The Role of Mercury and Cadmium Heavy Metals in Vascular Disease, Hypertension, Coronary Heart Disease, and Myocardial Infarction

Overview

Journal Altern Ther Health Med

Specialty Rehabilitation Medicine

Date 2007 Apr 5

PMID 17405690

Citations 67

Authors

Mark C Houston

Affiliations

Soon will be listed here.

Abstract

Mercury, cadmium, and other heavy metals have a high affinity for sulfhydryl (-SH) groups, inactivating numerous enzymatic reactions, amino acids, and sulfur-containing antioxidants (NAC, ALA, GSH), with subsequent decreased oxidant defense and increased oxidative stress. Both bind to metallothionein and substitute for zinc, copper, and other trace metals reducing the effectiveness of metalloenzymes. Mercury induces mitochondrial dysfunction with reduction in ATP, depletion of glutathione, and increased lipid peroxidation; increased oxidative stress is common. Selenium antagonizes mercury toxicity. The overall vascular effects of mercury include oxidative stress, inflammation, thrombosis, vascular smooth muscle dysfunction, endothelial dysfunction, dyslipidemia, immune dysfunction, and mitochondrial dysfunction. The clinical consequences of mercury toxicity include hypertension, CHD, MI, increased carotid IMT and obstruction, CVA, generalized atherosclerosis, and renal dysfunction with proteinuria. Pathological, biochemical, and functional medicine correlations are significant and logical. Mercury diminishes the protective effect of fish and omega-3 fatty acids. Mercury, cadmium, and other heavy metals inactivate COMT, which increases serum and urinary epinephrine, norepinephrine, and dopamine. This effect will increase blood pressure and may be a clinical clue to heavy metal toxicity. Cadmium concentrates in the kidney, particularly inducing proteinuria and renal dysfunction; it is associated with hypertension, but less so with CHD. Renal cadmium reduces CYP4A11 and PPARs, which may be related to hypertension, sodium retention, glucose intolerance, dyslipidemia, and zinc deficiency. Dietary calcium may mitigate some of the toxicity of cadmium. Heavy metal toxicity, especially mercury and cadmium, should be evaluated in any patient with hypertension, CHD, or other vascular disease. Specific testing for acute and chronic toxicity and total body burden using hair, toenail, urine, serum, etc. with baseline and provoked evaluation should be done.

Citing Articles

Selective fluoride ion sensing using novel quinoline chemosensor insights into kinetics and molecular logic gate functions.

Ashwathi A, Basheer S Sci Rep. 2025; 15(1):1859.

PMID: 39806002 PMC: 11730337. DOI: 10.1038/s41598-024-84414-z.

Relation between Systemic Inflammatory Index (SII) and Hair Trace Elements, Metals and Metalloids Concentration in Epicardial Coronary Artery Disease-Preliminary Report.

Urbanowicz T, Hanc A, Olasinska-Wisniewska A, Komosa A, Filipiak K, Radziemski A Rev Cardiovasc Med. 2024; 24(12):358.

PMID: 39077068 PMC: 11272833. DOI: 10.31083/j.rcm2412358.

A Bayesian network for estimating hypertension risk due to occupational aluminum exposure.

Zhao L, Yin J, Huan J, Han X, Zhao D, Song J Chronic Dis Transl Med. 2024; 10(2):130-139.

PMID: 38872757 PMC: 11166680. DOI: 10.1002/cdt3.134.

Medicinal Plant-derived Phytochemicals in Detoxification.

Bjorklund G, Cruz-Martins N, Goh B, Mykhailenko O, Lysiuk R, Shanaida M Curr Pharm Des. 2023; 30(13):988-1015.

PMID: 37559241 DOI: 10.2174/1381612829666230809094242.

Metals and Trace Elements in Calcified Valves in Patients with Acquired Severe Aortic Valve Stenosis: Is There a Connection with the Degeneration Process?.

Tomasek A, Manousek J, Kuta J, Hlasensky J, Kren L, Sindler M J Pers Med. 2023; 13(2).

PMID: 36836554 PMC: 9967375. DOI: 10.3390/jpm13020320.