Next Article in Journal
Post-COVID-19 Spondylodiscitis: A Case Study and Review of the Literature
Previous Article in Journal
The Survival Outcomes of Patients Requiring Prolonged Mechanical Ventilation
 
 
Font Type:
Arial Georgia Verdana
Font Size:
Aa Aa Aa
Line Spacing:
Column Width:
Background:
Case Report

Hereditary Congenital Methemoglobinemia Diagnosed at the Age of 79 Years: A Case Report

1
Department of Cardiology, Urasoe General Hospital, Urasoe 901-2132, Japan
2
Department of Internal Medicine, Naha City Hospital, Naha 902-8511, Japan
3
Division of Genomics, Medical Institute of Bioregulation, Kyushu University, Fukuoka 812-8582, Japan
4
Division of Community Medicine and Career Development, Kobe University Graduate School of Medicine, Kobe 652-0032, Japan
*
Author to whom correspondence should be addressed.
Medicina 2023, 59(3), 615; https://doi.org/10.3390/medicina59030615
Submission received: 20 February 2023 / Revised: 14 March 2023 / Accepted: 17 March 2023 / Published: 20 March 2023

Abstract

:
Background: Cardiopulmonary disorders are the most common cause of central cyanosis, and methemoglobinemia is often overlooked in the differential diagnosis of patients with central cyanosis. In most cases, methemoglobinemia is acquired and hereditary congenital methemoglobinemia is rare. Only a few case reports of congenital methemoglobinemia can be found in PubMed. To date, only four cases of congenital methemoglobinemia diagnosed after the age of 50 years have been reported. Case Presentation: A 79-year-old Japanese woman presented at our hospital with the chief complaints of dyspnea and cyanosis. She exhibited cyanosis of the lips and extremities, and her SpO2 was 80%, with oxygen administration at 5 L/min. Blood gas analysis revealed a PaO2 of 325.4 mmHg and methemoglobin level of 36.9%. The SpO2 and PaO2 values were dissociated, and methemoglobin levels were markedly elevated. Genetic analysis revealed a nonsynonymous variant in the gene encoding nicotinamide adenine dinucleotide cytochrome (NADH) B5 reductase 3 (CYB5R3), and the patient was diagnosed with congenital methemoglobinemia. Conclusions: It is important to consider methemoglobinemia in the differential diagnosis of patients with central cyanosis. At 79 years of age, our patient represents the oldest patient with this diagnosis. This report indicates that it is crucial to consider the possibility of methemoglobinemia regardless of the patient’s age.

1. Introduction

Methemoglobinemia is a disease that can cause cyanosis and shortness of breath. Pulse oximeters generally rely on data from healthy individuals with low levels of carboxyhemoglobin and methemoglobin. Hence, pulse oximeter signals may be invalid in patients with underlying conditions. Dissociation between SpO2 and PaO2 values may aid in the diagnosis of methemoglobinemia. Methemoglobinemia can be either congenital or acquired, and the most common cause of congenital methemoglobinemia is functional variants in the gene encoding NADH-cytochrome B5 reductase 3 (CYB5R3). Methemoglobin is a form of the protein hemoglobin in which the iron is in the ferric state, rather than the normal ferrous state. Although a small percentage of methemoglobin is present in healthy individuals, an increase in methemoglobin content occurs due to loss of function of CYB5R3. Methemoglobinemia is caused by functional variants of CYB5R3 transmitted in an autosomal recessive manner. Herein, we present a case of congenital methemoglobinemia diagnosed at the age of 79 years; this may be the oldest patient with this diagnosis reported to date.

2. Case Report

2.1. Case Presentation

A 79-year-old Japanese woman presented to our hospital with the chief complaints of dyspnea and cyanosis. She had a history of pulmonary tuberculosis, lung cancer (following partial right lobe resection and radiotherapy), and bronchiectasis. In addition, the patient had undergone home oxygen therapy 6 months prior due to chronic respiratory failure. Two hours before arriving at our hospital, the patient reported dyspnea and her usual oxygen dosage of 2 L/min was increased to 5 L/min. Nonetheless, her dyspnea did not improve, and her SpO2 decreased to as low as 80%. This prompted her to seek emergency care at our hospital.

2.2. Investigation

At the time of examination, the patient’s vital signs were as follows: blood pressure, 134/62 mmHg; pulse, 60 beats per minute; respiratory rate, 23 breaths per minute, SpO2, 80% (while receiving 5 L/min of oxygen via a mask); and body temperature, 37.3 °C. Physical examination revealed cyanosis of the lips and extremities, and auscultation revealed diminished breath sounds (but no wheezes or crackles). Chest radiography revealed no infiltrative shadows.

2.3. Differential Diagnosis

Despite the absence of infiltrative shadows on chest radiography, the patient was admitted to our hospital with a diagnosis of acute bronchitis based on her history of bronchiectasis and the presence of low-grade fever and purulent sputum. Gram staining of the sputum revealed the presence of Gram-negative bacilli. Because Pseudomonas aeruginosa had been detected previously in sputum culture tests, antimicrobial therapy with ceftazidime (1 g administered every 12 h) was initiated. Despite the administration of oxygen, the patient’s SpO2 remained low. Therefore, we initiated noninvasive positive pressure ventilation, which also did not improve the SpO2 value. Arterial blood gas analysis revealed a high PaO2 (325.4 mmHg)—indicating a marked discrepancy with the SpO2 of 80%—and elevated methemoglobin (36.9%; Table 1). Based on these findings, the patient was diagnosed with methemoglobinemia.

2.4. Genetic Analysis

Genetic testing was performed since the chronic elevation of methemoglobin levels strongly suggested the possibility of congenital methemoglobinemia. We extracted genomic DNA from the patient with approval from the Ethics Committee of the School of Medicine, Kyushu University (#680-01). Since CYB5R3 is known to be the most common responsible gene in congenital methemoglobinemia, we examined all exons of CYB5R3 using Sanger sequencing. We observed a rare homozygous nonsynonymous variant in exon 3 (NM_000398.7:c.173G>A [p.Arg58Gln], rs121965007; Figure 1) [1]. The nucleotide variant has a CADD score of 27.5 (https://cadd.gs.washington.edu, accessed on 31 January 2023) and has been previously reported as a causative variant in only three Japanese patients with methemoglobinemia [2]. We did not observe any other sequence variants in the other eight exons examined in CYB5R3. The resulting amino acid substitution, Arg58Gln, was predicted to be probably damaging by PolyPhen2 (http://genetics.bwh.harvard.edu/pph2/, accessed on 31 January 2023) and damaging by SIFT (https://sift.bii.a-star.edu.sg, accessed on 31 January 2023) software. Since the variant is located in the flavin adenine dinucleotide (FAD)-binding domain, it is likely to affect binding affinity to FAD, resulting in the reduced efficiency of electron transfer (Figure 2) [3,4].

3. Outcome and Follow-Up

Following the diagnosis of methemoglobinemia and administration of 8 mL methylene blue (0.2 mL/kg), the SpO2 increased to 99% within approximately 10 min (Figure 3 and Figure 4), with resolution of cyanosis (Figure 5). The color of the blood samples changed from dark red to red (Figure 6), and the methemoglobin level decreased to 2.0%. The patient had previously visited our hospital, and a review of her medical records revealed that her methemoglobin level had been elevated for some time (10% and 20% at 5 and 2 years prior to the latest visit, respectively). Although we considered the possibility of acquired methemoglobinemia, there was no history of drug use that would potentially induce methemoglobinemia. Genetic testing revealed congenital methemoglobinemia. After starting ascorbic acid therapy (750 mg/day), the methemoglobin level remained in the range of 6–8% and SpO2 remained above 90%, allowing for the discontinuation of home oxygen therapy. In this instance, the presence of Pseudomonas aeruginosa was confirmed through sputum culture, and the patient received a 5-day regimen of ceftazidime.

4. Discussion

4.1. First and Second Novelty

Cardiopulmonary diseases are the most common cause of central cyanosis, and methemoglobinemia is often overlooked in the differential diagnosis [5]. However, methemoglobinemia should definitely be considered when there is a discrepancy between SpO2 and PaO2 values [5,6]. To the best of our knowledge, only four cases of congenital methemoglobinemia diagnosed after the age of 50 years have been reported to date [5,6,7,8,9]. As such, our patient is the oldest person (79 years old) in whom the diagnosis of congenital methemoglobinemia has been made.

4.2. Significance of the First and Second Novelty

Central cyanosis is induced by hypoxemia and is commonly caused by cardiopulmonary diseases. The specific causes of central cyanosis include right–left shunting (leading to atrial septal defects, transposition of the great arteries, tetralogy of Fallot, or pneumonia) and mismatched ventilation and blood flow (leading to bronchial asthma, emphysema, atelectasis, or pulmonary edema) [10]. However, methemoglobinemia is often overlooked in the differential diagnosis of patients with central cyanosis [5]. Our patient had a history of pulmonary tuberculosis, lung cancer, and bronchiectasis and had been on home oxygen therapy for 6 months. Therefore, the cause of cyanosis was initially thought to be pulmonary disease. However, the SpO2 did not increase, and cyanosis did not improve with noninvasive positive pressure ventilation. In addition, we noticed a dissociation between the SpO2 and PaO2 values and observed an increase in the level of methemoglobin.
Pulse oximeters do not directly measure oxygen saturation in the blood. Instead, the measurements are obtained by transmitting two wavelengths of light (red light, 660 nm; infrared light, 940 nm) through tissue (usually a finger or an earlobe) and detecting light that is not attenuated by the tissue bed [10]. Because SpO2 is based on data from healthy individuals with low levels of carboxyhemoglobin and methemoglobin, the values obtained from pulse oximetry may be invalid for patients with hemoglobin with different absorbance spectra [11]. The absorption coefficient of methemoglobin at 660 nm is almost the same as that at 940 nm, resulting in a 1:1 ratio of red light to infrared light. The SpO2 value is approximately 85% for this ratio, and SpO2 measures tends to approach 85% with an increase in the concentration of methemoglobin. An animal study reported that when methemoglobin concentration reaches 30–35%, with SpO2 plateaus between 82–86%; thereafter, SpO2 values become independent of methemoglobin concentration [11]. Our patient showed a methemoglobin concentration of 36.9% and SpO2 of 81%. This is largely consistent with the results of the previous animal study. In methemoglobinemia, cyanosis depends not on the concentration of methemoglobin, but on the total amount of methemoglobin present (calculated as hemoglobin value × %methemoglobin). Cyanosis occurs when the total amount of methemoglobin exceeds 1.5 g/dL. Therefore, a high erythrocyte count contributes to cyanosis, and anemic conditions cause cyanosis to be less prominent [12].
Congenital methemoglobinemia has three genetic causes [6,7]. The most common cause is CYB5R3 deficiency, followed by hemoglobin M disease and cytochrome B5 deficiency. There are two types of CYB5R3 deficiencies: type I deficiency is limited to erythrocytes, whereas type II deficiency occurs in all tissues. Patients with type I disease exhibit mild symptoms and have a normal lifespan, whereas those with type II disease exhibit cyanosis, experience neurological damage, and have a significantly shorter lifespan [7]. Type I patients are usually asymptomatic, although they may exhibit mild cyanosis in childhood. However, the decline of cardiopulmonary function with aging may cause additional symptoms, such as shortness of breath and fatigue. In the present case, genetic analysis (performed at the Division of Genomics, Medical Institute of Bioregulation, Kyushu University) revealed a mutation in the CYB5R3 gene—specifically, an arginine-to-glutamine substitution—that is known to cause type I disease [1]. Because the patient had type I disease, she was able to survive until the age of 79 years without major symptoms. Congenital methemoglobinemia due to CYB5R3 deficiency is inherited in an autosomal recessive manner and has been reported in certain populations [6,13,14,15]. Although there were no diagnosed cases of congenital methemoglobinemia in the family history of our patient, 28 cases of congenital methemoglobinemia have been reported in 12 families from the patient’s native place [16]. Kiyama et al. have previously reported 15 cases of congenital methemoglobinemia [17] and found that congenital methemoglobinemia is common on the islands of Henza and Miyagi in Okinawa, Japan. They surveyed 2876 islanders on the islands of Henza and Miyagi and found an additional 13 cases, leading to a total of 28 cases in 12 families. Of the 28 cases, 46.4% (13 of 28) were male; mean age was 27.3 years (median: 22, standard deviation: 15.8), 3 were over the age of 50 years, and 1 was 70-year-old; 25 were asymptomatic, 1 had epilepsy, and 2 had an intellectual disability. These findings suggest that the local population at this place may have a higher prevalence of congenital methemoglobinemia. We informed the patient’s daughter of this possibility.

4.3. Clinical Implications

Methemoglobinemia should be considered in the differential diagnosis of patients with central cyanosis, especially when there is significant dissociation between SpO2 and PaO2 values. This difference is generally greater than 5% in cases of methemoglobinemia [5]. A methemoglobin level of 20% suggests enzyme deficiency [5]. There are few subjective symptoms in the case of type I disease. However, the life expectancy of the patient is not shortened, as exemplified by the present case in which the diagnosis was not made until the age of 79 years.

5. Conclusions

Herein, we present a case of congenital methemoglobinemia first diagnosed at the age of 79 years. Cyanosis is the most common symptom indicative of congenital methemoglobinemia [5,6,7,8,9]. When evaluating central cyanosis, it is important to check for any dissociation between SpO2 and PaO2 values; if the difference exceeds 5%, methemoglobinemia should be considered as a possible diagnosis. Most cases of methemoglobinemia are acquired, and patients with type I CYB5R3 deficiency can have a prolonged lifespan. Furthermore, these patients may not be diagnosed until later in life, as observed in the present case.

Author Contributions

M.N. managed the case and wrote and revised the manuscript. N.Y., K.T., T.M., H.S. and T.K. assisted with the preparation and revision of the manuscript. All authors approved the final manuscript as submitted and agreed to be accountable for all aspects of this work. All authors take full responsibility for the integrity of the study and final manuscript. All authors have read and agreed to the published version of the manuscript.

Funding

This research received no external funding.

Institutional Review Board Statement

Due to the retrospective nature of the study, the need for ethics approval and consent was waived by the ethics committee of Naha City Hospital.

Informed Consent Statement

Written informed consent was obtained from the patient for publication of this case report and accompanying images. A copy of the written consent form is available for review by the Journal Editor.

Data Availability Statement

All data generated or analyzed during this study are included in this published article.

Conflicts of Interest

The authors declare no conflict of interest.

References

  1. Katsube, T.; Sakamoto, N.; Kobayashi, Y.; Seki, R.; Hirano, M.; Tanishima, K.; Tomoda, A.; Takazakura, E.; Yubisui, T.; Takeshita, M. Exonic Point Mutations in NADH-Cytochrome B5 Reductase Genes of Homozygotes for Hereditary Methemoglobinemia, Types I and III: Putative Mechanisms of Tissue-Dependent Enzyme Deficiency. Am. J. Hum. Genet. 1991, 48, 799–808. [Google Scholar] [PubMed]
  2. Shirabe, K.; Yubisui, T.; Borgese, N.; Tang, C.Y.; Hultquist, D.E.; Takeshita, M. Enzymatic Instability of NADH-Cytochrome b5 Reductase as a Cause of Hereditary Methemoglobinemia Type I (Red Cell Type). J. Biol. Chem. 1992, 267, 20416–20421. [Google Scholar] [CrossRef] [PubMed]
  3. Hall, R.; Yuan, S.; Wood, K.; Katona, M.; Straub, A.C. Cytochrome b5 Reductases: Redox Regulators of Cell Homeostasis. J. Biol. Chem. 2022, 298, 102654. [Google Scholar] [CrossRef] [PubMed]
  4. Ullah, A.; Shah, A.A.; Syed, F.; Mahmood, A.; Ur Rehman, H.; Khurshid, B.; Samad, A.; Ahmad, W.; Basit, S. Molecular Dynamic Simulation Analysis of a Novel Missense Variant in CYB5R3 Gene in Patients with Methemoglobinemia. Medicina 2023, 59, 379. [Google Scholar] [CrossRef] [PubMed]
  5. Soliman, D.S.; Yassin, M. Congenital Methemoglobinemia Misdiagnosed as Polycythemia Vera: Case Report and Review of Literature. Hematol. Rep. 2018, 10, 7221. [Google Scholar] [CrossRef] [PubMed] [Green Version]
  6. Alotaibi, A.T.; Alhowaish, A.A.; Alshahrani, A.; Alfaraj, D. Congenital Methemoglobinemia-Induced Cyanosis in Assault Victim. Cureus 2021, 13, e14079. [Google Scholar] [CrossRef] [PubMed]
  7. Izadi Firouzabadi, L.I.; Mead, P. Congenital Methaemoglobinaemia Presenting in a 55-Year-Old Man. BMJ Case Rep. 2020, 13, e236677. [Google Scholar] [CrossRef] [PubMed]
  8. Wang, Y.; Wu, Y.S.; Zheng, P.Z.; Yang, W.X.; Fang, G.A.; Tang, Y.C.; Xie, F.; Lan, F.H.; Zhu, Z.Y. A Novel Mutation in the NADH-Cytochrome b5 Reductase Gene of a Chinese Patient with Recessive Congenital Methemoglobinemia. Blood 2000, 95, 3250–3255. [Google Scholar] [CrossRef] [PubMed]
  9. Champigneulle, B.; Lecorre, M.; Bouzguenda, H.; Lemaire, S.; Ethuin, F.; Deleuze, P.; Rouquette, I.; Bouhemad, B. Late Diagnosis of Congenital Methemoglobinemia in an Elderly Patient During Cardiac Surgery. J. Cardiothorac. Vasc. Anesth. 2014, 28, 730–732. [Google Scholar] [CrossRef] [PubMed] [Green Version]
  10. Hurford, W.E.; Kratz, A. Case Records of the Massachusetts General Hospital. Weekly Clinicopathological Exercises. Case 23-2004. A 50-Year-Old Woman with Low Oxygen Saturation. N. Engl. J. Med. 2004, 351, 380–387. [Google Scholar] [CrossRef] [PubMed]
  11. Alexander, C.M.; Teller, L.E.; Gross, J.B. Principles of Pulse Oximetry: Theoretical and Practical Considerations. Anesth. Analg. 1989, 68, 368–376. [Google Scholar] [CrossRef] [PubMed]
  12. Prchal, J.T. Methemoglobinemia. In UpToDate®; Post, T.W., Burns, M.M., Burns, M.M., Tirnauer, J.S., Eds.; Wolters Kluwer: Alphen aan den Rijn, The Netherlands, 2022; Available online: https://www.uptodate.com/contents/methemoglobinemia?search=Methemoglobinemia&source=search_result&selectedTitle=1~150&usage_type=default&display_rank=1 (accessed on 11 March 2023).
  13. Burtseva, T.; Ammosova, T.; Prchal, J.T.; Chasnyk, V.; Nekhai, S.; Gordeuk, V.R. Type I Methemoglobinemia Caused by the Cytochrome b5 Reductase 806C>T Mutation Is Present in the Indigenous Evenk People of Yakutia. Blood 2009, 114, 2588. [Google Scholar] [CrossRef]
  14. Scott, E.M.; Hoskins, D.D. Hereditary Methemoglobinemia in Alaskan Eskimos and Indians. Blood 1958, 13, 795–802. [Google Scholar] [CrossRef] [PubMed]
  15. Scott, E.M. The Relation of Diaphorase of Human Erythrocytes to Inheritance of Methemoglobinemia. J. Clin. Investig. 1960, 39, 1176–1179. [Google Scholar] [CrossRef] [PubMed]
  16. Kiyama, T.; Tokeshi, H.; Kusumoto, Y.; Takekuma, Y.; Uchida, M. Studies on the Congenital Methemoglobinemia in Okinawa Islands. 3. Mass Survey on Henza and Miyagi Islands. Kumamoto Med. J. 1973, 26, 57–62. [Google Scholar] [PubMed]
  17. Kawakita, Y.; Tokeshi, H.; Miyake, T.; Fukutomi, J.; Dekita, K. Studies on the Congenital Methemoglobinemia in Okinawa Island. II. Diaphorase Activity. Kumamoto Med. J. 1966, 19, 211–219. [Google Scholar] [PubMed]
Figure 1. Electropherogram of the region of the variant NM_000398.7:c.173G>A [p.Arg58Gln]. The location of the variant is shown using a purple arrowhead. Abbreviations: Asp: Aspartic Acid; Thr: Phenylalanine; Arg: Arginine; Phe: Phenylalanine; Gln: Glutamine.
Figure 1. Electropherogram of the region of the variant NM_000398.7:c.173G>A [p.Arg58Gln]. The location of the variant is shown using a purple arrowhead. Abbreviations: Asp: Aspartic Acid; Thr: Phenylalanine; Arg: Arginine; Phe: Phenylalanine; Gln: Glutamine.
Medicina 59 00615 g001
Figure 2. Enzymatic activity of CYB5R3. (a) Structure of CYB5R3 protein. CYB5R3 is composed of three domains. The variant we identified is shown by a red arrowhead. (b) The process by which iron (Fe) ions are reduced by CYB5R3. Flavin adenine dinucleotide (FAD) is responsible for the transfer of electrons. Abbreviations: aa: amino acid; NADH: nicotinamide adenine dinucleotide cytochrome; NAD: nicotinamide adenine dinucleotide.
Figure 2. Enzymatic activity of CYB5R3. (a) Structure of CYB5R3 protein. CYB5R3 is composed of three domains. The variant we identified is shown by a red arrowhead. (b) The process by which iron (Fe) ions are reduced by CYB5R3. Flavin adenine dinucleotide (FAD) is responsible for the transfer of electrons. Abbreviations: aa: amino acid; NADH: nicotinamide adenine dinucleotide cytochrome; NAD: nicotinamide adenine dinucleotide.
Medicina 59 00615 g002
Figure 3. SpO2 values and other vital signs before the administration of methylene blue.
Figure 3. SpO2 values and other vital signs before the administration of methylene blue.
Medicina 59 00615 g003
Figure 4. SpO2 values and other vital signs after the administration of methylene blue.
Figure 4. SpO2 values and other vital signs after the administration of methylene blue.
Medicina 59 00615 g004
Figure 5. Lips of the patient before (top, showing cyanosis) and after (bottom, no cyanosis) the administration of methylene blue.
Figure 5. Lips of the patient before (top, showing cyanosis) and after (bottom, no cyanosis) the administration of methylene blue.
Medicina 59 00615 g005
Figure 6. Color of the patient’s blood before (left) and after (right) the administration of methylene blue.
Figure 6. Color of the patient’s blood before (left) and after (right) the administration of methylene blue.
Medicina 59 00615 g006
Table 1. Laboratory test results at admission.
Table 1. Laboratory test results at admission.
ParameterRecorded ValueStandard Value
White blood cell count5800/µL3300–8600/µL
Hemoglobin13.2 g/dL11.5–15.0 g/dL
Platelet count20.9 × 104/µL15–35 × 103/µL
C-reactive protein1.31 mg/dL≤0.14 mg/dL
Total protein7.3 g/dL6.6–8.1 g/dL
Albumin3.7 g/dL4.1–5.1 g/dL
Aspartate aminotransferase13 U/L13–30 U/L
Alanine aminotransferase8 U/L7–23 U/L
Lactase dehydrogenase131 U/L124–222 U/L
Blood urea nitrogen 14.0 mg/dL8–20 mg/dL
Creatinine0.93 mg/dL0.46–0.79 mg/dL
Sodium 139 mEq/L138–145 mEq/L
Potassium 4.1 mEq/L3.6–4.8 mEq/L
Chloride104 mEq/L101–108 mEq/L
Glucose100 mg/dL75–110 mg/dL
Atrial blood gas
pH7.4577.35–7.45
pCO236.8 mmHg35–45 mmHg
pO2325.4 mmHg80–90 mmHg
O2 saturation99.8%92.0–98.5%
HCO325.4 mmol/L21–30 mmol/L
Lactate1.10 mmol/L0.5–1.6 mmol/L
Methemoglobin36.9%0–1.5%
Abbreviations: pCO2: partial pressure of arterial carbon dioxide; pO2:partial pressure of arterial oxygen; HCO3: bicarbonate.
Disclaimer/Publisher’s Note: The statements, opinions and data contained in all publications are solely those of the individual author(s) and contributor(s) and not of MDPI and/or the editor(s). MDPI and/or the editor(s) disclaim responsibility for any injury to people or property resulting from any ideas, methods, instructions or products referred to in the content.

Share and Cite

MDPI and ACS Style

Nakata, M.; Yokota, N.; Tabata, K.; Morikawa, T.; Shibata, H.; Kenzaka, T. Hereditary Congenital Methemoglobinemia Diagnosed at the Age of 79 Years: A Case Report. Medicina 2023, 59, 615. https://doi.org/10.3390/medicina59030615

AMA Style

Nakata M, Yokota N, Tabata K, Morikawa T, Shibata H, Kenzaka T. Hereditary Congenital Methemoglobinemia Diagnosed at the Age of 79 Years: A Case Report. Medicina. 2023; 59(3):615. https://doi.org/10.3390/medicina59030615

Chicago/Turabian Style

Nakata, Marohito, Naoko Yokota, Kazuhiko Tabata, Takuya Morikawa, Hiroki Shibata, and Tsuneaki Kenzaka. 2023. "Hereditary Congenital Methemoglobinemia Diagnosed at the Age of 79 Years: A Case Report" Medicina 59, no. 3: 615. https://doi.org/10.3390/medicina59030615

Article Metrics

Back to TopTop