Literature DB >> 17257434

Transient trimethylaminuria related to menstruation.

Makiko Shimizu¹, John R Cashman, Hiroshi Yamazaki.

Abstract

BACKGROUND: Trimethylaminuria, or fish odor syndrome, includes a transient or mild malodor caused by an excessive amount of malodorous trimethylamine as a result of body secretions. Herein, we describe data to support the proposal that menses can be an additional factor causing transient trimethylaminuria in self-reported subjects suffering from malodor and even in healthy women harboring functionally active flavin-containing monooxygenase 3 (FMO3).
METHODS: FMO3 metabolic capacity (conversion of trimethylamine to trimethylamine N-oxide) was defined as the urinary ratio of trimethylamine N-oxide to total trimethylamine.
RESULTS: Self-reported Case (A) that was homozygous for inactive Arg500stop FMO3, showed decreased metabolic capacity of FMO3 (i.e., approximately 10% the unaffected metabolic capacity) during 120 days of observation. For Case (B) that was homozygous for common [Glu158Lys; Glu308Gly] FMO3 polymorphisms, metabolic capacity of FMO3 was almost approximately 90%, except for a few days surrounding menstruation showing < 40% metabolic capacity. In comparison, three healthy control subjects that harbored heterozygous polymorphisms for [Glu158Lys; Glu308Gly] FMO3 or homozygous for wild FMO3 showed normal (> 90%) metabolic capacity, however, on days around menstruation the FMO3 metabolic capacity was decreased to ~60-70%.
CONCLUSION: Together, these results indicate that abnormal FMO3 capacity is caused by menstruation particularly in the presence, in homozygous form, of mild genetic variants such as [Glu158Lys; Glu308Gly] that cause a reduced FMO3 function.

Entities: Chemical Disease Gene Species

Mesh：

Substances：

Year: 2007 PMID： 17257434 PMCID： PMC1790885 DOI： 10.1186/1471-2350-8-2

Source DB: PubMed Journal: BMC Med Genet ISSN： 1471-2350 Impact factor: 2.103

Background

Trimethylaminuria, or fish odor syndrome, includes a transient or mild malodor caused by an excessive amount of malodorous trimethylamine as a result of body secretions [1,2]. The causal factor of excessive free trimethylamine is reduced enzyme capacity, or maybe substrate overload. The decreased enzyme capacity to form non-odorous trimethylamine N-oxide could be a result by an inherited deficiency (primary genetic trimethylaminuria) and/or by hormonal modulation or liver damage (transient trimethylaminuria) [2,3]. For trimethylaminuria, at least 40 genetic polymorphisms of the flavin-containing monooxygenase 3 (FMO3) gene have been reported [4,5]. For transient trimethylaminuria, a change of metabolic capacity in one individual around the time of menstruation has been reported [6]. Herein, we describe data to support the proposal that menses can be an additional factor causing transient trimethylaminuria in self-reported subjects suffering from malodor and even in healthy women harboring functionally active FMO3.

Methods

Japanese female volunteers included two subjects suffering self-reported malodor that responded to an Internet article and three healthy laboratory members as controls, ranging from 21 to 37 years of age [5,7]. Written consent was obtained from the individuals for publication of study. FMO3 metabolic capacity (conversion of trimethylamine to trimethylamine N-oxide) was defined as the urinary ratio of trimethylamine N-oxide to total trimethylamine (% of trimethylamine N-oxide/[trimethylamine + trimethylamine N-oxide]) determined by GC [7]. The FMO3 DNA sequence of genomic DNA prepared from peripheral lymphocytes or buccal cells from the study participants was also analyzed [3,5]. The study participants collected their urine samples using a procedure described previously [7]. The ethics committee of Showa Pharmaceutical University approved this study.

Results and discussion

As shown in Figure 1, Case (A) that was homozygous for inactive Arg500stop FMO3 [5], showed decreased metabolic capacity of FMO3 (i.e., 13 ± 10 % (mean ± SD, n = 20) of the unaffected metabolic capacity) during 120 days of observation. For Case (B) that was homozygous for common [Glu158Lys; Glu308Gly] FMO3 polymorphisms [1-3], metabolic capacity of FMO3 was almost ~90%, except for a few days surrounding menstruation. In comparison, healthy control Case (C) that harbored heterozygous polymorphisms for [Glu158Lys; Glu308Gly] FMO3 showed > 90% metabolic capacity and this was greater than the reported unaffected ratio [1,6,7]. However, for Case (C), on days around menstruation the FMO3 metabolic capacity was decreased to ~60–70%. Control Cases (D) and (E) that were homozygous for wild FMO3 also showed normal FMO3 metabolic capacity (i.e., ~> 90%), except for days around menstruation. Together, these results indicate that abnormal FMO3 capacity is caused by menstruation particularly in the presence, in homozygous form, of mild genetic variants such as [Glu158Lys; Glu308Gly] that cause a reduced FMO3 function. This would further suggest that sex hormones play a role in the variable regulation of FMO3. Induced FMO3 activity during pregnancy [8] has been reported, in accordance with the present results.

Figure 1

Decreased metabolic capacity of FMO3 (△), as indicated as percent free trimethylamine (TMA, ●) to total trimethylamine (○) excreted in the urine, in relation to menstruation. Filled boxes indicate the period of menstruation. Total urinary trimethylamine and free trimethylamine concentrations were calculated as mmol trimethylamine (TMA)/mol creatinine. Cases (A) and (B) were self-reported subjects suffering from malodour genotyped for homozygotic inactive Arg500stop FMO3 and homozygotic common [Glu158Lys; Glu308Gly] FMO3, respectively. Cases (C) and (D and E) were control subjects genotyped as heterozygotic for [Glu158Lys; Glu308Gly] FMO3 and homozygotic for wild FMO3, respectively.

Conclusion

Menses can be a factor causing transient trimethylaminuria even in healthy women harboring active enzymes. The present information could be useful in relieving the symptoms for transient and/or mild trimethylaminuria for affected females during menstruation.

Competing interests

The author(s) declare that they have no competing interests.

Authors' contributions

MS undertook genotyping and some analyses. JRC was involved in the supervision of the project and revised the paper. HY undertook planning and most analyses and drafted the paper. All authors read and approved the final manuscript.

Pre-publication history

The pre-publication history for this paper can be accessed here:

8 in total

1. Mild trimethylaminuria caused by common variants in FMO3 gene.

Authors: J Zschocke; D Kohlmueller; E Quak; T Meissner; G F Hoffmann; E Mayatepek
Journal: Lancet Date: 1999-09-04 Impact factor: 79.321

2. Trimethylaminuria: susceptibility of heterozygotes.

Authors: S C Mitchell
Journal: Lancet Date: 1999 Dec 18-25 Impact factor: 79.321

3. Mild trimethylaminuria observed in a Japanese cohort with liver damage.

Authors: Hiroshi Yamazaki; Masaki Fujieda; John R Cashman; Tetsuya Kamataki
Journal: Am J Med Date: 2005-07 Impact factor: 4.965

4. Effect of pregnancy on a measure of FMO3 activity.

Authors: Janne Hukkanen; Delia Dempsey; Peyton Jacob; Neal L Benowitz
Journal: Br J Clin Pharmacol Date: 2005-08 Impact factor: 4.335

5. Exacerbation of symptoms of fish-odour syndrome during menstruation.

Authors: A Q Zhang; S C Mitchell; R L Smith
Journal: Lancet Date: 1996 Dec 21-28 Impact factor: 79.321

6. Stop codon mutations in the flavin-containing monooxygenase 3 (FMO3) gene responsible for trimethylaminuria in a Japanese population.

Authors: Hiroshi Yamazaki; Haruka Fujita; Takaaki Gunji; Jun Zhang; Tetsuya Kamataki; John R Cashman; Makiko Shimizu
Journal: Mol Genet Metab Date: 2006-09-25 Impact factor: 4.797

Review 7. Trimethylaminuria and a human FMO3 mutation database.

Authors: Diana Hernandez; Sarah Addou; David Lee; Christine Orengo; Elizabeth A Shephard; Ian R Phillips
Journal: Hum Mutat Date: 2003-09 Impact factor: 4.878

8. Effects of the dietary supplements, activated charcoal and copper chlorophyllin, on urinary excretion of trimethylamine in Japanese trimethylaminuria patients.

Authors: Hiroshi Yamazaki; Masaki Fujieda; Masahiro Togashi; Tetsuya Saito; George Preti; John R Cashman; Tetsuya Kamataki
Journal: Life Sci Date: 2004-04-16 Impact factor: 5.037

8 in total

21 in total

1. Clinical utility gene card for: trimethylaminuria.

Authors: Elizabeth A Shephard; Eileen P Treacy; Ian R Phillips
Journal: Eur J Hum Genet Date: 2011-11-30 Impact factor: 4.246

2. Relationships between flavin-containing mono-oxygenase 3 (FMO3) genotype and trimethylaminuria phenotype in a Japanese population.

Authors: Makiko Shimizu; Charles K Allerston; Elizabeth A Shephard; Hiroshi Yamazaki; Ian R Phillips
Journal: Br J Clin Pharmacol Date: 2014-05 Impact factor: 4.335

3. Transient massive trimethylaminuria associated with food protein-induced enterocolitis syndrome.

Authors: Natalie B Miller; Avraham Beigelman; Elizabeth Utterson; Marwan Shinawi
Journal: JIMD Rep Date: 2013-07-03

4. Trimethylaminuria: causes and diagnosis of a socially distressing condition.

Authors: Richard J Mackay; Christopher J McEntyre; Caroline Henderson; Michael Lever; Peter M George
Journal: Clin Biochem Rev Date: 2011-02

Review 5. Microbial volatile compounds in health and disease conditions.

Authors: Robin Michael Statham Thorn; John Greenman
Journal: J Breath Res Date: 2012-05-04 Impact factor: 3.262

6. Trimethylamine-N-oxide, a metabolite associated with atherosclerosis, exhibits complex genetic and dietary regulation.

Authors: Brian J Bennett; Thomas Q de Aguiar Vallim; Zeneng Wang; Diana M Shih; Yonghong Meng; Jill Gregory; Hooman Allayee; Richard Lee; Mark Graham; Rosanne Crooke; Peter A Edwards; Stanley L Hazen; Aldons J Lusis
Journal: Cell Metab Date: 2013-01-08 Impact factor: 27.287