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Article: Neuronal ceroid lipofuscinosis in the South American-Caribbean region: An epidemiological overview.

Guelbert, Guillermo / Venier, Ana Clara / Cismondi, Ines Adriana / Becerra, Adriana / Vazquez, Juan Carlos / Fernández, Elmer Andrés / De Paul, Ana Lucía / Guelbert, Norberto / Noher, Ines / Pesaola, Favio

Frontiers in neurology

2022 Volume 13, Page(s) 920421

Abstract: Neuronal ceroid lipofuscinoses (NCLs) comprise 13 hereditary neurodegenerative pathologies of very low frequency that affect individuals of all ages around the world. All NCLs share a set of symptoms that are similar to other diseases. The exhaustive ... ...

Abstract	Neuronal ceroid lipofuscinoses (NCLs) comprise 13 hereditary neurodegenerative pathologies of very low frequency that affect individuals of all ages around the world. All NCLs share a set of symptoms that are similar to other diseases. The exhaustive collection of data from diverse sources (clinical, genetic, neurology, ophthalmology, etc.) would allow being able in the future to define this group with greater precision for a more efficient diagnostic and therapeutic approach. Despite the large amount of information worldwide, a detailed study of the characteristics of the NCLs in South America and the Caribbean region (SA&C) has not yet been done. Here, we aim to present and analyse the multidisciplinary evidence from all the SA&C with qualitative weighting and biostatistical evaluation of the casuistry. Seventy-one publications from seven countries were reviewed, and data from 261 individuals (including 44 individuals from the Cordoba cohort) were collected. Each NCL disease, as well as phenotypical and genetic data were described and discussed in the whole group. The CLN2, CLN6, and CLN3 disorders are the most frequent in the region. Eighty-seven percent of the individuals were 10 years old or less at the onset of symptoms. Seizures were the most common symptom, both at onset (51%) and throughout the disease course, followed by language (16%), motor (15%), and visual impairments (11%). Although symptoms were similar in all NCLs, some chronological differences could be observed. Sixty DNA variants were described, ranging from single nucleotide variants to large chromosomal deletions. The diagnostic odyssey was probably substantially decreased after medical education activities promoted by the pharmaceutical industry and parent organizations in some SA&C countries. There is a statistical deviation in the data probably due to the approval of the enzyme replacement therapy for CLN2 disease, which has led to a greater interest among the medical community for the early description of this pathology. As a general conclusion, it became clear in this work that the combined bibliographical/retrospective evaluation approach allowed a general overview of the multidisciplinary components and the epidemiological tendencies of NCLs in the SA&C region.
Language	English
Publishing date	2022-08-12
Publishing country	Switzerland
Document type	Journal Article ; Review
ZDB-ID	2564214-5
ISSN	1664-2295
ISSN	1664-2295
DOI	10.3389/fneur.2022.920421
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Article ; Online: “Atypical” Phenotypes of Neuronal Ceroid Lipofuscinosis

Favio Pesaola / Guillermo Guelbert / Ana Clara Venier / Inés Adriana Cismondi / Adriana Becerra / Juan Carlos G. Vazquez / Elmer Fernandez / Ana Lucia De Paul / Norberto Guelbert / Inés Noher

Journal of Inborn Errors of Metabolism and Screening, Vol

The Argentine Experience in the Genomic Era

2021 Volume 9

Abstract: ABSTRACT Neuronal Ceroid Lipofuscinosis (NCL) refers to a group of inherited lysosomal storage disorders characterized by the intracellular accumulation of ceroid-lipofuscin compounds and neurodegeneration. Fourteen genes are currently recognized with ... ...

Abstract	ABSTRACT Neuronal Ceroid Lipofuscinosis (NCL) refers to a group of inherited lysosomal storage disorders characterized by the intracellular accumulation of ceroid-lipofuscin compounds and neurodegeneration. Fourteen genes are currently recognized with disease-causing DNA variants: PPT1/CLN1, TPP1/CLN2, CLN3, DNAJC5/CLN4, CLN5, CLN6, MFSD8/CLN7, CLN8, CTSD/CN10, GRN/CLN11, ATP13A2/CLN12, CTSF/CLN13, KCTD7/CLN14, TBCK/CLN15. In the frame of the Cordoba cohort, we studied N=51 cases. The aim of this paper is the observational and retrospective analysis of the “atypical” phenotypes. PCR-Sanger sequencing and/or massive exome sequencing were used as a screening methodology. One CLN1 subject showed an atypical prolonged (P) phenotype with null PPT1 activity and a heterozygous compound genotype: E5 c.451C>T, p.Arg151*/g.6302T>G (I3 c.363-3T>G). Other 11 CLN2 individuals (except one girl) showed TPP1 activity decreased to around 10% of the minimum value of the reference interval in leukocytes and saliva. The DNA variants E7 c.827A>T, p.Asp276Val and I7 c.887-10A>G were the most prevalent. One CLN8 individual showed an atypical congenital phenotype with a heterozygous combination of DNA variants: E2 c.1A>G, p.?/E3 c.792C>G, p.Asn264Lys. Massive sequencing was installed as a screening methodology for the precision diagnosis of atypical CLN1, CLN2, and CLN8 phenotypes. A genetic/phenotypic local registry is under construction.
Keywords	Neuronal CeroidLipofuscinosis ; Genomics ; CLN1 ; CLN2 ; CLN8 ; Atypical Phenotypes ; Medicine (General) ; R5-920
Subject code	610
Language	English
Publishing date	2021-05-01T00:00:00Z
Publisher	SciELO
Document type	Article ; Online
Database	BASE - Bielefeld Academic Search Engine (life sciences selection)

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Article: The neuronal ceroid lipofuscinoses program: A translational research experience in Argentina.

Kohan, Romina / Pesaola, Favio / Guelbert, Norberto / Pons, Patricia / Oller-Ramírez, Ana María / Rautenberg, Gisela / Becerra, Adriana / Sims, Katherine / Xin, Winnie / Cismondi, Inés Adriana / Noher de Halac, Inés

Biochimica et biophysica acta

2015 Volume 1852, Issue 10 Pt B, Page(s) 2301–2311

Abstract: Background: The Argentinean program was initiated more than a decade ago as the first experience of systematic translational research focused on NCL in Latin America. The aim was to overcome misdiagnoses and underdiagnoses in the region.: Subjects: ... ...

Abstract	Background: The Argentinean program was initiated more than a decade ago as the first experience of systematic translational research focused on NCL in Latin America. The aim was to overcome misdiagnoses and underdiagnoses in the region. Subjects: 216 NCL suspected individuals from 8 different countries and their direct family members. Methods: Clinical assessment, enzyme testing, electron microscopy, and DNA screening. Results and discussion: 1) The study confirmed NCL disease in 122 subjects. Phenotypic studies comprised epileptic seizures and movement disorders, ophthalmology, neurophysiology, image analysis, rating scales, enzyme testing, and electron microscopy, carried out under a consensus algorithm; 2) DNA screening and validation of mutations in genes PPT1 (CLN1), TPP1 (CLN2), CLN3, CLN5, CLN6, MFSD8 (CLN7), and CLN8: characterization of variant types, novel/known mutations and polymorphisms; 3) Progress of the epidemiological picture in Latin America; and 4) NCL-like pathology studies in progress. The Translational Research Program was highly efficient in addressing the misdiagnosis/underdiagnosis in the NCL disorders. The study of "orphan diseases" in a public administrated hospital should be adopted by the health systems, as it positively impacts upon the family's quality of life, the collection of epidemiological data, and triggers research advances. This article is part of a Special Issue entitled: "Current Research on the Neuronal Ceroid Lipofuscinoses (Batten Disease)".
Language	English
Publishing date	2015-10
Publishing country	Netherlands
Document type	Journal Article ; Review
ZDB-ID	60-7
ISSN	1879-2596 ; 1879-260X ; 1872-8006 ; 1879-2642 ; 1879-2618 ; 1879-2650 ; 0006-3002 ; 0005-2728 ; 0005-2736 ; 0304-4165 ; 0167-4838 ; 1388-1981 ; 0167-4889 ; 0167-4781 ; 0304-419X ; 1570-9639 ; 0925-4439 ; 1874-9399
ISSN (online)	1879-2596 ; 1879-260X ; 1872-8006 ; 1879-2642 ; 1879-2618 ; 1879-2650
ISSN	0006-3002 ; 0005-2728 ; 0005-2736 ; 0304-4165 ; 0167-4838 ; 1388-1981 ; 0167-4889 ; 0167-4781 ; 0304-419X ; 1570-9639 ; 0925-4439 ; 1874-9399
DOI	10.1016/j.bbadis.2015.05.003
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Article ; Online: Gene symbol: CLN6. Disease: Neuronal ceroid lipofuscinosis, late infantile.

Cismondi, I Adriana / Kohan, Romina / Ghio, Addy / Ramirez, Ana M Oller / Halac, Inés Noher

Human genetics

2008 Volume 124, Issue 3, Page(s) 323–324

MeSH term(s)	Adolescent ; Argentina ; Biopsy ; Codon/genetics ; Codon, Terminator ; Exons ; Female ; Frameshift Mutation ; Heterozygote ; Humans ; Male ; Membrane Proteins/genetics ; Mutation ; Neuronal Ceroid-Lipofuscinoses/ethnology ; Neuronal Ceroid-Lipofuscinoses/genetics ; Phenotype
Chemical Substances	CLN6 protein, human ; Codon ; Codon, Terminator ; Membrane Proteins
Language	English
Publishing date	2008-10
Publishing country	Germany
Document type	Case Reports ; Journal Article
ZDB-ID	223009-4
ISSN	1432-1203 ; 0340-6717
ISSN (online)	1432-1203
ISSN	0340-6717
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Article ; Online: Gene symbol: CLN6. Disease: Neuronal ceroid lipofuscinosis, late Infantile.

Cismondi, I Adriana / Kohan, Romina / Ghio, Addy / Ramirez, Ana M Oller / Halac, Inés Noher

Human genetics

2008 Volume 124, Issue 3, Page(s) 324

MeSH term(s)	Adolescent ; Amino Acid Substitution ; Argentina ; Biopsy ; Codon/genetics ; Exons ; Female ; Heterozygote ; Humans ; Male ; Membrane Proteins/genetics ; Mutation, Missense ; Neuronal Ceroid-Lipofuscinoses/ethnology ; Neuronal Ceroid-Lipofuscinoses/genetics ; Phenotype ; Point Mutation
Chemical Substances	CLN6 protein, human ; Codon ; Membrane Proteins
Language	English
Publishing date	2008-10
Publishing country	Germany
Document type	Case Reports ; Journal Article
ZDB-ID	223009-4
ISSN	1432-1203 ; 0340-6717
ISSN (online)	1432-1203
ISSN	0340-6717
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Article: Guidelines for incorporating scientific knowledge and practice on rare diseases into higher education: neuronal ceroid lipofuscinoses as a model disorder.

Cismondi, Inés Adriana / Kohan, Romina / Adams, Heather / Bond, Mike / Brown, Rachel / Cooper, Jonathan D / de Hidalgo, Perla K / Holthaus, Sophia-Martha Kleine / Mole, Sara E / Mugnaini, Julia / de Ramirez, Ana María Oller / Pesaola, Favio / Rautenberg, Gisela / Platt, Frances M / Noher de Halac, Inés

Biochimica et biophysica acta

2015 Volume 1852, Issue 10 Pt B, Page(s) 2316–2323

Abstract: This article addresses the educational issues associated with rare diseases (RD) and in particular the Neuronal Ceroid Lipofuscinoses (NCLs, or CLN diseases) in the curricula of Health Sciences and Professional's Training Programs. Our aim is to develop ... ...

Abstract	This article addresses the educational issues associated with rare diseases (RD) and in particular the Neuronal Ceroid Lipofuscinoses (NCLs, or CLN diseases) in the curricula of Health Sciences and Professional's Training Programs. Our aim is to develop guidelines for improving scientific knowledge and practice in higher education and continuous learning programs. Rare diseases (RD) are collectively common in the general population with 1 in 17 people affected by a RD in their lifetime. Inherited defects in genes involved in metabolism are the commonest group of RD with over 8000 known inborn errors of metabolism. The majority of these diseases are neurodegenerative including the NCLs. Any professional training program on NCL must take into account the medical, social and economic burdens related to RDs. To address these challenges and find solutions to them it is necessary that individuals in the government and administrative authorities, academia, teaching hospitals and medical schools, the pharmaceutical industry, investment community and patient advocacy groups all work together to achieve these goals. The logistical issues of including RD lectures in university curricula and in continuing medical education should reflect its complex nature. To evaluate the state of education in the RD field, a summary should be periodically up dated in order to assess the progress achieved in each country that signed up to the international conventions addressing RD issues in society. It is anticipated that auditing current practice will lead to higher standards and provide a framework for those educators involved in establishing RD teaching programs world-wide.
Language	English
Publishing date	2015-10
Publishing country	Netherlands
Document type	Journal Article
ZDB-ID	60-7
ISSN	1879-2596 ; 1879-260X ; 1872-8006 ; 1879-2642 ; 1879-2618 ; 1879-2650 ; 0006-3002 ; 0005-2728 ; 0005-2736 ; 0304-4165 ; 0167-4838 ; 1388-1981 ; 0167-4889 ; 0167-4781 ; 0304-419X ; 1570-9639 ; 0925-4439 ; 1874-9399
ISSN (online)	1879-2596 ; 1879-260X ; 1872-8006 ; 1879-2642 ; 1879-2618 ; 1879-2650
ISSN	0006-3002 ; 0005-2728 ; 0005-2736 ; 0304-4165 ; 0167-4838 ; 1388-1981 ; 0167-4889 ; 0167-4781 ; 0304-419X ; 1570-9639 ; 0925-4439 ; 1874-9399
DOI	10.1016/j.bbadis.2015.06.018
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Article ; Online: Gene symbol: CLN5. Disease: Neuronal Ceroid Lipofuscinosis, Finnish Variant.

Cismondi, I Adriana / Cannelli, Natalia / Aiello, Chiara / Santorelli, Filippo M / Kohan, Romina / Oller Ramírez, Ana M / Halac, Inés Noher

Human genetics

2010 Volume 123, Issue 5, Page(s) 554

MeSH term(s)	Age of Onset ; Frameshift Mutation/genetics ; Gene Deletion ; Genetic Variation/genetics ; Humans ; Infant ; Lysosomal Membrane Proteins ; Membrane Proteins/genetics ; Molecular Sequence Data ; Neuronal Ceroid-Lipofuscinoses/genetics ; Neuronal Ceroid-Lipofuscinoses/pathology
Chemical Substances	CLN5 protein, human ; Lysosomal Membrane Proteins ; Membrane Proteins
Language	English
Publishing date	2010-10-20
Publishing country	Germany
Document type	Journal Article
ZDB-ID	223009-4
ISSN	1432-1203 ; 0340-6717
ISSN (online)	1432-1203
ISSN	0340-6717
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Article ; Online: Gene symbol: CLN5. Disease: Neuronal Ceroid Lipofuscinosis, finnish variant.

Kohan, Romina / Cannelli, Natalia / Aiello, Chiara / Santorelli, Filippo M / Cismondi, Adriana I / Milà, Montserrat / Oller Ramírez, Ana M / Halac, Inés Noher

Human genetics

2010 Volume 123, Issue 5, Page(s) 552

MeSH term(s)	Adolescent ; Age of Onset ; Child ; Female ; Gene Deletion ; Genetic Variation/genetics ; Humans ; Lysosomal Membrane Proteins ; Male ; Membrane Proteins/genetics ; Molecular Sequence Data ; Neuronal Ceroid-Lipofuscinoses/genetics ; Neuronal Ceroid-Lipofuscinoses/pathology
Chemical Substances	CLN5 protein, human ; Lysosomal Membrane Proteins ; Membrane Proteins
Language	English
Publishing date	2010-10-20
Publishing country	Germany
Document type	Journal Article
ZDB-ID	223009-4
ISSN	1432-1203 ; 0340-6717
ISSN (online)	1432-1203
ISSN	0340-6717
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Article ; Online: Gene symbol: TPP1. Disease: Neuronal Ceroid Lipofuscinosis, late infantile.

Kohan, Romina / Muller, Vivien J / Fietz, Michael J / Cismondi, Adriana I / Oller Ramírez, Ana M / Halac, Inés Noher

Human genetics

2010 Volume 123, Issue 5, Page(s) 553

MeSH term(s)	Age of Onset ; Aminopeptidases/genetics ; Codon, Nonsense/genetics ; Dipeptidyl-Peptidases and Tripeptidyl-Peptidases/genetics ; Humans ; Infant ; Molecular Sequence Data ; Mutation, Missense/genetics ; Neuronal Ceroid-Lipofuscinoses/genetics ; Neuronal Ceroid-Lipofuscinoses/pathology ; Serine Proteases/genetics ; Tripeptidyl-Peptidase 1
Chemical Substances	Codon, Nonsense ; Tripeptidyl-Peptidase 1 ; Serine Proteases (EC 3.4.-) ; Aminopeptidases (EC 3.4.11.-) ; Dipeptidyl-Peptidases and Tripeptidyl-Peptidases (EC 3.4.14.-) ; TPP1 protein, human (EC 3.4.14.9)
Language	English
Publishing date	2010-10-08
Publishing country	Germany
Document type	Journal Article
ZDB-ID	223009-4
ISSN	1432-1203 ; 0340-6717
ISSN (online)	1432-1203
ISSN	0340-6717
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Article: Neuronal ceroid lipofuscinosis type CLN2: A new rationale for the construction of phenotypic subgroups based on a survey of 25 cases in South America

Kohan, Romina / Carabelos, María Noelia / Xin, Winnie / Sims, Katherine / Guelbert, Norberto / Cismondi, Inés Adriana / Pons, Patricia / Alonso, Graciela Irene / Troncoso, Mónica / Witting, Scarlet / Pearce, David A / Dodelson de Kremer, Raquel / Oller-Ramírez, Ana María / Noher de Halac, Inés

Gene. 2013 Mar. 1, v. 516, no. 1

2013

Abstract: Tripeptidyl-peptidase 1 (TPP1) null or residual activity occurs in neuronal ceroid lipofuscinosis (NCL) with underlying TPP1/CLN2 mutations. A survey of 25 South American CLN2 affected individuals enabled the differentiation of two phenotypes: classical ... ...

Abstract	Tripeptidyl-peptidase 1 (TPP1) null or residual activity occurs in neuronal ceroid lipofuscinosis (NCL) with underlying TPP1/CLN2 mutations. A survey of 25 South American CLN2 affected individuals enabled the differentiation of two phenotypes: classical late-infantile and variant juvenile, each in approximately 50% of patients, with residual TPP1 activity occurring in approximately 32%. Each individual was assigned to one of three subgroups: (I) n=11, null TPP1 activity in leukocytes; (II) n=8, residual TPP1 activity of 0.60–15.85nmol/h/mg (nr 110–476); (III) n=6, activity not measured in leukocytes. Curvilinear bodies (CB) appeared in almost all studied CLN2 subjects; the only exceptions occurred in cases of subgroup II: two individuals had combined CBs/fingerprints (FPs), and one case had pure FPs. There were 15 mutations (4 first published in this paper, 3 previously observed in South America by our group, and 8 previously observed by others). In subgroup I, mutations were either missense or nonsense; in subgroups II and III, mutations prevailed at the non-conserved intronic site, c.887−10A>G (intron 7), and to a lesser extent at c.89+5G>C (intron 2), in heterozygous combinations. Grouping phenotypically and genetically known individuals on the basis of TPP1 activity supported the concept that residual enzyme activity underlies a protracted disease course. The prevalence of intronic mutations at non-conserved sites in subgroup II individuals indicates that some alternative splicing might allow some residual TPP1 activity.
Keywords	alternative splicing ; disease course ; enzyme activity ; heterozygosity ; introns ; leukocytes ; mutation ; patients ; phenotype ; surveys ; South America
Language	English
Dates of publication	2013-0301
Size	p. 114-121.
Publishing place	Elsevier B.V.
Document type	Article
ZDB-ID	391792-7
ISSN	1879-0038 ; 0378-1119
ISSN (online)	1879-0038
ISSN	0378-1119
DOI	10.1016/j.gene.2012.12.058
Database	NAL-Catalogue (AGRICOLA)

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