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Cyanide Analysis (Free, Physiologically Available)

The environmental chemistry of cyanide is extremely complex. The cyanide chemistry associated with MGP wastes in the environment is of particular interest because a wide range of cyanide species can be present, and there can be a significant difference in toxicity observed among them.  This risk-based approach to characterizing cyanide requires reliable analytical procedures that can delineate the cyanide species that are present into categories based on their relative toxicities. In addition, the use of specific analytical methods is often mandated for samples collected under various regulatory settings. For example, the EPA Clean Water Act (CWA) regulations generally require the use of total and amenable cyanide procedures for National Pollutant Discharge Elimination Systems (NPDES) and Publicly-Owned Treatment Works (POTW) discharge applications, as well as EPA's Resource Conservation and Recovery Act (RCRA); and Comprehensive Environmental Response, Compensation and Liability Act (CERCLA) regulations that generally specify the use of total cyanide. For MGP applications, where a risk-based corrective action approach is being utilized, the concentration of cyanide species that are bioavailable is often of interest.

Alpha offers the following cyanide analytical methods that can be used to determine cyanide species considered to be bioavailable:

Free Cyanide via EPA Method 9016

This procedure was initially developed with the Sediment Contaminant Bioavailability Alliance (SCBA),  a consortium that involved industry, utilities, government and consultants. Originally an ASTM procedure that has now been incorporated into EPA's SW-846 methods manual, the Free Cyanide via EPA Method 9016 is particularly useful for   free cyanide (CN, HCN), the species that represent the most risk and  the smallest contribution to overall total cyanide present, generally and proportionally..

Physiologically Available Cyanide (PAC) via MCP Method

The Massachusetts Contingency Plan (MCP) Physiologically Available Cyanide (PAC) method was originally developed through an initiative of the Massachusetts Natural Gas Council and the Mass. Department of Environmental Protection (MassDEP). The impetus for developing the method was based on the need for a risk-based procedure for use with MGP applications and to   model the amount of cyanide that would be converted into bioavailable forms under conditions present in the human stomach. MGP wastes containing cyanide are typically composed of a high percentage of the strongly-complexed iron cyanides as a result of the use of iron as a cyanide scavenger in the typical MGP process stream. The iron-complexed cyanides, however, are relatively low in toxicity and the use of an analytical procedure that does not exclude them from the total cyanide concentration determined by the method can greatly overestimate the risk these wastes pose to human health.

The original 1996 protocol was produced by the combined efforts of Ogden Environmental & Energy Services (now AMEC), Boston Gas (now National Grid), Bay State Gas, NET Atlantic and MassDEP. This procedure was then reviewed, revised and reformatted by the MassDEP Data Quality Enhancement Workgroup in 2004 and again in 2010. It was released with the MCP Total Cyanide Method, as one of the MCP methods listed in the Compendium of Analytical Methods. This procedure is unique, in that it incorporates both positive and negative controls that ensure that the sum of weakly-complexed cyanide species-- ranging from free cyanides up to, but not including iron cyanides-- is accurately represented.

Alpha Analytical published the following peer-reviewed paper concerning cyanide analysis for MGP applications: "A Comparison of Commonly Used Cyanide Analytical Methodologies for Manufactured Gas Plant (MGP) Applications", by James F. Occhialini, James C. Todaro, Joseph Clements, James Roth, Elena Dayn, Tamara Burke Devine, William R. Swanson and Michael Rostkowski, published in the Journal of Environmental Forensics, Taylor & Francis Publishers, Volume 5, Number 2, June 2004.

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