[Background] Lipoid proteinosis (LP) is a rare autosomal recessive disorder characterized by a hoarse voice, variable scarring, and infiltration of the skin and mucosa. This disease is associated with mutations of the gene encoding extracellular matrix protein 1 (ECM1). 
[Case Report]This was a clinical and molecular study of a new case of LP with a severe phenotype. A 35-year-old female born to nonconsanguineous parents developed dermatological and extracutaneous symptoms in her 9th month of life. The neurological abnormalities of the disease began to appear at the age of 19 years. Computed tomography revealed cranial calcifications. 
[Conclusions]The diagnosis of LP was confirmed by histopathological findings and direct sequencing of ECM1. A new homozygous nonsense mutation was identified in exon 7 of ECM1, c.1076G>A (p.Trp359*). This mutation was not detected in 106 chromosomes of healthy individuals with a similar demographic origin. Microsatellite markers around ECM1 were used to construct the haplotype in both the parents and the patient. Reports on genotype-phenotype correlations in LP point to a milder phenotype in carriers of missense mutations in the Ecm1a isoform, whereas mutations in the Ecm1b isoform are thought to be associated with more severe phenotypes. The present findings in a Spanish patient carrying a truncating mutation in exon 7 revealed complete dermatological and neurological manifestations. © 2014 Korean Neurological Association.The authors thank the patient and her family for their participation, and the financial support of grants from MICINN (no. SAF2007-60508) and Consejería de Ciencia Junta de Andalucía (no. CVI02790).Peer Reviewe

Delgado-Valverde, Mercedes

García-Bravo, Begoña

García-Moreno, José Manuel

Lucas, Miguel

Martínez Mir, Amalia

Mondéjar, Rufino

Rubio, Rocío

Ríos-Martín, Juan José

Solano, Francisca

Digital.CSIC

64  Copyright © 2014 Korean Neurological Association  Print ISSN 1738-6586 / On-line ISSN 2005-5013http://dx.doi.org/10.3988/jcn.2014.10.1.64CASE REPORTJ Clin Neurol 2014;10:64-68Clinical and Molecular Study of the Extracellular Matrix Protein 1 Gene in a Spanish Family with Lipoid ProteinosisRufino Mondejar,a Jose Manuel Garcia-Moreno,b Rocio Rubio,c Francisca Solano,c Mercedes Delgado,c  Begona Garcia-Bravo,d Juan Jose Rios-Martin,e Amalia Martinez-Mir,f Miguel LucascaDepartments of Clinical Biochemistry, bNeurology, cMolecular Biology, dDermatology, and ePathology, Virgen Macarena University Hospital Saville, Spain fInstituto de Biomedicina de Sevilla (IBiS), Virgen del Rocio University Hospital, CSIC, Sevilla, SpainReceived September 24, 2012Revised November 14, 2012Accepted November 14, 2012CorrespondenceMiguel Lucas, MDDepartment of Molecular Biology, Virgen Macarena University Hospital,Dr. Fedriani S/N, 41009 Seville, SpainTel    +34955008114Fax   +34955008015E-mail    lucas@us.esBackgroundzzLipoid proteinosis (LP) is a rare autosomal recessive disorder characterized by a hoarse voice, variable scarring, and infiltration of the skin and mucosa. This disease is associ-ated with mutations of the gene encoding extracellular matrix protein 1 (ECM1).Case ReportzzThis was a clinical and molecular study of a new case of LP with a severe phe-notype. A 35-year-old female born to nonconsanguineous parents developed dermatological and extracutaneous symptoms in her 9th month of life. The neurological abnormalities of the disease began to appear at the age of 19 years. Computed tomography revealed cranial calcifi-cations.ConclusionszzThe diagnosis of LP was confirmed by histopathological findings and direct se-quencing of ECM1. A new homozygous nonsense mutation was identified in exon 7 of ECM1, c.1076G>A (p.Trp359*). This mutation was not detected in 106 chromosomes of healthy individ-uals with a similar demographic origin. Microsatellite markers around ECM1 were used to con-struct the haplotype in both the parents and the patient. Reports on genotype-phenotype correla-tions in LP point to a milder phenotype in carriers of missense mutations in the Ecm1a isoform, whereas mutations in the Ecm1b isoform are thought to be associated with more severe pheno-types. The present findings in a Spanish patient carrying a truncating mutation in exon 7 revealed complete dermatological and neurological manifestations. J Clin Neurol 2014;10:64-68Key Wordszz ECM1 gene, lipoid proteinosis, mutation, exon 7, phenotype.Open Accesscc  This is an Open Access article distributed under the terms of the Cre-ative Commons Attribution Non-Commercial License (http://creative-commons.org/licenses/by-nc/3.0) which permits unrestricted non-com-mercial use, distribution, and reproduction in any medium, provided the ori-ginal work is properly cited.IntroductionLipoid proteinosis (LP; OMIM 247100), also known as Ur-bach-Wiethe disease, is a rare autosomal recessive disorder characterized by variable scarring and infiltration of the skin and mucosa. Clinical features include warty skin infiltration, papules on the eyelids, and skin scarring, in addition to extra-cutaneous abnormalities such as hoarseness of the voice, epi-lepsy, and neuropsychiatric abnormalities.1 In severe cases this infiltration can lead to respiratory obstruction. Histological ex-aminations reveal the widespread deposition of hyaline mate-rial and disruption of the basement membrane around blood vessels and at the dermal-epidermal junction.The molecular basis of LP has been elucidated: it appears to result from mutations in the gene encoding extracellular ma-trix protein 1 (Ecm1, ECM1; OMIM 602201).2 Ecm1 is a key protein in epidermal differentiation, binding of dermal colla-gens and proteoglycans, and regulation of angiogenesis. Ho-mozygous and compound heterozygous mutations in ECM1 have previously been described in patients with LP. ECM1 maps to chromosome 1q21.2, and there are three known splice variants (Ecm1a, Ecm1b, and Ecm1c) and a putative fourth variant.2,3 Ecm1a is the most widely expressed splice variant, while Ecm1b has a much more restricted expression pattern.4 Ecm1 contains numerous cysteine residues that are arranged in a specific manner. The cysteine-containing do-Mondejar R et al.www.thejcn.com  65mains all have the typical CC-(X7-10)-C arrangement that is capable of the forming protein double loops involved in pro-tein-protein interactions.5 Therefore, Ecm1 and its alternative splicing isoforms may serve as binding and transport proteins in epidermal differentiation.6 Ecm1 was found to negatively regulate endochondral bone formation by inhibiting alkaline phosphatase activity and mineralization.7,8This report describes the case of an LP patient who carries a homozygous, undescribed nucleotide transition in exon 7 of ECM1 causing a homozygous nonsense mutation. Her clini-cal, histological, and molecular features indicate that the trun-cating mutation of exon 7 causes a severe phenotype.Case ReportPatientsThe index patient was a 35-year-old woman born to unrelated parents who developed a progressively hoarse voice from 9 months of age, and vesicular and bullous lesions that appeared after minimal trauma. A physical examination revealed depo-sition of hyaline material in the larynx, epidermolysis bullosa, multiple yellowish warty skin papules on the body, and diffuse acneiform scars over her face, with blisters in the mouth, eyes, and areas subject to friction. Neurological symptoms included unilateral paresthesia, dizziness, and memory loss associated with depression, in addition to a decline in verbal fluency and impaired coordination of movement from the age of 19 years. Computed tomography revealed bilateral and symmetric amyg-daloid-uncal calcifications (Fig. 1A and B). Gradient refo-cused-echo T2*-weighted MRI images (Fig. 1C and D) re-vealed marked hypointense bilateral rounded symmetric lesions in the mesial temporal lobes, involving the amygdaloid complex. A routine EEG (awake and sleep) recording was slightly unstable, but no epileptiform activity was evident. A cognitive event-related potential P-300 wave revealed a reac-tion-time delay during development of the Posner task, with a normal latency of the P3 component during the oddball task. The results of a neurological examination were unremark-Fig. 1. A and B: Axial brain computed tomography image showing bilateral and symmetric calcifications of the mesial temporal lobes (amyg-dala complex, uncinate, hippocampi, and parahippocampal giri). C: Axial brain GRE T2*-weighted MRI image (TR; TE) depicting bilaterally hypointense lesions in both amygdaloid bodies. D: Coronal brain T2*-weighted MRI image showing the same horn-shaped amygdaloid le-sions. E: Homogeneous eosinophilic material was deposited around the sweat coils and capillaries, with the perineurium of a nerve also being affected (hematoxylin and eosin stain, ×200). F: The deposited material stained very strongly with periodic acid Schiff (diastase-resis-tant; ×200).A  DBECFTruncating Mutation of ECM1 in Lipoid Proteinosis66  J Clin Neurol 2014;10:64-68able, and a neuropsychological evaluation revealed a de-crease in information processing speed and disturbances in episodic memory and the amnesic evocation process. These findings could be explained by her depressed mood. The re-sults of a blood workup were unremarkable.A skin biopsy (Fig. 1E and F) of the granuloma annulare revealed sweat glands and small nerves with deposition of strongly periodic-acid-Schiff-positive homogeneous, eosino-philic, hyaline-like material and diastase resistant granules around dermal blood vessels, revealing its glycoproteic nature, which is consistent with LP.Sequencing of the coding region of ECM1Genomic DNA was purified from blood samples using a salt-ing-out procedure, and stored in TE buffer. ECM1 was ampli-fied by a polymerase chain reaction (PCR) with primers span-ning all ten exons and intronic flanking regions. Genomic DNA (100 ng) was amplified in 20-μL reaction volumes con-taining 20 pmol of primers (Table 1), 1.5 nmol of MgCl2, 4 nmol of dNTP, and 1 U of AmpliTaq DNA polymerase (Ap-plied Biosystems, Warrington, UK). The PCR products were separated by 1.5%-agarose-gel electrophoresis and purified with the Qiaquick Gel Extraction Kit (Qiagen, Crawley, UK). Amplified fragments were run and sequenced in an ABI 3130 genetic analyzer.Sequencing of exon 7 revealed the presence of a single base substitution at position 1076 of cDNA (GenBank acces-sion no. NM_004425.3). The c.1076G>A transversion causes a premature termination codon, p.Trp359*, that affects the Ecm1a isoform. The patient was found to be homozygous for the mutation, while her parents were heterozygous carriers (Fig. 2). No other changes or polymorphisms were found in the ECM1 coding region. The mutation causes the loss of a restric-tion target for NlaIII endonuclease, which was therefore used as a screening test. The mutation was not present in 106 chromosomes of unrelated control subjects.Haplotype studyFour different polymorphic dinucleotide microsatellites were analyzed in this study: D1S2344, D1S2345, D1S305, and D1S2624. The primer sequences were obtained from the uniSTS database of the National Center for Biotechnology Information. The sizes of the microsatellites were determined by direct sequencing in the ABI 3130 genetic analyzer.The four markers allowed determination of the segregation phase and the haplotypes associated with the c.1076G>A trans-version. The parents’ haplotypes differed significantly in the mutated chromosomes, although double recombination events cannot be ruled out (Fig. 2).DiscussionLipoid proteinosis was first described in 1929, but the current literature still contains only around 300 published cases. A Spanish patient carrier of a homozygous mutation (c.1076G>A) ECM1 has been described herein. A previous report5 described a different mutation in two Caucasian brothers (c.1077G>A). Nonetheless, the same stop codon, W359X, predicts a truncat-ed protein in both cases. Reports on the genotype-phenotype relationship point to a milder phenotype in carriers of mis-sense mutations in the Ecm1a isoform, whereas mutations in the Ecm1b isoform (i.e., with exon-7 skipping) have been as-sociated with more severe phenotypes.9 This is in agreement with the present finding in a Spanish patient carrying a trun-cating mutation in exon 7 and exhibiting a complete dermato-logical and neurological manifestation. It is difficult to study the genotype-phenotype correlation because of the different ages of patients, since many clinical features vary with age. The patient studied herein reported spontaneous hemorrhagic blisters under both humid and very dry environmental condi-tions, which suggests that both genetic and environmental factors can modify the disease severity. Therefore, genotype-phenotype differences among reports can be at least partially attributed to age and nongenetic factors that differentially af-fect the development of neurologic symptoms and the sever-Table 1. Primers used for sequencing ECM1Exon Forward primer Reverse primerAnnealing temperature (ºC)PCR product size (bp)Exon 1 AGCAGCTGGGACTGAGTCAT TGCTAGTGATGAGCCGTCTG 61 350Exon 2, 3 CCTGACTTGCCCTTCTTCC CTCTTCCCTCCTTTCCACCT 60 347Exon 4, 5 CAGTGACCCTCCAGGTTTCT CAGAGCCCACCGTCTTGTCT 60 484Exon 6 CACTGTTTTCCCCATTCCAG GGCATCAAGAACCCAACCT 60 365Exon 7 CTGATCCTCCCCTCTTGCTC CAGGCAAACAGGCTCTCAG 61 439Exon 8 AGGAGAGAAGGGGCCAAGT TAGGGTCTTTGGGCATCTTC 61 400Exon 9 AGTTGCCTAGTCCTTCCCCA AGGCCAGGTCAGAGTGAAGA 60 408Exon 10 GGCACCCAAGTATCTACATCTG CCAAATCCAAGAGGTGTTTAGTG 61 399PCR: polymerase chain reaction.Mondejar R et al.www.thejcn.com  67ity of this disease.Extracellular matrix protein 1 has specific binding sites for several extracellular matrix proteins and polysaccharides: 1) the NH2-terminal free cysteine domain can bind collagen IV [amino acids (aa) 14-207]; 2) the tandem repeat can bind fib-ulin 1C/1D, matrix metalloproteinase 9 (MMP-9), and lam-inin (aa 207-361); 3) the C-terminal region can interact with domain V of perlecan (aa 424-540); and 4) Ecm1 promotes the link between collagen IV and laminin.6,10-12 Moreover, Sercu et al.12 suggested that Ecm1 can act as a “biological glue” in the skin’s basement membrane to maintain the struc-tural and functional integrity of this organ. If translated, the stop codon described in the present Spanish patient predicts a truncated protein that would impair the interaction with per-lecan, MMP-9, fibulin, and laminin. Given the lack of symp-toms in the carrier parents, haploinsufficiency or toxic effects could be discarded as pathogenic mechanisms. Extracutaneous manifestations such as epilepsy and neuropsychiatric disor-ders13,14 can be related to the inhibition by Ecm1 of MMP-9 ac-tivity,10 a protein that is strongly expressed in the brain.15 The truncated 358 polypeptide lacks regulatory MMP-9 activity and the aforementioned binding domains to several other matrix components, and therefore causes impairment of the extracellular matrix structure. The histological images obtained in this study clearly showed material deposition around sweat coils and capillaries.A new mutation in exon 7 of ECM1 is described herein that leads to a premature termination codon as the cause of a se-vere phenotype of LP. The lack of coincidence in the parents’ haplotypes is noteworthy, although a recombination among the microsatellite markers cannot be ruled out. In conclusion, the identification of pathogenic mutations in ECM1 is significant for genetic counseling with respect to clinical severity and prognosis.Conflicts of InterestThe authors have no financial conflicts of interest.AcknowledgementsThe authors thank the patient and her family for their participation, and the financial support of grants from MICINN (no. SAF2007-60508) and Consejería de Ciencia Junta de Andalucía (no. CVI02790).REFERENCES1. Hamada T. Lipoid proteinosis. Clin Exp Dermatol 2002;27:624-629.Fig. 2. Identification of the c.1076G>A transversion in ECM1 in exon 7. (A) Homozygous mutation in the patient, (B) wild-type sequence, and (C) restriction fragment analysis with NlaIII. The c.1076G>A transversion causes loss of the restriction site. Fragments of digested amplicons of homozygous carriers (-/-), heterozygous carriers (+/-), and the wild-type control (+/+) were separated on a 1.5% agarose gel. The PCR prod-uct was not digested in the homozygous patient, and a single band of 439 bp was detected. MW refers to the 50-bp molecular-weight marker. D: The mutation causes a premature termination codon that predicts a truncated protein. E: Pedigree of the family with LP.MW +/- +/- -/- +/+← 439 bp← 391 bpD1S2344D1S2345D1S305D1S2624D1S2344D1S2345D1S305D1S2624181520181918191718182018191819171818201820182217A  C D EBTruncating Mutation of ECM1 in Lipoid Proteinosis68  J Clin Neurol 2014;10:64-68proteinosis and genotype-phenotype correlation. J Invest Dermatol 2003;120:345-350.10. Fujimoto N, Terlizzi J, Aho S, Brittingham R, Fertala A, Oyama N, et al. Extracellular matrix protein 1 inhibits the activity of matrix metallo-proteinase 9 through high-affinity protein/protein interactions. Exp Der-matol 2006;15:300-307.11. Fujimoto N, Terlizzi J, Brittingham R, Fertala A, McGrath JA, Uitto J. Extracellular matrix protein 1 interacts with the domain III of fibulin-1C and 1D variants through its central tandem repeat 2. Biochem Biophys Res Commun 2005;333:1327-1333.12. Sercu S, Zhang M, Oyama N, Hansen U, Ghalbzouri AE, Jun G, et al. Interaction of extracellular matrix protein 1 with extracellular matrix components: ECM1 is a basement membrane protein of the skin. J In-vest Dermatol 2008;128:1397-1408.13. Sung HJ, Johnson CE, Lessner SM, Magid R, Drury DN, Galis ZS. Matrix metalloproteinase 9 facilitates collagen remodeling and angio-genesis for vascular constructs. Tissue Eng 2005;11:267-276.14. Nagy V, Bozdagi O, Matynia A, Balcerzyk M, Okulski P, Dzwonek J, et al. Matrix metalloproteinase-9 is required for hippocampal late-phase long-term potentiation and memory. J Neurosci 2006;26:1923-1934.15. Szklarczyk A, Lapinska J, Rylski M, McKay RD, Kaczmarek L. Ma-trix metalloproteinase-9 undergoes expression and activation during dendritic remodeling in adult hippocampus. J Neurosci 2002;22:920-930.2. Chan I, Liu L, Hamada T, Sethuraman G, McGrath JA. The molecular basis of lipoid proteinosis: mutations in extracellular matrix protein 1. Exp Dermatol 2007;16:881-890.3. Horev L, Potikha T, Ayalon S, Molho-Pessach V, Ingber A, Gany MA, et al. A novel splice-site mutation in ECM-1 gene in a consanguineous family with lipoid proteinosis. Exp Dermatol 2005;14:891-897.4. Smits P, Ni J, Feng P, Wauters J, Van Hul W, Boutaibi ME, et al. The human extracellular matrix gene 1 (ECM1): genomic structure, cDNA cloning, expression pattern, and chromosomal localization. Genomics 1997;45:487-495.5. Kragh-Hansen U. Structure and ligand binding properties of human serum albumin. Dan Med Bull 1990;37:57-84.6. Smits P, Poumay Y, Karperien M, Tylzanowski P, Wauters J, Huylebroeck D, et al. Differentiation-dependent alternative splicing and expression of the extracellular matrix protein 1 gene in human ke-ratinocytes. J Invest Dermatol 2000;114:718-724.7. Deckers MM, Smits P, Karperien M, Ni J, Tylzanowski P, Feng P, et al. Recombinant human extracellular matrix protein 1 inhibits alkaline phosphatase activity and mineralization of mouse embryonic metatar-sals in vitro. Bone 2001;28:14-20.8. Sekiya I, Vuoristo JT, Larson BL, Prockop DJ. In vitro cartilage forma-tion by human adult stem cells from bone marrow stroma defines the sequence of cellular and molecular events during chondrogenesis. Proc Natl Acad Sci U S A 2002;99:4397-4402.9. Hamada T, Wessagowit V, South AP, Ashton GH, Chan I, Oyama N, et al. Extracellular matrix protein 1 gene (ECM1) mutations in lipoid 

Clinical and molecular study of the extracellular matrix protein 1 gene in a spanish family with lipoid proteinosis

Clinical and molecular study of the extracellular matrix protein 1 gene in a spanish family with lipoid proteinosis

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