BACKGROUND: DNA and mRNA sequencing of the coding regions of the human albumin gene (ALB) and of its intron/exon junctions has revealed twenty-one different molecular defects causing congenital analbuminaemia (CAA). SCOPE OF REVIEW: To describe the mutations in molecular terms and to present the current knowledge about the most important biochemical and clinical effects of CAA. MAJOR CONCLUSIONS: CAA is rare, but its frequency seems to be significantly higher in restricted and minimally admixed populations. The condition affects especially the lipid metabolism but apart from a possible increased risk for atherosclerotic complications, it is generally associated with mild clinical symptoms in adults. By contrast, several reports indicate that analbuminaemic individuals may be at risk during the perinatal and childhood periods, in which they seem to show increased morbidity and mortality. The twenty-one causative defects include seven nonsense mutations, seven changes affecting splicing, five frame-shift/deletions, one frame-shift/insertion and one mutation in the start codon. These results indicate that the trait is an allelic heterogeneous disorder caused by homozygous (nineteen cases) or compound heterozygous (single case) inheritance of defects. Most mutations are unique, but one, named Kayseri, is responsible for about half of the known cases. GENERAL SIGNIFICANCE: Study of the defects in the ALB resulting in CAA allows the identification of "hot spot" regions and contributes to understanding the molecular mechanism underlying the trait. Such studies could also give molecular information about different aspects of ALB regulation and shed light on the regulatory mechanisms involved in the synthesis of the protein. This article is part of a Special Issue entitled Serum Albumin.
BACKGROUND: DNA and mRNA sequencing of the coding regions of the humanalbumin gene (ALB) and of its intron/exon junctions has revealed twenty-one different molecular defects causing congenital analbuminaemia (CAA). SCOPE OF REVIEW: To describe the mutations in molecular terms and to present the current knowledge about the most important biochemical and clinical effects of CAA. MAJOR CONCLUSIONS:CAA is rare, but its frequency seems to be significantly higher in restricted and minimally admixed populations. The condition affects especially the lipid metabolism but apart from a possible increased risk for atherosclerotic complications, it is generally associated with mild clinical symptoms in adults. By contrast, several reports indicate that analbuminaemic individuals may be at risk during the perinatal and childhood periods, in which they seem to show increased morbidity and mortality. The twenty-one causative defects include seven nonsense mutations, seven changes affecting splicing, five frame-shift/deletions, one frame-shift/insertion and one mutation in the start codon. These results indicate that the trait is an allelic heterogeneous disorder caused by homozygous (nineteen cases) or compound heterozygous (single case) inheritance of defects. Most mutations are unique, but one, named Kayseri, is responsible for about half of the known cases. GENERAL SIGNIFICANCE: Study of the defects in the ALB resulting in CAA allows the identification of "hot spot" regions and contributes to understanding the molecular mechanism underlying the trait. Such studies could also give molecular information about different aspects of ALB regulation and shed light on the regulatory mechanisms involved in the synthesis of the protein. This article is part of a Special Issue entitled Serum Albumin.
Authors: George Hindy; Peter Dornbos; Mark D Chaffin; Dajiang J Liu; Minxian Wang; Margaret Sunitha Selvaraj; David Zhang; Joseph Park; Carlos A Aguilar-Salinas; Lucinda Antonacci-Fulton; Diego Ardissino; Donna K Arnett; Stella Aslibekyan; Gil Atzmon; Christie M Ballantyne; Francisco Barajas-Olmos; Nir Barzilai; Lewis C Becker; Lawrence F Bielak; Joshua C Bis; John Blangero; Eric Boerwinkle; Lori L Bonnycastle; Erwin Bottinger; Donald W Bowden; Matthew J Bown; Jennifer A Brody; Jai G Broome; Noël P Burtt; Brian E Cade; Federico Centeno-Cruz; Edmund Chan; Yi-Cheng Chang; Yii-Der I Chen; Ching-Yu Cheng; Won Jung Choi; Rajiv Chowdhury; Cecilia Contreras-Cubas; Emilio J Córdova; Adolfo Correa; L Adrienne Cupples; Joanne E Curran; John Danesh; Paul S de Vries; Ralph A DeFronzo; Harsha Doddapaneni; Ravindranath Duggirala; Susan K Dutcher; Patrick T Ellinor; Leslie S Emery; Jose C Florez; Myriam Fornage; Barry I Freedman; Valentin Fuster; Ma Eugenia Garay-Sevilla; Humberto García-Ortiz; Soren Germer; Richard A Gibbs; Christian Gieger; Benjamin Glaser; Clicerio Gonzalez; Maria Elena Gonzalez-Villalpando; Mariaelisa Graff; Sarah E Graham; Niels Grarup; Leif C Groop; Xiuqing Guo; Namrata Gupta; Sohee Han; Craig L Hanis; Torben Hansen; Jiang He; Nancy L Heard-Costa; Yi-Jen Hung; Mi Yeong Hwang; Marguerite R Irvin; Sergio Islas-Andrade; Gail P Jarvik; Hyun Min Kang; Sharon L R Kardia; Tanika Kelly; Eimear E Kenny; Alyna T Khan; Bong-Jo Kim; Ryan W Kim; Young Jin Kim; Heikki A Koistinen; Charles Kooperberg; Johanna Kuusisto; Soo Heon Kwak; Markku Laakso; Leslie A Lange; Jiwon Lee; Juyoung Lee; Seonwook Lee; Donna M Lehman; Rozenn N Lemaitre; Allan Linneberg; Jianjun Liu; Ruth J F Loos; Steven A Lubitz; Valeriya Lyssenko; Ronald C W Ma; Lisa Warsinger Martin; Angélica Martínez-Hernández; Rasika A Mathias; Stephen T McGarvey; Ruth McPherson; James B Meigs; Thomas Meitinger; Olle Melander; Elvia Mendoza-Caamal; Ginger A Metcalf; Xuenan Mi; Karen L Mohlke; May E Montasser; Jee-Young Moon; Hortensia Moreno-Macías; Alanna C Morrison; Donna M Muzny; Sarah C Nelson; Peter M Nilsson; Jeffrey R O'Connell; Marju Orho-Melander; Lorena Orozco; Colin N A Palmer; Nicholette D Palmer; Cheol Joo Park; Kyong Soo Park; Oluf Pedersen; Juan M Peralta; Patricia A Peyser; Wendy S Post; Michael Preuss; Bruce M Psaty; Qibin Qi; D C Rao; Susan Redline; Alexander P Reiner; Cristina Revilla-Monsalve; Stephen S Rich; Nilesh Samani; Heribert Schunkert; Claudia Schurmann; Daekwan Seo; Jeong-Sun Seo; Xueling Sim; Rob Sladek; Kerrin S Small; Wing Yee So; Adrienne M Stilp; E Shyong Tai; Claudia H T Tam; Kent D Taylor; Yik Ying Teo; Farook Thameem; Brian Tomlinson; Michael Y Tsai; Tiinamaija Tuomi; Jaakko Tuomilehto; Teresa Tusié-Luna; Miriam S Udler; Rob M van Dam; Ramachandran S Vasan; Karine A Viaud Martinez; Fei Fei Wang; Xuzhi Wang; Hugh Watkins; Daniel E Weeks; James G Wilson; Daniel R Witte; Tien-Yin Wong; Lisa R Yanek; Sekar Kathiresan; Daniel J Rader; Jerome I Rotter; Michael Boehnke; Mark I McCarthy; Cristen J Willer; Pradeep Natarajan; Jason A Flannick; Amit V Khera; Gina M Peloso Journal: Am J Hum Genet Date: 2021-12-20 Impact factor: 11.043
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