) [5,6].

A 10 years old girl of consanguineous parents presented complain of left side weakness and right loin pain for 2days. Here parents stated that she developed sudden left side hemiplegia to extent that she unable to stand or walk. After this episode she gradually improved in standing & walking but weakness persist that made her walking difficult There was no history of fever, Loss of consiousness, vomiting, or aphasia along with this illness and no history of radiation exposure or head trauma mentioned before this. No family history of similar condition. Had past history of appendectomy, not on long term medications. On examination she has no dysmorphic features, vital signs within normal range, no skin change. Neurological examinations revealed that she had normal tone, power 4l5 on left side along with hyperreflexia, exaggrarated ankle clonus and positive Babinski sign. Other CNS examinations were normal. Investigations requested include complete blood count, random blood glucose, urine analysis were normal abdominal ultrasound revealed right renal stone. MRI brain with contrast revealed: Bilateral signal changes involving both temporal lobes with partial involvement of adjacent gyri of both frontal lobes may represent encephalitis. The acute infract involving the territory of MCA could be a complication of this encephalitis or represent separate entity so we have periventricular leukomalacia more extensive seen on left side, this could be a result of previous hypoxic event involving branches of this left MCA. The bilateral involvement of deep white matter of both cerebellar hemispheres with associated cortical multiple ischemic foci could be a result of posterior circulation insuffiency (Figure 1). Other investigations was done cerebral angiogram and revealed moderate proximal right MCA together with aplastic A1… The left ICA showed T occlusion at distal bifurcation with very strong collaterals… Normal vertebra-basilar system…. Features consist with vasculitis (Figure 2).

Figure 1

Figure 2

Compared with adults, acute stroke is an infrequent disease of pediatric patients. In fact, the reported incidence of childhood stroke has increased in the last 20 years according to population studies, most likely related to improvements in neurological techniques [7]. There are numerous causes of stroke in childhood, These include congenital heart disease, sickle cell disease, immune disorders, clotting disorders, and head and neck trauma. However, MMD should be included in the differential for a stroke in a child. In fact, MMD represents one of the most severe arteriopathies and accounts for approximately one fifth of identified cerebral arteriopathies in children presenting with acute stroke and is diagnosed in up to 20% of cases of childhood acute ischemic stroke (AIS) [8]. The condition is common In Japan and East Asia, where familial cases are also clearly recognized. In Japan, the annual prevalence and incidence have been estimated to be 3.16–10.5 and 0.35–0.94 per 100,000 [9]. The female to male ratio has been shown to be 1.8-2.2 (female predominance) [10]. The familial form accounts for 10–15% [11]. Moyamoya is categorized as MMD when there is no underlying etiology or association and as moyamoya syndrome if an underlying etiology or association of other conditions is recognized, including trisomy 21, Down syndrome, neurofibromatosis type 1, and cranial irradiation. In our patient, no association of any other systemic disorder was described. Furthermore, most general medical conditions were excluded by normal blood, urine studies, and negative history of fever or trauma. A normal physical examination ruled out increased intracranial pressure as well as meningitis. Pathological changes in moyamoya patients include intimal thickening with brous tissue, abnormalities of internal lamina elastica, variable lipid deposition and virtual absence of inflammatory reaction in the blood vessel [12,13]. Clinically, the presentation of patients with moyamoya disease may include seizures, transient ischemic attacks, ischemic strokes, and hemorrhagic strokes [14-16].

Visual decits, speech disturbance, migrane like headache, intellectual deterioration, cranial nerve palsies, and disturbance of gait can also be evident [17,18]. Our patient presented with ishchemic stroke. Conventional angiogram or Digital subtraction angiogram (DSA) is the investigation of choice. MRA has a reliable diagonostic modality for MMD [19]. Treatment in the acute phase is symptomatic with the goal of maintaining cerebro-vascular perfusion and function. Anticoagulant and antiplatelet agents have shown no remarkable benet [20]. e same lack of obvious ecacy has been described for corticosteroids in moyamoya disease [21]. McLean et al, elucidated the use of verapamil hydrochloride to curtail the ischemic symptoms associated with moyamoyadisease [22], Surgical treatment modalities have been used to manage the hemorrhagic and ischemic consequences of moyamoya disease [12,23-25] Dir ectrevascularization techniques, which are typically used in adults, include the supercial temporal artery to middle cerebral artery bypass or the middle meningeal artery to middle cerebral artery bypass are commonly applied in children [25,26].

Although Moyamoya is predominat in Japanese population but should not overlooked in other population. e patient who will fulll the clinical characteristics, MR angiogram should be done to diagnose Moyamoya disease.

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3. Dr Subrota Kumar Roy, Assistant Professor, Department of Paediatrics, Dhaka Medical College, Dhaka
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