The relationship between exacerbated diabetic peripheral neuropathy and metformin treatment in type 2 diabetes mellitus

Metformin-treated diabetics (MTD) showed a decrease in cobalamin, a rise in homocysteine, and methylmalonic acid, leading to accentuated diabetic peripheral neuropathy (DPN). This study aimed to determine whether or not metformin is a risk factor for DPN. We compared MTD to non-metformin-treated diabetics (NMTD) clinically using the Toronto Clinical Scoring System (TCSS), laboratory (methylmalonic acid, cobalamin, and homocysteine), and electrophysiological studies. Median homocysteine and methylmalonic acid levels in MTD vs. NMTD were 15.3 vs. 9.6 µmol/l; P < 0.001 and 0.25 vs. 0.13 µmol/l; P = 0.02, respectively with high statistical significance in MTD. There was a significantly lower plasma level of cobalamin in MTD than NMTD. Spearman’s correlation showed a significant negative correlation between cobalamin and increased dose of metformin and a significant positive correlation between TCSS and increased dose of metformin. Logistic regression analysis showed that MTD had significantly longer metformin use duration, higher metformin dose > 2 g, higher TCSS, lower plasma cobalamin, and significant higher homocysteine. Diabetics treated with metformin for prolonged duration and higher doses were associated with lower cobalamin and more severe DPN.

www.nature.com/scientificreports/ not generally distinguish early changes of neuronal damage and some DPN patients give negative results in the clinical assessment 23 . Our study intends to distinguish the serum level of cobalamin, methylmalonic acid and homocysteine changes in Metformin-treated diabetics (MTD) and to evaluate the connection between the severity of DPN and the long-term utilization of metformin.

Methods
Participants and inclusion criteria. 150 adult patients with Type 2 DM (T2DM) were included according to Standards of Medical Care in Diabetes Guidelines 24 . We prospectively identified patients diagnosed with T2DM who were treated with metformin for more than 6 months. Also, we select non-metformin treated age and sex matched with metformin treated group with the same number of cases. The study design was a casecontrol, prospective, analytical, observational study. Cases were T2DM patients on metformin (75 participants). Controls were T2DM patients not taking metformin (75 participants). The present prospective study was conducted during the period from the first of May 2017 to the end of September 2018 in the neurology outpatient clinic, Mansoura University Hospital, Egypt. The included patients were type two diabetics on oral hypoglycemic therapy with clinical proof for DPN. Patients were classified into 2 groups; Metformin treated (group I): included 75 patients administered metformin for the previous 6 months or more and non-metformin treated (group II): included 75 patients who weren't administered metformin for the previous 6 months (but administered other oral hypoglycemic drugs). The duration of DPN was determined by the history of onset of symptoms or the previous electrophysiological studies done.
Sample size determination. The formula for estimation of sample size is: where n is the needed sample size, Z is the critical value at 95% confidence level (1.96), p is the prevalence of vitamin B12 deficiency in cases with type 2 DM on metformin (9.7%) obtained from the study of de Groot et al. 25 . e is the error margin that the researcher was willing to accept, and in this condition, was equal to 0.05. Note that (1-p) = q, which was the proportion of the sample population not covered by the study.
Exclusion criteria. The patients excluded from this study possessed the following characteristics: type 1 diabetes mellitus, impaired glucose tolerance, peripheral neuropathy because of different causes other than diabetes or cobalamin insufficiency and patient cease treatment by metformin or administrated metformin for less than 6 months. Clinical assessment. Complete history taking for symptoms of DPN, family history of DPN, medical history, duration of DM, and current medications for DM or other systemic diseases was taken. Also, complete general and neurological examinations were done. The clinical assessment of the severity of DPN was done by the Toronto Clinical Scoring System (TCSS) which comprises of three sections: symptom scores, reflex scores, and sensory test scores. The greatest score is 19 points: 0-5 if there is no diabetic peripheral neuropathy, 6-8 if there is mild diabetic peripheral neuropathy, 9-11 if there is moderate diabetic peripheral neuropathy, 12-19 if there is severe diabetic peripheral neuropathy 24,26 . Electrophysiological studies and laboratory investigations. Regarding the electrophysiological studies, a nerve conduction study was carried out for all patients by utilizing Xilec-Xcalibur from Natus neurology, USA, 2010. The selected nerves, according to clinical symptoms and findings were examined for motor and sensory conduction studies, the distal latency, the amplitude of action potential, motor and sensory conduction velocities were measured 25,27 . The laboratory investigations include complete blood count, electrolytes, renal and hepatic functions, thyroid-stimulating hormone, rheumatoid factor, serum folate, Hemoglobin A1c, and serum cobalamin level according to the classic method of radioimmunoassay. High-performance liquid chromatography used to measure the homocysteine levels and mass spectrometry used to measure methylmalonic acid levels for all patients. Statistical analysis. The Statistical Package for Social Sciences (SPSS) programming, version 21.0 was utilized for information registration, approval, and analysis. Frequency, tables, and diagrams were produced for the categorical variables. Tests of significance were created for various variables. The Chi-square test was utilized to test categorical variables, and independent t-tests were utilized to test the importance of the results of the two groups. The Mann-Whitney U test was utilized to contrast and to investigate the means of the independent variables. The correlation coefficient and Chi-squared tests were utilized to gauge the relation between two quantitative and qualitative variables. The degree of statistical significance was characterized by an estimation of P-value < 0.05. Spearman's correlation coefficient was done to analyze the relationship between continuous variables such as metformin dose and vitamin B12 levels and also between metformin dose and TCSS scores. www.nature.com/scientificreports/ Logistic regression analysis was carried out to identify independent risk factors for diabetic PN in metformintreated patients.

Patients demographic and clinical characteristics.
This study was carried out on 150 patients with type 2 diabetes mellitus. Group I included 75 patients administered metformin for the previous 6 months or more. Group II included 75 patients who weren't administered metformin for the previous 6 months (but administered other oral hypoglycemic drugs). The two groups were similar in age, sex. Also, there was no important difference between both groups regarding differences in the disease severity, the duration of diabetes, and duration of diabetic PN (P = 0.9 and 0.82 respectively (Table 1). MTD had a significantly higher moderate to severe DPN and higher total scores of TCSS (10 ± 7.5 vs. 5 ± 9.5, P < 0.001) indicated that metformin users had a more severe DPN (Table 1). Table 2 showed a lower median serum cobalamin in the metformin-treated diabetics with high statistical significance (222 vs. 471 pmol/l; P < 0.001). There were also significant differences between the two groups in median serum homocysteine and methylmalonic acid levels, and MTD showed higher levels with P < 0.05. HbA1c was higher in metformin-treated diabetics without statistical significance (P = 0.09).  sural nerves in MTD showed significant slower conductivity with P < 0.05. Additionally, median sensory nerve action potentials (SNAP) studies for sural and superficial peroneal nerves in the MTD showed a significantly lower level with P < 0.05 (Table 3).

Laboratory findings for metformin-treated and non-metformin-treated groups.
Correlation of metformin dose to vitamin B12 and Cbl plasma levels. Spearman's correlation coefficient was used to examine the bivariate relationship between the two continuous variables of metformin dose and vitamin B12 levels and metformin dose and TCSS. Figure 1A showed a significant negative correlation between cobalamin plasma levels and higher doses of metformin (r = − 0.522 and P = 0.01). Figure 1B showed a significant positive correlation between TCSS and increased dose of metformin (r = 0.891 and P < 0.05).
Correlation of the severity of DPN with cobalamin, homocysteine, and methylmalonic acid (Fig. 2). There was a significant inverse relationship with the severity of DPN and cobalamine level (r = − 0.81 and P < 0.05), while the severity of DPN was directly related to higher levels of both methylmalonic acid, and homocysteine (r = 0.71 and P < 0.05; and r = 0.73 and P < 0.05 respectively).  (Table 4).

Discussion
Diabetic patients have different degrees of nervous system damage ranging from mild to severe forms, the most widely recognized being peripheral neuropathy which affects 60% to 70% of cases 28 . The aim of this study was to assess whether metformin is a risk factor for the development of DPN by evaluating the impact of metformin Table 3. Comparison of nerve conduction study features for metformin-treated and non-metformin-treated groups. SNAP: sensory nerve action potential, MT: metformin-treated, NMT: non-metformin-treated, N: number.

Electrophysiological findings MT N (75) NMT N (75) P-value
Superficial peroneal nerve SNAP (amplitude µv) 3.2 ± 5.7 5.9 ± 6.9 < 0.05  The present single-center prospective study during a one and half year duration was carried out on 150 patients (80 males and 70 females) with DPN, during their attendance to the neurology outpatient clinic. The current study stated that the MTD had significant higher DPN (50.7%), total TCSS scores (10 ± 7.5), serum levels www.nature.com/scientificreports/ of homocysteine (15.3 µmol/l) and methylmalonic acid (0.25 µmol/l), lower cobalamin (222 pmol/l), median conduction velocity and SNAP for superficial peroneal, and sural nerves. Also, there was a significant negative correlation between cobalamin and metformin. On the other hand, there was a significant positive correlation between TCSS and metformin. The significant predictors' explanatory parameters associated with DPN occurrence in MTD were larger dose and longer duration of metformin usage, low cobalamin level, and high homocysteine level. Our results were in harmony with Khan et al. who concluded that patients with type 2 DM with prolonged duration of treatment with metformin were accompanied by a higher occurrence of vitamin B12 inadequacy 35 . So, clinicians should screen diabetic patients who are metformin users for any B12 deficiency accordingly. Our study exhibited a higher median serum level of Hcy and MMA. These variations from the normal values were highly related to metformin users. Our findings were as per that of Ahmed and Chapman et al., demonstrating that long-term metformin users compared to the non-metformin users had lower serum Cbl, higher MMA and Hcy 36,37 .
Our results demonstrate that metformin treatment conveys a potential hazard for the occurrence of cobalamin lack. However, this would most likely be little if cobalamin status is monitored consistently. Cobalamin inadequacy is increased among patients with type 2 diabetes mellitus. There is a requirement for a more precise differential conclusion to recognize diabetic neuropathy and metformin-induced neuropathy. We also found that patients with type 2 DM, DPN, and more than 6 months of treatment by metformin demonstrated higher scores on the TCSS, indicating more clinically severe DPN when contrasted with comparative to non-metformin users. These findings were frequently connected with cumulative metformin utilization with a positive correlation between DPN and cumulative metformin dose. These results were similar to that of Holay et al. who found the incidence of neuropathy by TCSS and NCV test was significantly higher in metformin users with a positive correlation with cumulative dose and duration of metformin and a negative correlation with serum vitamin B12 levels 38 . Similar to our results, Singh et al. discovered a smaller yet significant difference in neuropathy scores in between metformin and non-metformin users 39 .
Electrophysiologically, this study exhibited that the metformin users had more severe DPN. Measurements of the mean conduction velocity and mean amplitude of SNAP of the examined nerves were altogether significantly lower in the metformin users' group. These results are not quite the same as Wile and Toth who found an insignificant lower mean conduction velocity and mean amplitude of SNAP in the metformin users' group 40 . This may be explained by the difference in demographic characteristics and longer duration of the disease in our study. The nerves of lower limbs, especially sural and superficial peroneal nerves were more sensitive to diabetic effects. This may be also supported by the study of Shibata et al. and Agarwal et al. who found that the sural nerve conduction study had the most reliable test that correlates well with the severity of diabetic PN 41,42 .
In our study the severity of DPN was inversely correlated with the cobalamine level and directly correlated with higher levels of both methylmalonic acid, and homocysteine. Similarly, Wile and Toth found that the clinically worsened DPN was associated with lower cobalamine level and higher levels of both methylmalonic acid, and homocysteine 40 . It has been shown that elevated levels of total homocysteine significantly correlated with DPN, independent of other risk factors 43,44 . The serum MMA positively correlated with the severity of neuropathic pain and this can be used as a useful marker in assessment of peripheral neuropathy 45 .
The discoveries in this study recommended that a cumulative dose of metformin is accompanied with a decrease in levels of cobalamin and deterioration of DPN. However, metformin is the main therapy in type 2 DM Limitations and directions of future work. Finally, the present study had some limitations. The first limitation was the relatively small number of patients due to the limitation of resources and financial issues. Glycemic control not being assessed is also a limitation of this study. Also, this study, cannot evaluate long-term effects of risk factors concerning the development of DPN. Further studies should be conducted on a larger number of patients for a longer duration and to follow up patients with DPN for the improvement of manifestations especially after stoppage of metformin.

Conclusion
Patients with type 2 DM who were treated with metformin for prolonged duration and higher doses were associated with lower plasma cobalamin and more severe DPN. Patients on metformin treatment must monitor regularly for plasma levels of cobalamin, methylmalonic acid, and homocysteine.

Recommendation
• Routine screening of type 2 diabetic patients on metformin for vitamin B12 inadequacy is highly recommended due to its high prevalence and the significant clinical impacts that may result in DPN. • Besides, we suggest, beginning treating patients with B12 once a borderline or low level is recognized. www.nature.com/scientificreports/ Open Access This article is licensed under a Creative Commons Attribution 4.0 International License, which permits use, sharing, adaptation, distribution and reproduction in any medium or format, as long as you give appropriate credit to the original author(s) and the source, provide a link to the Creative Commons licence, and indicate if changes were made. The images or other third party material in this article are included in the article's Creative Commons licence, unless indicated otherwise in a credit line to the material. If material is not included in the article's Creative Commons licence and your intended use is not permitted by statutory regulation or exceeds the permitted use, you will need to obtain permission directly from the copyright holder. To view a copy of this licence, visit http://creat iveco mmons .org/licen ses/by/4.0/.