Human choriogonadotrophin protein core and sugar branches heterogeneity: basic and clinical insights

doi:10.1093/humupd/dmn036

Human Reproduction Update Advance Access originally published online on October 22, 2008
Human Reproduction Update 2009 15(1):69-95; doi:10.1093/humupd/dmn036

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© The Author 2008. Published by Oxford University Press on behalf of the European Society of Human Reproduction and Embryology. All rights reserved. For Permissions, please email: journals.permissions@oxfordjournals.org

Human choriogonadotrophin protein core and sugar branches heterogeneity: basic and clinical insights

S.F. de Medeiros¹^,2^,5 and R.J. Norman³^,4

¹ Department of Gynaecology and Obstetrics, Faculty of Medical Sciences, Federal University of Mato Grosso, Rua Marechal Deodoro, 1055, Apto. 1302, 78005-101 Cuiabá, Mato Grosso, Brazil ² Tropical Institute of Reproductive Medicine and Menopause, Cuiabá, Mato Grosso, Brazil ³ Reproductive Medicine at The Queen Elizabeth Hospital, Discipline of Obstetrics and Gynaecology, University of Adelaide, South Australia, Australia ⁴ Research Centre for Reproductive Medicine, Adelaide, South Australia, Australia

⁵ Correspondence address. Tel: +55-65-3322-7342; Fax: +55-65-3623-0079; E-mail: de.medeiros{at}terra.com.br

BACKGROUND: Human chorionic gonadotrophin (hCG) is measured in serum andurine for the early detection of ectopic pregnancy, patientswith higher risk of miscarriage, embryos or fetuses with chromosomeabnormalities, prediction of pre-eclampsia or fetal growth restrictionand identification or follow-up of trophoblast neoplasia. Thisreview examines basic knowledge on the heterogeneity of hCGprotein core and sugar branches and its relevance to assaysused in a clinical setting.

METHODS: The databases Scielo and Medline/Pubmed were consulted for identificationof the most relevant published papers. Search terms were gonadotrophin,glycoprotein structure, hCG structure and molecular forms ofhCG.

RESULTS: The synthesis of alpha (hCG ${alpha}$ ) and beta (hCGβ) peptide chainsand their further glycosylation involve the complex action ofdifferent enzymes. After assembly, hCG reaches the cell surfaceand is secreted as a bioactive heterodimer. The complex cascadeof enzymes acting in hCG secretion results in heterogeneousmolecular forms. The hCG molecules are differently metabolizedby the liver, ovary and kidney, but the majority of hCG formsare excreted in the urine. Intact hCG, hCG ${alpha}$ , hCGβ, hyperglycosylated(hCGh), nicked (hCGn) and core fragment of hCGβ (hCGβcf)forms have relevant clinical use. The immunogenicity of eachhCG variant, their epitopes distribution and the available antibodiesare important for the development of specific assays. Dependingon the prevalent form or proportion in relation to the intacthCG, the choice of assay for measurement of a specific moleculein a particular clinical setting is paramount.

CONCLUSIONS: Measurement of hCG and/or its related molecules is useful inclinical practice, but greater awareness is needed worldwideregarding the use of new sensitive and specific assays tailoredfor different clinical applications.

Key words: human choriogonadotrophin / heterogeneity / structure / application

Received on May 7, 2007; revised April 18, 2008; accepted on July 14, 2008

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