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A patient with pycnodysostosis presenting with seizures and porencephalic cysts
Address for correspondence: Dr. Subhash Kumar, 103, Type IV, Block 2, All India Institute of Medical Sciences, AIIMS Residential Complex, Hydraulic, Khagaul, Patna - 801 105, Bihar, India. E-mail: drsubhash.dm@gmail.com
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Abstract
Pycnodysostosis is a rare autosomal recessive disorder caused by mutations in the cysteine protease Cathepsin K gene located on chromosome 1q21. It has a well characterized skeletal phenotype which include short stature, generalized increased bone density with propensity of fractures, open calvarial sutures and fontanelle, dental abnormalities, obtuse mandibular angle, resorption of lateral end of clavicle, acro-osteolysis, and in some cases visceromegaly. Central nervous system involvement is very rare and porencephalic cysts has been reported only once, the cause being hypothesised to be an imbalance between the growing brain, its vascular supply and intraventricular fluid pressure. We had a patient with bilateral frontal lobe porencephalic cysts; the patient presenting with complex partial seizures. Cathepsins have been found to be involved in neurological diseases and role of proteases has been well established in gliosis.
Keywords
Cathepsin K
porencephalic cyst
porencephaly
pycnodysostosis
seizures
Introduction
Pycnodysostosis is a rare autosomal recessive disorder caused by mutations in the gene encoding the cysteine protease Cathepsin K.[1] It has a well characterized skeletal phenotype,[2] but rarely reported central nervous system involvement. Porencephalic cysts in pycnodysostosis have been described only once previously and its cause proposed to be an imbalance between the brain growth and its vascular supply and a normal but unopposed cerebrospinal fluid pressure.[3] Recent genetic advances however provide more insight into the involvement of the brain.
Case Report
An 18 year old male, 2nd child out of five from a non-consanguineous marriage, presented with recurrent episodes of right sided complex partial seizures for last three years. Initial frequency of seizures was 1-2 per month which had increased to 3-4 per month at the time of presentation. No history of trauma or other significant medical or surgical illnesses was present. There was no history of seizure disorder or dwarfism in his family. On examination he was of short stature (4 feet and 4 inches) and underweight (25 kg) with a normal upper-lower segment ratio, normal arm span and normally developed secondary sexual characters. He had normal mental and memory functions and had no sensory and motor abnormalities. No cranial nerve deficits were present. Hematological examination was normal and an ultrasonographic exam of abdomen was normal as well. MRI of the brain showed bilateral frontal lobe porencephalic cysts [Figure 1]. Radiographs and plain CT scan of the head revealed generalized increased bone density [Figure 2]. Obtuse angle of mandible and dental crowding were noted [Figure 2a]. The calvarial sutures and fontanelle were wide open with presence of multiple Wormian bones in the region of the lambda [Figure 2b]. The skull base was also sclerotic [Figure 2c]. The vertebrae were spool shaped [Figure 2d] and there was presence of acro-osteolysis [Figure 2e and f]. The thoracic cage was narrow [Figure 2g]. Bone within bone appearance or Erlenmeyer flask deformity of the long bones were not seen [Figure 2h].
- (a) Axial T2W and (b) Coronal FLAIR images show bilateral frontal lobe porencephalic cysts
- (a) X-ray showing obtuse gonial angle and crowded teeth (b) CT head showing open sutures and fontanelle with multiple Wormian bones (c) Axial CT head, showing sclerosed skull base (d) Dorsolumbar spine X-ray showing sclerosed, spool shaped vertebrae (e) X-ray both hands and (f) Feet showing acro-osteolysis (g) Narrow chest; the clavicles do not appear hypoplastic in this case (h) X-ray both legs, showing sclerosed long bones; there is no ‘bone within bone appearance’ or ‘Erlenmeyer flask deformity’ thus differentiating from osteopetrosis. Also see the supplementary file
Discussion
Pycnodysostosis is a rare autosomal recessive disorder first described in 1962[4] and its gene mapped to chromosome 1q21 in 1995.[5] It is caused by mutations in Cathepsin K gene, a cysteine protease highly expressed in osteoclasts.[1] Apart from the classical diagnostic features of short stature with fragile sclerotic bones, obtuse mandibular angle, acro-osteolysis, hypoplastic clavicles (not seen in the present case - Figure 2g), and open cranial sutures and fontanelles with the presence of multiple Wormian bones, other features include[167] thick calvaria, hypoplastic paranasal sinuses, relative proptosis and beaked nose, persistence of deciduous teeth, with premature or delayed eruption of permanent teeth, causing crowding and double row of teeth. Also seen are tooth misalignment, enamel hypoplasia, and a grooved palate.[6] Trunk deformities like kyphosis, scoliosis, and a narrow chest are seen. Patients may present with frequent fractures, recurrent dental abscesses or sleep apnea[6] although our patient did not have any of these and had presented with complex partial seizures which has not been reported earlier. Usually there are no visceral manifestations, although cases of extra medullary hematopoiesis and hepato-splenomegaly have been reported.[8]
A variety of neurological abnormalities have been described in the various skeletal dysplasias however; pycnodysostosis seems to have been spared at large.[9] Porencephalic cysts have been reported only once earlier.[3] The authors proposed that the persistence of open sutures and fontanelles allows the normal but unopposed intra-ventricular fluid pressure to progressively distend the brain parenchyma. Thus a state of imbalance is created between the enlarging brain and its vascular supply resulting in the porencephalic cyst. This simplistic explanation gets a little complicated by the genetic information added over the last few years. Among all the various cathepsins, the Cathepsin K protease, whose deficiency is considered responsible for pycnodysostosis, is the most potent mammalian elastase yet described. In adults, it is generously distributed in various tissues such as bone, heart, lung, spleen, kidney, liver, thymus, intestine and pancreas, arterial smooth muscle cells, synoviocytes, breast carcinoma cells, endometrium, thyroid epithelial cells, multinucleated giant cells, etc., although it is predominantly expressed in osteoclasts and macrophages.[110] Parenchymal microglial cells are uncommitted myeloid progenitors of immature dendritic cells and macrophages and match their Cathepsin profile.[11] Considering that the role of microglia has been established in gliosis, it is not hard to surmise a more direct interrelation between pycnodysostosis and gliotic changes in brain. Neuronal death has been found to be associated with Cathepsins B and L[12] but not Cathepsin K which is not overtly expressed in brain. However, there is an interplay between the various proteases[13] and Cathepsin K has been found to be associated with schizophrenia.[14] A skeletal dysplasia with known cerebral abnormalities including porencephaly is the oculo-facial-digital syndrome.[15] which is caused by a mutation in CXORF5 gene, located on Xp22.3-22.2. OFD I protein, which is essential for foetal survival and early development of the mouth, face, hands and feet is entirely different form the Cathepsins.
A better understanding of the molecular events responsible for pycnodysostosis, gliosis, porencephalic cysts and the role of cathepsin K in the nervous system is thus required, especially so since trials of anti-cathepsin drugs are underway in an attempt to treat osteoporosis.
Acknowledgments
Dr. NK Mishra, Prof and Head, and Dr. SB Gaikwad, Prof, Department of Neuroradiology, AIIMS, New Delhi.
Source of Support: Nil.
Conflict of Interest: None declared.
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