Search

Your search keyword '"Makitie, Outi"' showing total 224 results
Start Over Author "Makitie, Outi"
224 results on '"Makitie, Outi"'

1. Nosology of genetic skeletal disorders: 2023 revision.

Author

Unger, Sheila, Ferreira, Carlos, Mortier, Geert, Ali, Houda, Bertola, Débora, Calder, Alistair, Cohn, Daniel, Cormier-Daire, Valerie, Girisha, Katta, Hall, Christine, Makitie, Outi, Mundlos, Stefan, Nishimura, Gen, Robertson, Stephen, Savarirayan, Ravi, Sillence, David, Simon, Marleen, Sutton, V, Warman, Matthew, Superti-Furga, Andrea, and Krakow, Deborah

Abstract

The Nosology of genetic skeletal disorders has undergone its 11th revision and now contains 771 entries associated with 552 genes reflecting advances in molecular delineation of new disorders thanks to advances in DNA sequencing technology. The most significant change as compared to previous versions is the adoption of the dyadic naming system, systematically associating a phenotypic entity with the gene it arises from. We consider this a significant step forward as dyadic naming is more informative and less prone to errors than the traditional use of list numberings and eponyms. Despite the adoption of dyadic naming, efforts have been made to maintain strong ties to the MIM catalog and its historical data. As with the previous versions, the list of disorders and genes in the Nosology may be useful in considering the differential diagnosis in the clinic, directing bioinformatic analysis of next-generation sequencing results, and providing a basis for novel advances in biology and medicine.

Published
2023

5. Demographic and disease-related factors impact bone turnover and vitamin D in children with hemato-oncological diseases

Author

Jackmann, Natalja, Gustafsson, Jan, Utriainen, Pauliina, Magnusson, Per, Harila, Arja, Atanasova, Diana, Rinaldo, Carina, Frisk, Per, Makitie, Outi, Jackmann, Natalja, Gustafsson, Jan, Utriainen, Pauliina, Magnusson, Per, Harila, Arja, Atanasova, Diana, Rinaldo, Carina, Frisk, Per, and Makitie, Outi

Abstract

Children with hemato-oncological diseases may have significant skeletal morbidity, not only during and after treatment but also at the time of diagnosis before cancer treatment. This study was designed to evaluate the vitamin D status and circulating bone metabolic markers and their determinants in children at the time of diagnostic evaluation for hemato-oncological disease. This cross-sectional study included 165 children (91 males, median age 6.9 yr range 0.2-17.7 yr). Of them, 76 patients were diagnosed with extracranial or intracranial solid tumors, 83 with leukemia, and 6 with bone marrow failure. Bone metabolism was assessed by measuring serum 25OHD, PTH, bone alkaline phosphatase, intact N-terminal propeptide of type I procollagen, and C-terminal cross-linked telopeptide of type I collagen. Vitamin D deficiency was found in 30.9% of children. Lower 25OHD levels were associated with older age, lack of vitamin D supplementation, season outside summer, and a country of parental origin located between latitudes -45 degrees and 45 degrees. Children diagnosed with leukemia had lower levels of markers of bone formation and bone resorption than those who had solid tumors or bone marrow failure. In conclusion, vitamin D deficiency was observed in one-third of children with newly diagnosed cancer. Bone turnover markers were decreased in children with leukemia, possibly because of the suppression of osteoblasts and osteoclasts by leukemic cells. The identification of patients with suboptimal vitamin D status and compromised bone remodeling at cancer diagnosis may aid in the development of supportive treatment to reduce the adverse effects of cancer and its treatment., Funding Agencies|Swedish Childhood Cancer Foundation [ST2013-0008, TJ2020-0069, PR2021-0090]; Mary Beves Foundation

Published
2024
Full Text
View/download PDF

9. Truncating mutations in the last exon of NOTCH3 cause lateral meningocele syndrome

Author

Gripp, Karen W, Robbins, Katherine M, Sobreira, Nara L, Witmer, P Dane, Bird, Lynne M, Avela, Kristiina, Makitie, Outi, Alves, Daniela, Hogue, Jacob S, Zackai, Elaine H, Doheny, Kimberly F, Stabley, Deborah L, and Sol‐Church, Katia

Subjects
Biological Sciences, Biomedical and Clinical Sciences, Genetics, Human Genome, Pediatric, Congenital Structural Anomalies, Clinical Research, Rare Diseases, 2.1 Biological and endogenous factors, Aetiology, Congenital, Abnormalities, Multiple, Child, Child, Preschool, DNA Mutational Analysis, Exome, Exons, Facies, High-Throughput Nucleotide Sequencing, Humans, Magnetic Resonance Imaging, Male, Meningocele, Mutation, Phenotype, Receptor, Notch3, Receptors, Notch, Young Adult, NOTCH3, lateral meningocele syndrome, Lehman syndrome, Hajdu-Cheney syndrome, PEST domain, dural ectasia, Clinical Sciences, Clinical sciences
Abstract

Lateral meningocele syndrome (LMS, OMIM%130720), also known as Lehman syndrome, is a very rare skeletal disorder with facial anomalies, hypotonia and meningocele-related neurologic dysfunction. The characteristic lateral meningoceles represent the severe end of the dural ectasia spectrum and are typically most severe in the lower spine. Facial features of LMS include hypertelorism and telecanthus, high arched eyebrows, ptosis, midfacial hypoplasia, micrognathia, high and narrow palate, low-set ears and a hypotonic appearance. Hyperextensibility, hernias and scoliosis reflect a connective tissue abnormality, and aortic dilation, a high-pitched nasal voice, wormian bones and osteolysis may be present. Lateral meningocele syndrome has phenotypic overlap with Hajdu-Cheney syndrome. We performed exome resequencing in five unrelated individuals with LMS and identified heterozygous truncating NOTCH3 mutations. In an additional unrelated individual Sanger sequencing revealed a deleterious variant in the same exon 33. In total, five novel de novo NOTCH3 mutations were identified in six unrelated patients. One had a 26 bp deletion (c.6461_6486del, p.G2154fsTer78), two carried the same single base pair insertion (c.6692_93insC, p.P2231fsTer11), and three individuals had a nonsense point mutation at c.6247A > T (pK2083*), c.6663C > G (p.Y2221*) or c.6732C > A, (p.Y2244*). All mutations cluster into the last coding exon, resulting in premature termination of the protein and truncation of the negative regulatory proline-glutamate-serine-threonine rich PEST domain. Our results suggest that mutant mRNA products escape nonsense mediated decay. The truncated NOTCH3 may cause gain-of-function through decreased clearance of the active intracellular product, resembling NOTCH2 mutations in the clinically related Hajdu-Cheney syndrome and contrasting the NOTCH3 missense mutations causing CADASIL.

Published
2015

11. Real-world non-interventional post-authorization safety study of long-term use of burosumab in children and adolescents with X-linked hypophosphatemia: first interim analysis.

Author

M. Boot, Annemieke, Ariceta, Gema, Beck-Nielsen, Signe Sparre, Brandi, Maria Luisa, Briot, Karine, Collantes, Carmen de Lucas, Giannini, Sandro, Haffner, Dieter, Keen, Richard, Levtchenko, Elena, Mughal, M. Zulf, Makitie, Outi, Nilsson, Ola, Schnabel, Dirk, Tripto-Shkolnik, Liana, Zillikens, M. Carola, Liu, Jonathan, Tudor, Alina, and Emma, Francesco

Published
2024
Full Text
View/download PDF

12. Non-genetic, non-pharmacologic risk factors for osteoporosis: an umbrella review of observational studies

Author

Christou, Maria, primary, Markozannes, Georgios, additional, Christou, Evangelos, additional, Oei, Ling, additional, Tigas, Stelios, additional, Cianferotti, Luisella, additional, Goulis, Dimitrios, additional, Karasik, David, additional, Makitie, Outi, additional, Rivadeneira, Fernando, additional, Kiel, Douglas, additional, and Ntzani, Evangelia, additional

Published
2023
Full Text
View/download PDF

13. Nosology of genetic skeletal disorders: 2023 revision

Author

Genetica Klinische Genetica, Unger, Sheila, Ferreira, Carlos R, Mortier, Geert R, Ali, Houda, Bertola, Débora R, Calder, Alistair, Cohn, Daniel H, Cormier-Daire, Valerie, Girisha, Katta M, Hall, Christine, Krakow, Deborah, Makitie, Outi, Mundlos, Stefan, Nishimura, Gen, Robertson, Stephen P, Savarirayan, Ravi, Sillence, David, Simon, Marleen, Sutton, V Reid, Warman, Matthew L, Superti-Furga, Andrea, Genetica Klinische Genetica, Unger, Sheila, Ferreira, Carlos R, Mortier, Geert R, Ali, Houda, Bertola, Débora R, Calder, Alistair, Cohn, Daniel H, Cormier-Daire, Valerie, Girisha, Katta M, Hall, Christine, Krakow, Deborah, Makitie, Outi, Mundlos, Stefan, Nishimura, Gen, Robertson, Stephen P, Savarirayan, Ravi, Sillence, David, Simon, Marleen, Sutton, V Reid, Warman, Matthew L, and Superti-Furga, Andrea

Published
2023

17. BiallelicKIF24Variants Are Responsible for a Spectrum of Skeletal Disorders Ranging From Lethal Skeletal Ciliopathy to Severe Acromesomelic Dysplasia

Author

Reilly, Madeline Louise, primary, Ain, Noor ul, additional, Muurinen, Mari, additional, Tata, Alice, additional, Huber, Céline, additional, Simon, Marleen, additional, Ishaq, Tayyaba, additional, Shaw, Nick, additional, Rusanen, Salla, additional, Pekkinen, Minna, additional, Högler, Wolfgang, additional, Knapen, Maarten F. C. M., additional, van den Born, Myrthe, additional, Saunier, Sophie, additional, Naz, Sadaf, additional, Cormier‐Daire, Valérie, additional, Benmerah, Alexandre, additional, and Makitie, Outi, additional

Published
2022
Full Text
View/download PDF

19. The human cathelicidin hCAP-18 in serum of children with haemato-oncological diseases

Author

Jackmann, Natalja, Englund, Sofia, Frisk, Per, Makitie, Outi, Utriainen, Pauliina, Mortberg, Anette, Henriques-Normark, Birgitta, Putsep, Katrin, Harila-Saari, Arja H., Jackmann, Natalja, Englund, Sofia, Frisk, Per, Makitie, Outi, Utriainen, Pauliina, Mortberg, Anette, Henriques-Normark, Birgitta, Putsep, Katrin, and Harila-Saari, Arja H.

Abstract

The human cathelicidin hCAP-18 (pro-LL-37) is the pro-protein of the antimicrobial peptide LL-37. hCAP-18 can be produced by many different cell types; bone marrow neutrophil precursors are the main source of hCAP-18 in the circulation. Neutrophil count is used as a marker for myelopoiesis but does not always reflect neutrophil production in the bone marrow, and thus additional markers are needed. In this study, we established the reference interval of serum hCAP-18 level in healthy children and compared serum hCAP-18 levels between different diagnostic groups of children with haemato-oncological diseases, at diagnosis. We found that children with diseases that impair myelopoiesis, such as acute leukaemia, aplastic anaemia, or myelodysplastic syndrome, presented with low hCAP-18 levels, whereas patients with non-haematological malignancies displayed serum hCAP-18 levels in the same range as healthy children. Children with chronic myeloid leukaemia presented with high circulating levels of hCAP-18, probably reflecting the high number of all differentiation stages of myeloid cells. We suggest that analysis of serum hCAP-18 provides additional information regarding myelopoiesis in children with haemato-oncological diseases, which may have future implications in assessment of myelopoiesis in clinical management.

Published
2022
Full Text
View/download PDF

20. Lipocalin-2 is associated with FGF23 in WNT1 and PLS3 osteoporosis

Author

Loid, Petra, Hauta-Alus, Helena, Makitie, Outi, Magnusson, Per, Makitie, Riikka E., Loid, Petra, Hauta-Alus, Helena, Makitie, Outi, Magnusson, Per, and Makitie, Riikka E.

Abstract

BackgroundThe pathogenic mechanisms of early-onset osteoporosis caused by WNT1 and PLS3 mutations are incompletely understood and diagnostic biomarkers of these disorders are limited. Recently, lipocalin-2 has been recognized as an osteokine involved in bone development and homeostasis. However, the role of lipocalin-2 in WNT1 and PLS3 osteoporosis is unknown. ObjectiveWe aimed to investigate if plasma lipocalin-2 could be utilized as a biomarker for WNT1 and PLS3 osteoporosis and to evaluate the association between lipocalin-2 and other parameters of bone metabolism. MethodsWe measured plasma lipocalin-2 in 17 WNT1 and 14 PLS3 mutation-positive patients and compared them to those of 34 mutation-negative (MN) healthy subjects. We investigated possible associations between lipocalin-2 and several bone biomarkers including collagen type I cross-linked C-telopeptide (CTX), alkaline phosphatase (ALP), type I procollagen intact N-terminal propeptide (PINP), intact and C-terminal fibroblast growth factor 23 (FGF23), dickkopf-1 (DKK1) and sclerostin as well as parameters of iron metabolism (iron, transferrin, transferrin saturation, soluble transferrin receptor and ferritin). ResultsWe found no differences in plasma lipocalin-2 levels in WNT1 or PLS3 patients compared with MN subjects. However, lipocalin-2 was associated with C-terminal FGF23 in WNT1 patients (r=0.62; p=0.008) and PLS3 patients (r=0.63, p=0.017), and with intact FGF23 in PLS3 patients (r=0.80; p<0.001). In addition, lipocalin-2 correlated with serum transferrin in WNT1 patients (r=0.72; p=0.001). ConclusionWe conclude that plasma lipocalin-2 is not altered in WNT1 or PLS3 mutation-positive subjects but is associated with FGF23 in abnormal WNT1 or PLS3 signaling and with iron status in abnormal WNT1 signaling., Funding Agencies|University of Helsinki; Helsinki University Hospital through the Doctoral Programme in Clinical Research; Finnish Medical Foundation; Paeivikki and Sakari Sohlberg Foundation; Juho Vainio Foundation; Sigrid Juselius Foundation; Novo Nordisk Foundation; Folkhaelsan Research Foundation; Finnish ORL- HNS Foundation; Region OEstergoetland

Published
2022
Full Text
View/download PDF

21. Early-Onset Osteoporosis

Author

Makitie, Outi, Zillikens, M. Carola, Makitie, Outi, and Zillikens, M. Carola

Abstract

Osteoporosis is a skeletal disorder with enhanced bone fragility, usually affecting the elderly. It is very rare in children and young adults and the definition is not only based on a low BMD (a Z-score < − 2.0 in growing children and a Z-score ≤ − 2.0 or a T-score ≤ − 2.5 in young adults) but also on the occurrence of fragility fractures and/or the existence of underlying chronic diseases or secondary factors such as use of glucocorticoids. In the absence of a known chronic disease, fragility fractures and low BMD should prompt extensive screening for secondary causes, which can be found in up to 90% of cases. When fragility fractures occur in childhood or young adulthood without an evident secondary cause, investigations should explore the possibility of an underlying monogenetic bone disease, where bone fragility is caused by a single variant in a gene that has a major role in the skeleton. Several monogenic forms relate to type I collagen, but other forms also exist. Loss-of-function variants in LRP5 and WNT1 may lead to early-onset osteoporosis. The X-chromosomal osteoporosis caused by PLS3 gene mutations affects especially males. Another recently discovered form relates to disturbed sphingolipid metabolism due to SGMS2 mutations, underscoring the complexity of molecular pathology in monogenic early-onset osteoporosis. Management of young patients consists of treatment of secondary factors, optimizing lifestyle factors including calcium and vitamin D and physical exercise. Treatment with bone-active medication should be discussed on a personalized basis, considering the severity of osteoporosis and underlying disease versus the absence of evidence on anti-fracture efficacy and potential harmful effects in pregnancy.

Published
2022

22. Biallelic KIF24 Variants Are Responsible for a Spectrum of Skeletal Disorders Ranging From Lethal Skeletal Ciliopathy to Severe Acromesomelic Dysplasia

Author

Reilly, Madeline Louise, Ain, Noor ul, Muurinen, Mari, Tata, Alice, Huber, Céline, Simon, Marleen, Ishaq, Tayyaba, Shaw, Nick, Rusanen, Salla, Pekkinen, Minna, Högler, Wolfgang, Knapen, Maarten F.C.M., van den Born, Myrthe, Saunier, Sophie, Naz, Sadaf, Cormier-Daire, Valérie, Benmerah, Alexandre, Makitie, Outi, Reilly, Madeline Louise, Ain, Noor ul, Muurinen, Mari, Tata, Alice, Huber, Céline, Simon, Marleen, Ishaq, Tayyaba, Shaw, Nick, Rusanen, Salla, Pekkinen, Minna, Högler, Wolfgang, Knapen, Maarten F.C.M., van den Born, Myrthe, Saunier, Sophie, Naz, Sadaf, Cormier-Daire, Valérie, Benmerah, Alexandre, and Makitie, Outi

Abstract

Skeletal dysplasias comprise a large spectrum of mostly monogenic disorders affecting bone growth, patterning, and homeostasis, and ranging in severity from lethal to mild phenotypes. This study aimed to underpin the genetic cause of skeletal dysplasia in three unrelated families with variable skeletal manifestations. The six affected individuals from three families had severe short stature with extreme shortening of forelimbs, short long-bones, and metatarsals, and brachydactyly (family 1); mild short stature, platyspondyly, and metaphyseal irregularities (family 2); or a prenatally lethal skeletal dysplasia with kidney features suggestive of a ciliopathy (family 3). Genetic studies by whole genome, whole exome, and ciliome panel sequencing identified in all affected individuals biallelic missense variants in KIF24, which encodes a kinesin family member controlling ciliogenesis. In families 1 and 3, with the more severe phenotype, the affected subjects harbored homozygous variants (c.1457A>G; p.(Ile486Val) and c.1565A>G; p.(Asn522Ser), respectively) in the motor domain which plays a crucial role in KIF24 function. In family 2, compound heterozygous variants (c.1697C>T; p.(Ser566Phe)/c.1811C>T; p.(Thr604Met)) were found C-terminal to the motor domain, in agreement with a genotype–phenotype correlation. In vitro experiments performed on amnioblasts of one affected fetus from family 3 showed that primary cilia assembly was severely impaired, and that cytokinesis was also affected. In conclusion, our study describes novel forms of skeletal dysplasia associated with biallelic variants in KIF24. To our knowledge this is the first report implicating KIF24 variants as the cause of a skeletal dysplasia, thereby extending the genetic heterogeneity and the phenotypic spectrum of rare bone disorders and underscoring the wide range of monogenetic skeletal ciliopathies.

Published
2022

23. Early-Onset Osteoporosis:Rare Monogenic Forms Elucidate the Complexity of Disease Pathogenesis Beyond Type I Collagen

Author

Costantini, Alice, Makitie, Riikka E., Hartmann, Markus A., Fratzl-Zelman, Nadja, Zillikens, M. Carola, Kornak, Uwe, Soe, Kent, Makitie, Outi, Costantini, Alice, Makitie, Riikka E., Hartmann, Markus A., Fratzl-Zelman, Nadja, Zillikens, M. Carola, Kornak, Uwe, Soe, Kent, and Makitie, Outi

Abstract

Early-onset osteoporosis (EOOP), characterized by low bone mineral density (BMD) and fractures, affects children, premenopausal women and men aged

Published
2022

24. Post-authorisation safety study of burosumab use in paediatric, adolescent and adult patients with X-Linked hypophosphataemia:rationale and description

Author

Brandi, Maria Luisa, Ariceta, Gema, Beck-Nielsen, Signe Sparre, Boot, Annemieke M., Briot, Karine, de Lucas Collantes, Carmen, Emma, Francesco, Giannini, Sandro, Haffner, Dieter, Keen, Richard, Levtchenko, Elena, Makitie, Outi, Nilsson, Ola, Schnabel, Dirk, Tripto-Shkolnik, Liana, Zillikens, M. Carola, Liu, Jonathan, Tudor, Alina, Mughal, M. Zulf, Brandi, Maria Luisa, Ariceta, Gema, Beck-Nielsen, Signe Sparre, Boot, Annemieke M., Briot, Karine, de Lucas Collantes, Carmen, Emma, Francesco, Giannini, Sandro, Haffner, Dieter, Keen, Richard, Levtchenko, Elena, Makitie, Outi, Nilsson, Ola, Schnabel, Dirk, Tripto-Shkolnik, Liana, Zillikens, M. Carola, Liu, Jonathan, Tudor, Alina, and Mughal, M. Zulf

Abstract

Background: X-linked hypophosphataemia (XLH) is a rare, inherited, phosphate-wasting disorder that elevates fibroblast growth factor 23 (FGF23), causing renal phosphate-wasting and impaired active vitamin D (1,25(OH) 2D) synthesis. Disease characteristics include rickets, osteomalacia, odontomalacia, and short stature. Historically, treatment has been oral phosphate and 1,25(OH) 2D supplements. However, these treatments do not correct the primary pathogenic mechanism or treat all symptoms and can be associated with adverse effects. Burosumab is a recombinant human immunoglobulin G1 monoclonal antibody against FGF23, approved for treating XLH in several geographical regions, including Europe and Israel. Burosumab restores normal serum phosphate levels, minimising the clinical consequences of XLH. Safety data on long-term treatment with burosumab are lacking owing to the rarity of XLH. This post-authorisation safety study (PASS) aims to evaluate the safety outcomes in patients aged >1 year. Methods: The PASS is a 10-year retrospective and prospective cohort study utilising data from the International XLH Registry (NCT03193476), which includes standard diagnostic and monitoring practice data at participating centres. The PASS aims to evaluate frequency and severity of safety outcomes, frequency and outcomes of pregnancies in female patients, and safety outcomes in patients with mild to moderate kidney disease at baseline, in children, adolescents and adults treated with burosumab for XLH. It is expected that there will be at least 400 patients who will be administered burosumab. Results: Data collection started on 24 April 2019. The expected date of the final study report is 31 December 2028, with two interim reports. Conclusion: This PASS will provide data on the long-term safety of burosumab treatment for XLH patients and describe safety outcomes for patients receiving burosumab contrasted with those patients receiving other XLH treatments

Published
2022

25. Biallelic KIF24 Variants Are Responsible for a Spectrum of Skeletal Disorders Ranging From Lethal Skeletal Ciliopathy to Severe Acromesomelic Dysplasia

Author

Genetica Klinische Genetica, Reilly, Madeline Louise, Ain, Noor Ul, Muurinen, Mari, Tata, Alice, Huber, Céline, Simon, Marleen, Ishaq, Tayyaba, Shaw, Nick, Rusanen, Salla, Pekkinen, Minna, Högler, Wolfgang, Knapen, Maarten F C M, van den Born, Myrthe, Saunier, Sophie, Naz, Sadaf, Cormier-Daire, Valérie, Benmerah, Alexandre, Makitie, Outi, Genetica Klinische Genetica, Reilly, Madeline Louise, Ain, Noor Ul, Muurinen, Mari, Tata, Alice, Huber, Céline, Simon, Marleen, Ishaq, Tayyaba, Shaw, Nick, Rusanen, Salla, Pekkinen, Minna, Högler, Wolfgang, Knapen, Maarten F C M, van den Born, Myrthe, Saunier, Sophie, Naz, Sadaf, Cormier-Daire, Valérie, Benmerah, Alexandre, and Makitie, Outi

Published
2022

27. Contributors

Author

Akikusa, Jonathan, primary, Albani, Salvatore, additional, Allen, Roger, additional, Alsaeid, Khaled, additional, Avčin, Tadej, additional, Babyn, Paul S., additional, Bagga, Arvind, additional, Barron, Karyl S., additional, Becker, Mara L., additional, Benseler, Susanne M., additional, Beukelman, Timothy, additional, Brogan, Paul, additional, Brunner, Hermine I., additional, Burgos-Vargas, Rubèn, additional, Buyon, Jill, additional, Cabral, David A., additional, Choo, Sharon, additional, Cimaz, Rolando, additional, Colbert, Robert Allen, additional, Cole, William G., additional, Davidson, Iris, additional, Benedetti, Fabrizio De, additional, Doria, Andrea S., additional, Dressler, Frank, additional, Duffy, Ciarán M., additional, Eleftheriou, Despina, additional, Feldman, Brian M., additional, Ferguson, Polly J., additional, Fuhlbrigge, Robert, additional, Gattorno, Marco, additional, Grom, Alexei A., additional, Hashkes, Philip J., additional, Houghton, Kristin, additional, Huppertz, Hans-Iko, additional, Ilowite, Norman T., additional, Jaeggi, Edgar, additional, Kastner, Daniel L., additional, Kirton, Adam, additional, Klein-Gitelman, Marisa, additional, Kuchta, Gay, additional, Lane, Jerome Charles, additional, Laxer, Ronald M., additional, LeBlanc, Claire, additional, Leeder, Steven J., additional, Legger, G. Elizabeth, additional, Li, Suzanne C., additional, Lindsley, Carol B., additional, Lovell, Dan, additional, Makitie, Outi, additional, Martini, Alberto, additional, Miller, Frederick W., additional, Morishita, Kimberly, additional, Nigrovic, Peter A., additional, Oen, Kiem G., additional, O'Neil, Kathleen M., additional, Ozen, Seza, additional, Pepmueller, Peri H., additional, Petty, Ross E., additional, Pope, Elena, additional, Prahalad, Sampath, additional, Prakken, Berent, additional, Rapoff, Michael, additional, Rider, Lisa G., additional, Rosé, Carlos Daniel, additional, Rosenbaum, James T., additional, Rosenberg, Alan M., additional, Roth, Johannes, additional, Guillermo, Ricardo Alberto, additional, Schneider, Rayfel, additional, Scott, Christiaan, additional, Sherry, David D., additional, Silverman, Earl, additional, Son, Mary Beth, additional, Sundel, Robert P., additional, Thompson, Susan D., additional, Tiedemann, Karin, additional, Tse, Shirley M.L., additional, Tucker, Lori, additional, Uziel, Yosef, additional, van Montfrans, Joris, additional, Vazques-Mellado, Janitzia, additional, Ward, Leanne, additional, Wedderburn, Lucy R., additional, Wouters, Carine, additional, Wright, James, additional, Wulffraat, Nico M., additional, Zemel, Lawrence, additional, and Zulian, Francesco, additional

Published
2016
Full Text
View/download PDF

28. Pediatric solid organ transplantation and osteoporosis: a descriptive study on bone histomorphometric findings

Author

Tamminen, Inari S., Valta, Helena, Jalanko, Hannu, Salminen, Sari, Mayranpaa, Mervi K., Isaksson, Hanna, Kroger, Heikki, and Makitie, Outi

Subjects
Transplantation of organs, tissues, etc. -- Research -- Health aspects, Osteoporosis -- Research -- Care and treatment -- Complications and side effects, Health
Abstract

Background Organ transplantation may lead to secondary osteoporosis in children. This study characterized bone histomorphometric findings in pediatric solid organ transplant recipients who were assessed for suspected secondary osteoporosis. Methods Iliac crest biopsies were obtained from 19 children (7.6-18.8 years, 11 male) who had undergone kidney (n=6), liver (n=9), or heart (n=4) transplantation a median 4.6 years (range 0.6-16.3 years) earlier. All patients had received oral glucocorticoids at the time of the biopsy. Results Of the 19 patients, 21% had sustained peripheral fractures and 58% vertebral compression fractures. Nine children (47%) had a lumbar spine BMD Z-score below -2.0. Histomorphometric analyses showed low trabecular bone volume (< -1.0 SD) in 6 children (32%) and decreased trabecular thickness in 14 children (74%). Seven children (37%) had high bone turnover at biopsy, and low turnover was found in 6 children (32%), 1 of whom had adynamic bone disease. Conclusions There was a great heterogeneity in the histological findings in different transplant groups, and the results were unpredictable using non-invasive methods. The observed changes in bone quality (i.e. abnormal turnover rate, thin trabeculae) rather than the actual loss of trabecular bone, might explain the increased fracture risk in pediatric solid organ transplant recipients. Keywords Bone histomorphometry * Cancellous bone * Organ transplantation * Fracture * Glucocorticoid treatment * Children, Introduction Solid organ transplantation is an established treatment for children with end-stage renal disease, acute or chronic liver failure, and with terminal heart diseases. While the overall long-term patient survival [...]

Published
2014
Full Text
View/download PDF

29. The 'GEnomics of Musculo Skeletal Traits TranslatiOnal NEtwork' : Origins, Rationale, Organization, and Prospects

Author

Rivadeneira, Fernando, Valjevac, Amina, Teti, Anna, Soldatovic, Ivan, Soe, Kent, Rauner, Martina, Pietsch, Barbara, Ntzani, Evangelia, Makitie, Outi, Ohlsson, Claes, Morgenstern, Milana, Formosa, Melissa, Karasik, David, Ines, Foessl, Brandi, Maria Luisa, Alves, Ines, Alonso, Nerea, Fjorda, Fjorda, Kolev, Mikhail, HUS Children and Adolescents, Clinicum, Lastentautien yksikkö, Children's Hospital, and CAMM - Research Program for Clinical and Molecular Metabolism

Subjects
MUTATIONS, 3121 General medicine, internal medicine and other clinical medicine, translational medical research, collaborative learning, genomics, BONE MASS, personalized medicine, OSTEOPOROSIS, osteoporosis, GENE, PROJECT, DISEASE
Abstract

Musculoskeletal research has been enriched in the past ten years with a great wealth of new discoveries arising from genome wide association studies (GWAS). In addition to the novel factors identified by GWAS, the advent of whole-genome and whole-exome sequencing efforts in family based studies has also identified new genes and pathways. However, the function and the mechanisms by which such genes influence clinical traits remain largely unknown. There is imperative need to bring multidisciplinary expertise together that will allow translating these genomic discoveries into useful clinical applications with the potential of improving patient care. Therefore "GEnomics of MusculoSkeletal traits TranslatiOnal NEtwork" (GEMSTONE) aims to set the ground for the: 1) functional characterization of discovered genes and pathways; 2) understanding of the correspondence between molecular and clinical assessments; and 3) implementation of novel methodological approaches. This research network is funded by The European Cooperation in Science and Technology (COST). GEMSTONE includes six working groups (WG), each with specific objectives: WG1-Study populations and expertise groups: creating, maintaining and updating an inventory of experts and resources (studies and datasets) participating in the network, helping to assemble focus groups defined by phenotype, functional and methodological expertise. WG2-Phenotyping: describe ways to decompose the phenotypes of the different functional studies into meaningful components that will aid the interpretation of identified biological pathways. WG3 Monogenic conditions - human KO models: makes an inventory of genes underlying musculoskeletal monogenic conditions that aids the assignment of genes to GWAS signals and prioritizing GWAS genes as candidates responsible for monogenic presentations, through biological plausibility. WG4 Functional investigations: creating a roadmap of genes and pathways to be prioritized for functional assessment in cell and organism models of the musculoskeletal system. WG5 Bioinformatics seeks the integration of the knowledge derived from the distinct efforts, with particular emphasis on systems biology and artificial intelligence applications. Finally, WG6 Translational outreach: makes a synopsis of the knowledge derived from the distinct efforts, allowing to prioritize factors within biological pathways, use refined disease trait definitions and/or improve study design of future investigations in a potential therapeutic context (e.g. clinical trials) for musculoskeletal diseases.

Published
2021

30. The “GEnomics of Musculo Skeletal Traits TranslatiOnal NEtwork”: Origins, Rationale, Organization, and Prospects

Author

Koromani, Fjorda, primary, Alonso, Nerea, additional, Alves, Ines, additional, Brandi, Maria Luisa, additional, Foessl, Ines, additional, Formosa, Melissa M., additional, Morgenstern, Milana Frenkel, additional, Karasik, David, additional, Kolev, Mikhail, additional, Makitie, Outi, additional, Ntzani, Evangelia, additional, Pietsch, Barbara Obermayer, additional, Ohlsson, Claes, additional, Rauner, Martina, additional, Soe, Kent, additional, Soldatovic, Ivan, additional, Teti, Anna, additional, Valjevac, Amina, additional, and Rivadeneira, Fernando, additional

Published
2021
Full Text
View/download PDF

33. Vitamin D in Head and Neck Cancer : a Systematic Review

Author

Makitie, Antti, Tuokkola, Iida, Laurell, Göran, Makitie, Outi, Olsen, Kerry, Takes, Robert P., Florek, Ewa, Szyfter, Krzysztof, Sier, Cornelis F. M., Ferlito, Alfio, Makitie, Antti, Tuokkola, Iida, Laurell, Göran, Makitie, Outi, Olsen, Kerry, Takes, Robert P., Florek, Ewa, Szyfter, Krzysztof, Sier, Cornelis F. M., and Ferlito, Alfio

Abstract

Purpose of review Observational studies have shown that serum 25-OH vitamin D [25(OH)D] is inversely associated with overall cancer risk in many malignancies. We performed a systematic literature review to determine whether vitamin D deficiency is related to head and neck cancer (HNC) etiology and outcome. Recent findings The search yielded five prospective studies reporting 25(OH)D levels prior to cancer diagnosis and their effect on the risk of HNC. Eight studies were cross-sectional or case-control studies, in which 25(OH)D levels were only measured after cancer diagnosis. Two studies found an inverse association between 25(OH)D level and HNC risk, while two other prospective cohort studies demonstrated no connection between 25(OH)D and HNC risk. Several studies reported cancer patients to have significantly lower 25(OH)D levels than controls. Associations between 25(OH)D and prognosis and mortality were variable. The link between vitamin D and HNC has so far only been investigated in a few observational, prospective, and case-control studies. Vitamin D deficiency may be more common in HNC patients than in the healthy population. There is no evidence for a causal relationship. Further studies are needed to evaluate whether low 25(OH)D concentrations play a role in the development or outcome of HNCs.

Published
2021
Full Text
View/download PDF

34. Prevalence of and factors influencing vitamin D deficiency in paediatric patients diagnosed with cancer at northern latitudes

Author

Jackmann, Natalja, Gustafsson, Jan, Harila-Saari, Arja H., Ljungman, Gustaf, Nezirevic Dernroth, Dzeneta, Frisk, Per, Makitie, Outi, Jackmann, Natalja, Gustafsson, Jan, Harila-Saari, Arja H., Ljungman, Gustaf, Nezirevic Dernroth, Dzeneta, Frisk, Per, and Makitie, Outi

Abstract

Aim To investigate the prevalence of vitamin D deficiency among children with non-haematological malignancies and to explore possible causes of low vitamin D levels among these patients. Methods We performed a cross-sectional study of 458 children diagnosed with solid tumours, brain tumours, non-Hodgkin lymphoma or Hodgkin disease at the University Children's Hospital, Uppsala, Sweden. Serum 25-hydroxyvitamin D and parathyroid hormone levels were measured in samples taken at the time of cancer diagnosis and related to clinical data. Vitamin D deficiency was defined as a 25-hydroxyvitamin D level below 50 nmol/L. Results The prevalence rate of vitamin D deficiency among children with non-haematological malignancies was 41%. There was no association between sex or diagnosis and vitamin D status. Vitamin D deficiency was more common among school children than preschool children (51% vs. 24%). Older age, season outside summer, and a more recent calendar year were significant predictors of lower 25-hydroxyvitamin D. There was a significant, albeit weak, negative correlation between 25-hydroxyvitamin D and parathyroid hormone. Conclusion Vitamin D deficiency is common among children diagnosed with cancer, particularly among school-aged children diagnosed outside summer. The prevalence appears to be increasing, underlining the need for adequate replacement of vitamin D in these patients.

Published
2021
Full Text
View/download PDF

35. The “GEnomics of Musculo Skeletal Traits TranslatiOnal NEtwork”:Origins, Rationale, Organization, and Prospects

Author

Koromani, Fjorda, Alonso, Nerea, Alves, Ines, Brandi, Maria Luisa, Foessl, Ines, Formosa, Melissa M., Morgenstern, Milana Frenkel, Karasik, David, Kolev, Mikhail, Makitie, Outi, Ntzani, Evangelia, Pietsch, Barbara Obermayer, Ohlsson, Claes, Rauner, Martina, Soe, Kent, Soldatovic, Ivan, Teti, Anna, Valjevac, Amina, Rivadeneira, Fernando, Koromani, Fjorda, Alonso, Nerea, Alves, Ines, Brandi, Maria Luisa, Foessl, Ines, Formosa, Melissa M., Morgenstern, Milana Frenkel, Karasik, David, Kolev, Mikhail, Makitie, Outi, Ntzani, Evangelia, Pietsch, Barbara Obermayer, Ohlsson, Claes, Rauner, Martina, Soe, Kent, Soldatovic, Ivan, Teti, Anna, Valjevac, Amina, and Rivadeneira, Fernando

Abstract

Musculoskeletal research has been enriched in the past ten years with a great wealth of new discoveries arising from genome wide association studies (GWAS). In addition to the novel factors identified by GWAS, the advent of whole-genome and whole-exome sequencing efforts in family based studies has also identified new genes and pathways. However, the function and the mechanisms by which such genes influence clinical traits remain largely unknown. There is imperative need to bring multidisciplinary expertise together that will allow translating these genomic discoveries into useful clinical applications with the potential of improving patient care. Therefore “GEnomics of MusculoSkeletal traits TranslatiOnal NEtwork” (GEMSTONE) aims to set the ground for the: 1) functional characterization of discovered genes and pathways; 2) understanding of the correspondence between molecular and clinical assessments; and 3) implementation of novel methodological approaches. This research network is funded by The European Cooperation in Science and Technology (COST). GEMSTONE includes six working groups (WG), each with specific objectives: WG1-Study populations and expertise groups: creating, maintaining and updating an inventory of experts and resources (studies and datasets) participating in the network, helping to assemble focus groups defined by phenotype, functional and methodological expertise. WG2-Phenotyping: describe ways to decompose the phenotypes of the different functional studies into meaningful components that will aid the interpretation of identified biological pathways. WG3 Monogenic conditions - human KO models: makes an inventory of genes underlying musculoskeletal monogenic conditions that aids the assignment of genes to GWAS signals and prioritizing GWAS genes as candidates responsible for monogenic presentations, through biological plausibility. WG4 Functional investigations: creating a roadmap of genes and pathways to be prioritized for functional assessme

Published
2021

36. Glucose regulation in young adults with very low birth weight

Author

Hovi, Petteri, Andersson, Sture, Eriksson, Johan G., Jarvenpaa, Anna-Liisa, Strang-Karlsson, Sonja, Makitie, Outi, and Kajantie, Eero

Subjects
Birth weight, Low -- Complications and side effects, Birth weight, Low -- Research, Glucose intolerance -- Risk factors, Glucose intolerance -- Research, Young adults -- Health aspects, Insulin resistance -- Research, Insulin resistance -- Risk factors
Abstract

Tests on young adults with very low birth weight were performed to determine the association between small size at birth and impaired glucose regulation later in life. Young adults with a very low birth weight were found to have higher indexes of insulin resistance and glucose intolerance and higher blood pressure than those born at term.

Published
2007

37. The international X-linked hypophosphataemia (XLH) registry (NCT03193476) : rationale for and description of an international, observational study

Author

Padidela, Raja, Nilsson, Ola, Makitie, Outi, Beck-Nielsen, Signe, Ariceta Iraola, Gema, Schnabel, Dirk, Brandi, Maria Luisa, Boot, Annemieke, Levtchenko, Elena, Smyth, Michael, Jandhyala, Ravi, Mughal, Zulf, Padidela, Raja, Nilsson, Ola, Makitie, Outi, Beck-Nielsen, Signe, Ariceta Iraola, Gema, Schnabel, Dirk, Brandi, Maria Luisa, Boot, Annemieke, Levtchenko, Elena, Smyth, Michael, Jandhyala, Ravi, and Mughal, Zulf

Abstract

X-linked hypophosphataemia (XLH) is a rare, hereditary, progressive and lifelong phosphate wasting disorder characterised by pathological elevations in fibroblast growth factor (FGF) 23 concentration and activity; XLH has an incidence of approximately 1 in 20-25,000 individuals. Excess FGF23 activity leads to increased phosphate excretion in the kidneys - mediated by downregulation of renal tubular phosphate transporters - and reduced phosphate absorption in the intestines - due to impaired vitamin D activation. This results in impaired bone growth and mineralisation, short and disproportionate stature, leg bowing, musculoskeletal pain, spontaneous dental abscesses, rickets, and osteomalacia. The spectrum of manifestations differs between paediatric and adult patients. Those involved in the treatment of this condition face many challenges, including a lack of robust natural history and demographic data. This multicentre, international, rare-disease patient registry (XLH Registry) was established to address the paucity of data in XLH and to help inform future clinical practice. The XLH Registry collects standard diagnostic and monitoring practice data, including (where applicable) diagnosis and disease progression history, treatment regimens and family history; the protocol does not mandate any interventions or clinical assessments. The XLH Registry aims to recruit 1200 paediatric and adult patients with XLH over 10 years, and several data analyses and peer-reviewed publications are expected to be generated throughout this period. A post-authorisation safety study for Bburosumab, for which the registry Sponsor is the marketing authorisation holder, will be nested as a sub-study within the XLH Registry via a subsequent protocol amendment. The data collected within this rare-disease patient registry will be utilised to synthesise real-world evidence to inform the management of XLH, to improve the quality of life and standard of care of patients living with this rare de

Published
2020

38. Biallelic TMEM251 variants in patients with severe skeletal dysplasia and extreme short stature

Author

Ain, Noor U., Muhammad, Niaz, Dianatpour, Mehdi, Baroncelli, Marta, Iqbal, Muddassar, Fard, Mohammad A. F., Bukhari, Ihtisham, Ahmed, Sufian, Hajipour, Massoumeh, Tabatabaie, Zahra, Foroutan, Hamidreza, Nilsson, Ola, Faghihi, Mohammad A., Makitie, Outi, Naz, Sadaf, Ain, Noor U., Muhammad, Niaz, Dianatpour, Mehdi, Baroncelli, Marta, Iqbal, Muddassar, Fard, Mohammad A. F., Bukhari, Ihtisham, Ahmed, Sufian, Hajipour, Massoumeh, Tabatabaie, Zahra, Foroutan, Hamidreza, Nilsson, Ola, Faghihi, Mohammad A., Makitie, Outi, and Naz, Sadaf

Abstract

Skeletal dysplasias are a heterogeneous group of disorders ranging from mild to lethal skeletal defects. We investigated two unrelated families with individuals presenting with a severe skeletal disorder. In family NMD02, affected individuals had a dysostosis multiplex-like skeletal dysplasia and severe short stature (<-8.5 SD). They manifested increasingly coarse facial features, protruding abdomens, and progressive skeletal changes, reminiscent of mucopolysaccharidosis. The patients gradually lost mobility and the two oldest affected individuals died in their twenties. The affected child in family ID01 had coarse facial features and severe skeletal dysplasia with clinical features similar to mucopolysaccharidosis. She had short stature, craniosynostosis, kyphoscoliosis, and hip-joint subluxation. She died at the age of 5 years. Whole-exome sequencing identified two homozygous variants c.133C>T; p.(Arg45Trp) and c.215dupA; p.(Tyr72Ter), respectively, in the two families, affecting an evolutionary conserved gene TMEM251 (NM_001098621.1). Immunofluorescence and confocal studies using human osteosarcoma cells indicated that TMEM251 is localized to the Golgi complex. However, p.Arg45Trp mutant TMEM251 protein was targeted less efficiently and the localization was punctate. Tmem251 knockdown by small interfering RNA induced dedifferentiation of rat primary chondrocytes. Our work implicates TMEM251 in the pathogenesis of a novel disorder and suggests its potential function in chondrocyte differentiation., Funding Agencies:National Institute for Medical Research Development 940714Higher Eductation Comission Pakistan Koshish Foundation, USA Sigrid Juselius Foundation

Published
2020
Full Text
View/download PDF

39. Biomarkers in WNT1 and PLS3 Osteoporosis: Altered Concentrations of DKK1 and FGF23

Author

Makitie, Riikka E., Kampe, Anders, Costantini, Alice, Alm, Jessica J., Magnusson, Per, Makitie, Outi, Makitie, Riikka E., Kampe, Anders, Costantini, Alice, Alm, Jessica J., Magnusson, Per, and Makitie, Outi

Abstract

Recent advancements in genetic research have uncovered new forms of monogenic osteoporosis, expanding our understanding of the molecular pathways regulating bone health. Despite active research, knowledge on the pathomechanisms, disease-specific biomarkers, and optimal treatment in these disorders is still limited. Mutations in WNT1, encoding a WNT/beta-catenin pathway ligand WNT1, and PLS3, encoding X chromosomally inherited plastin 3 (PLS3), both result in early-onset osteoporosis with prevalent fractures and disrupted bone metabolism. However, despite marked skeletal pathology, conventional bone markers are usually normal in both diseases. Our study aimed to identify novel bone markers in PLS3 and WNT1 osteoporosis that could offer diagnostic potential and shed light on the mechanisms behind these skeletal pathologies. We measured several parameters of bone metabolism, including serum dickkopf-1 (DKK1), sclerostin, and intact and C-terminal fibroblast growth factor 23 (FGF23) concentrations in 17 WNT1 and 14 PLS3 mutation-positive subjects. Findings were compared with 34 healthy mutation-negative subjects from the same families. Results confirmed normal concentrations of conventional metabolic bone markers in both groups. DKK1 concentrations were significantly elevated in PLS3 mutation-positive subjects compared with WNT1 mutation-positive subjects (p amp;lt; .001) or the mutation-negative subjects (p = .002). Similar differences were not seen in WNT1 subjects. Sclerostin concentrations did not differ between any groups. Both intact and C-terminal FGF23 were significantly elevated in WNT1 mutation-positive subjects (p = .039 and p = .027, respectively) and normal in PLS3 subjects. Our results indicate a link between PLS3 and DKK1 and WNT1 and FGF23 in bone metabolism. The normal sclerostin and DKK1 levels in patients with impaired WNT signaling suggest another parallel regulatory mechanism. These findings provide novel information on the molecular networks in bon, Funding Agencies|Sigrid Juselius FoundationSigrid Juselius Foundation; Folkhalsan Research Foundation; Academy of FinlandAcademy of Finland; Foundation for Pediatric Research; Helsinki University Research Funds; Swedish Research CouncilSwedish Research Council; Novo Nordisk FoundationNovo Nordisk Foundation; Swedish Childhood Cancer Foundation; Stockholm County Council (ALF project)Stockholm County Council; ALF grants from Region Ostergotland; Finnish Cultural Foundation through the Foundations post-doctorate pool; HRH Crown Princess Lovisas Foundation; Helsinki University Hospital through the Doctoral Programme in Clinical Research; Finnish Medical Foundation; Paivikki and Sakari Sohlberg Foundation; Helsinki University; Finnish Norwegian Research Foundation; Orion Research Foundation; Finnish Otolaryngology-Head and Neck Surgery (ORL-HNS) Foundation

Published
2020
Full Text
View/download PDF

40. Vitamin D status in children with leukemia, its predictors, and association with outcome

Author

Jackmann, Natalja, Makitie, Outi, Harila-Saari, Arja, Gustafsson, Jan, Nezirevic Dernroth, Dzeneta, Frisk, Per, Jackmann, Natalja, Makitie, Outi, Harila-Saari, Arja, Gustafsson, Jan, Nezirevic Dernroth, Dzeneta, and Frisk, Per

Abstract

Background Children and adolescents with leukemia are potentially at high risk of vitamin D inadequacy, which may have clinical relevance for skeletal morbidity, infections, and cancer outcome. This study aimed to evaluate vitamin D status at the time of diagnosis to investigate its predictors and association with overall survival in children with leukemia. Procedure We included all 295 children and adolescents diagnosed with leukemia at our institution between 1990 and 2016 who had available serum sample from the time of diagnosis. We analyzed serum 25-hydroxyvitamin D and parathyroid hormone levels and correlated them with clinical data. Results The 25-hydroxyvitamin D level was deficient (amp;lt; 25 nmol/L), insufficient (25-50 nmol/L), sufficient (50-75 nmol/L), and optimal (amp;gt; 75 nmol/L) in 6.4%, 26.8%, 39.7%, and 27.1% of the children, respectively. Older age and a more recent time of sampling (calendar year) predicted lower 25-hydroxyvitamin D level. In preschool children (age amp;lt;= 6 years), lower 25-hydroxyvitamin D level was also associated with acute myeloid leukemia, and a 25-hydroxyvitamin D level amp;lt; 50 nmol/L was associated with inferior overall survival. In school-aged children (age amp;gt; 6 years), the 25-hydroxyvitamin D level showed significant seasonal variation. Conclusion It remains unclear whether vitamin D supplementation in pediatric leukemia patients will improve outcome., Funding Agencies|Swedish Childhood Cancer Foundation [ST2013-0008, TJ2014-0007]; Uppsala University Hospital Research Fund

Published
2020
Full Text
View/download PDF

43. Mutations in the RNA component of RNase MRP cause a pleiotropic human disease, cartilage-hair hypoplasia

Author

Ridanpaa, Maaret, Eenennaam, Hans van, Pelin, Katarina, Chadwick, Robert, Johnson, Cheryl, Yuan, Bo, VanVenrooij, Walther, Pruijn, Ger, Salmela, Riika, Rockas, Susanna, Makitie, Outi, Kaitila, Ilkka, and Chapelle, Albert de la

Subjects
Cell research -- Analysis, RNA -- Genetic aspects, Cartilage -- Genetic aspects, Gene mutations -- Physiological aspects, Biological sciences
Abstract

Research has been conducted on the cartilage-hair hypoplasia, an inherited developmental disorder with the predesposition to cancer. The results of the several mutations carried in the untranslated RMRP gene which cosegragate with this disorder are described.

Published
2001

45. Biallelic TMEM251 variants in patients with severe skeletal dysplasia and extreme short stature

Author

Ain, Noor U., primary, Muhammad, Niaz, additional, Dianatpour, Mehdi, additional, Baroncelli, Marta, additional, Iqbal, Muddassar, additional, Fard, Mohammad A. F., additional, Bukhari, Ihtisham, additional, Ahmed, Sufian, additional, Hajipour, Massoumeh, additional, Tabatabaie, Zahra, additional, Foroutan, Hamidreza, additional, Nilsson, Ola, additional, Faghihi, Mohammad A., additional, Makitie, Outi, additional, and Naz, Sadaf, additional

Published
2020
Full Text
View/download PDF

47. The international X-linked hypophosphataemia (XLH) registry (NCT03193476): rationale for and description of an international, observational study

Author

Padidela, Raja, primary, Nilsson, Ola, additional, Makitie, Outi, additional, Beck-Nielsen, Signe, additional, Ariceta, Gema, additional, Schnabel, Dirk, additional, Brandi, Maria Luisa, additional, Boot, Annemieke, additional, Levtchenko, Elena, additional, Smyth, Michael, additional, Jandhyala, Ravi, additional, and Mughal, Zulf, additional

Published
2020
Full Text
View/download PDF

48. Biallelic TMEM251 variants in patients with severe skeletal dysplasia and extreme short stature

Author

Ain, Noor, primary, Muhammad, Niaz, additional, Dianatpour, Mehdi, additional, Baroncelli, Marta, additional, Iqbal, Muddassar, additional, Farazifard, Mohammad A, additional, Bukhari, Ihtisham, additional, Ahmed, Sufian, additional, Hajipour, Massoumeh, additional, Tabatabaie, Zahra, additional, Foroutan, Hamidreza, additional, Nilsson, Ola, additional, Faghihi, Mohammad Ali, additional, Makitie, Outi, additional, and Naz, Sadaf, additional

Published
2020
Full Text
View/download PDF

Catalog

Books, media, physical & digital resources
See catalog results