Molecular defects in human carbamoy phosphate synthetase I: mutational spectrum, diagnostic and protein structure considerations

Häberle, Johannes; Shchelochkov, Oleg A.; Wang, Jing; Katsonis, Panagiotis; Hall, Lynn; Reiss, Sara; Eeds, Angela; Willis, Alecia; Yadav, Meeta; Summar, Samantha R.; Lichtarge, Olivier; Rubio, Vicente; Wong, Lee‐Jun C.; Summar, Marshall

doi:10.1002/humu.21406

Cited by 67 publications

(126 citation statements)

References 71 publications

(121 reference statements)

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“…Interestingly, the UFSD has been found to host missense mutations in CPS1D patients (Fig. 1C,D) with rather high frequency [2], suggesting an important and until now unclear role of this domain.…”

Section: Introductionmentioning

confidence: 99%

“…CPS1D has been associated with a relatively large number of different, generally "private" mutations which occur in single families with very little recurrence [2]. Many of the >130 missense mutations reported in CPS1D remain to be proven responsible for the deficiency.…”

Section: Introductionmentioning

confidence: 99%

“…Primary CPS1 deficiency (CPS1D; MIM #237300), a recessively inherited urea cycle disease leading to frequently fatal hyperammonemia [1,2], is due to mutations in the CPS1 gene. This gene, located in 2q35 [3] and being composed of 38 exons and 37…”

Section: Introductionmentioning

confidence: 99%

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Understanding carbamoyl phosphate synthetase (CPS1) deficiency by using the recombinantly purified human enzyme: Effects of CPS1 mutations that concentrate in a central domain of unknown function

Dı́ez-Fernández

Cervera

et al. 2014

Molecular Genetics and Metabolism

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Carbamoyl phosphate synthetase 1 deficiency (CPS1D) is an inborn error of the urea cycle that is due to mutations in the CPS1 gene. In the first large repertory of mutations found in CPS1D, a small CPS1 domain of unknown function (called the UFSD) was found to host missense changes with high frequency, despite the fact that this domain does not host substrate-binding or catalytic machinery. We investigate here by in vitro expression studies using baculovirus/insect cells the reasons for the prominence of the UFSD in CPS1D, as well as the disease-causing roles and pathogenic mechanisms of the mutations affecting this domain. All but three of the 18 missense changes found thus far mapping in this domain in CPS1D patients drastically decreased the yield of pure CPS1, mainly because of decreased enzyme solubility, strongly suggesting misfolding as a major determinant of the mutations negative effects. In addition, the majority of the mutations also decreased from modestly to very drastically the specific activity of the fraction of the enzyme that remained soluble and that could be purified, apparently because they decreased V max . Substantial although not dramatic increases in K m values for the substrates or for N-acetyl-L-glutamate were observed for only five mutations.Similarly, important thermal stability decreases were observed for three mutations. The results indicate a disease-causing role for all the mutations, due in most cases to the combined effects of the low enzyme level and the decreased activity. Our data strongly support the value of the present expression system for ascertaining the disease-causing potential of CPS1 mutations, provided that the CPS1 yield is monitored. The observed effects of the mutations have been rationalized on the basis of an existing structural model of CPS1. This model shows that the UFSD, which is in the middle of the 1462-residue multidomain CPS1 protein, plays a key integrating role for creating the CPS1 multidomain architecture leading us to propose here a denomination of "Integrating 3 Domain" for this CPS1 region. The majority of these 18 mutations distort the interaction of this domain with other CPS1 domains, in many cases by causing improper folding of structural elements of the Integrating Domain that play key roles in these interactions.

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Section: Introductionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

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Understanding carbamoyl phosphate synthetase (CPS1) deficiency by using the recombinantly purified human enzyme: Effects of CPS1 mutations that concentrate in a central domain of unknown function

Dı́ez-Fernández

Cervera

et al. 2014

Molecular Genetics and Metabolism

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“…Most monogenic disorders only have very rare cases; however, they have variable mutations for single genes. In fact, more than 90% of the known CPS1 mutations are private [14].…”

Section: Gene Therapies For Cps1 Deficiencymentioning

confidence: 99%

Cell and Gene Therapy for Carbamoyl Phosphate Synthetase 1 Deficiency

Zhang¹,

Li²

2017

JPNC

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Carbamoyl phosphate synthetase 1 (CPS1) is the first and rate-limiting enzyme in the urea cycle. CPS1 deficiency is a devastating condition, which is clinically characterized by periodic episodes of life-threatening hyperammonemia. Currently, there is no cure for CPS1 deficiency except for liver transplantation, which is limited by a severe shortage of donors and significant risk of mortality and morbidity. Based on the progress to date, cell-based therapies-including hepatocyte or stem cell transplantation-and new approaches for gene therapy have become the promising curative treatments for CPS1 deficiency. This review outlines the current progress and challenges of cell and gene therapies for CPS1 deficiency.

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“…However, pathological mutations are not always identified [23,24] and even when they are found, they may not provide much prognostic information, especially in the case of heterozygotes of OTC deficiency, the most common urea cycle disorder [25]. This may result in some scenarios where the non-invasive determination of urea cycle function can greatly contribute to clinical management.…”

Section: Stable-isotope Measurement Of Ureagenesis In Patients With Imentioning

confidence: 99%

Stable isotopes in the diagnosis and treatment of inherited hyperammonemia

Tuchman

Mew

2016

J Pediatr Biochem

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Stable isotopes have greatly contributed to our understanding of nitrogen metabolism and the urea cycle. The measurement of urea flux via isotopic methods has traditionally been utilized to determine total body protein synthesis in subjects with an intact urea cycle. However, isotopic studies of nitrogen metabolism are also a useful adjunct to conventional clinical investigations in the diagnosis and management of the inherited hyperammonemias. Such studies offer a safe noninvasive method of measuring the reduction of in vivo hepatic ureagenesis, and thus may provide a more accurate measure of phenotypic severity in affected patients. In addition, isotopic methods are ideally suited to evaluate the efficacy of novel therapies to augment urea production.

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Molecular defects in human carbamoy phosphate synthetase I: mutational spectrum, diagnostic and protein structure considerations

Cited by 67 publications

References 71 publications

Understanding carbamoyl phosphate synthetase (CPS1) deficiency by using the recombinantly purified human enzyme: Effects of CPS1 mutations that concentrate in a central domain of unknown function

Understanding carbamoyl phosphate synthetase (CPS1) deficiency by using the recombinantly purified human enzyme: Effects of CPS1 mutations that concentrate in a central domain of unknown function

Cell and Gene Therapy for Carbamoyl Phosphate Synthetase 1 Deficiency

Stable isotopes in the diagnosis and treatment of inherited hyperammonemia

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