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Friday, July 19, 2019

Hepatitis C

From Wikipedia, the free encyclopedia
 
Hepatitis C
HCV EM picture 2.png
Electron micrograph of hepatitis C virus from cell culture (scale = 50 nanometers)
SpecialtyGastroenterology, Infectious disease
SymptomsTypically none
ComplicationsLiver failure, liver cancer, esophageal and gastric varices
DurationLong term (80%)
CausesHepatitis C virus usually spread by blood-to-blood contact
Diagnostic methodBlood testing for antibodies or viral RNA
PreventionClean needles, testing donated blood
TreatmentMedications, liver transplant
MedicationSofosbuvir, simeprevir
Frequency143 million / 2% (2015)
Deaths496,000 (2015)

Hepatitis C is an infectious disease caused by the hepatitis C virus (HCV) that primarily affects the liver. During the initial infection people often have mild or no symptoms. Occasionally a fever, dark urine, abdominal pain, and yellow tinged skin occurs. The virus persists in the liver in about 75% to 85% of those initially infected. Early on chronic infection typically has no symptoms. Over many years however, it often leads to liver disease and occasionally cirrhosis. In some cases, those with cirrhosis will develop serious complications such as liver failure, liver cancer, or dilated blood vessels in the esophagus and stomach.

HCV is spread primarily by blood-to-blood contact associated with intravenous drug use, poorly sterilized medical equipment, needlestick injuries in healthcare, and transfusions. Using blood screening, the risk from a transfusion is less than one per two million. It may also be spread from an infected mother to her baby during birth. It is not spread by superficial contact. It is one of five known hepatitis viruses: A, B, C, D, and E. Diagnosis is by blood testing to look for either antibodies to the virus or its RNA. Testing is recommended in all people who are at risk.

There is no vaccine against hepatitis C. Prevention includes harm reduction efforts among people who use intravenous drugs and testing donated blood. Chronic infection can be cured about 95% of the time with antiviral medications such as sofosbuvir or simeprevir. Peginterferon and ribavirin were earlier generation treatments that had a cure rate of less than 50% and greater side effects. Getting access to the newer treatments however can be expensive. Those who develop cirrhosis or liver cancer may require a liver transplant. Hepatitis C is the leading reason for liver transplantation, though the virus usually recurs after transplantation.

An estimated 143 million people (2%) worldwide are infected with hepatitis C as of 2015. In 2013 about 11 million new cases occurred. It occurs most commonly in Africa and Central and East Asia. About 167,000 deaths due to liver cancer and 326,000 deaths due to cirrhosis occurred in 2015 due to hepatitis C. The existence of hepatitis C – originally identifiable only as a type of non-A non-B hepatitis – was suggested in the 1970s and proven in 1989. Hepatitis C infects only humans and chimpanzees.

Signs and symptoms

Acute infection

Hepatitis C infection causes acute symptoms in 15% of cases. Symptoms are generally mild and vague, including a decreased appetite, fatigue, nausea, muscle or joint pains, and weight loss and rarely does acute liver failure result. Most cases of acute infection are not associated with jaundice. The infection resolves spontaneously in 10–50% of cases, which occurs more frequently in individuals who are young and female.

Chronic infection

About 80% of those exposed to the virus develop a chronic infection. This is defined as the presence of detectable viral replication for at least six months. Most experience minimal or no symptoms during the initial few decades of the infection. Chronic hepatitis C can be associated with fatigue and mild cognitive problems. Chronic infection after several years may cause cirrhosis or liver cancer. The liver enzymes are normal in 7–53%. Late relapses after apparent cure have been reported, but these can be difficult to distinguish from reinfection.

Fatty changes to the liver occur in about half of those infected and are usually present before cirrhosis develops. Usually (80% of the time) this change affects less than a third of the liver. Worldwide hepatitis C is the cause of 27% of cirrhosis cases and 25% of hepatocellular carcinoma. About 10–30% of those infected develop cirrhosis over 30 years. Cirrhosis is more common in those also infected with hepatitis B, schistosoma, or HIV, in alcoholics and in those of male gender. In those with hepatitis C, excess alcohol increases the risk of developing cirrhosis 100-fold. Those who develop cirrhosis have a 20-fold greater risk of hepatocellular carcinoma. This transformation occurs at a rate of 1–3% per year. Being infected with hepatitis B in addition to hepatitis C increases this risk further.

Liver cirrhosis may lead to portal hypertension, ascites (accumulation of fluid in the abdomen), easy bruising or bleeding, varices (enlarged veins, especially in the stomach and esophagus), jaundice, and a syndrome of cognitive impairment known as hepatic encephalopathy. Ascites occurs at some stage in more than half of those who have a chronic infection.

Extrahepatic complications

The most common problem due to hepatitis C but not involving the liver is mixed cryoglobulinemia (usually the type II form) — an inflammation of small and medium-sized blood vessels. Hepatitis C is also associated with the autoimmune disorder such as Sjögren's syndrome, lichen planus, a low platelet count, porphyria cutanea tarda, necrolytic acral erythema, insulin resistance, diabetes mellitus, diabetic nephropathy, autoimmune thyroiditis, and B-cell lymphoproliferative disorders. 20–30% of people infected have rheumatoid factor — a type of antibody. Possible associations include Hyde's prurigo nodularis and membranoproliferative glomerulonephritis. Cardiomyopathy with associated abnormal heart rhythms has also been reported. A variety of central nervous system disorders has been reported. Chronic infection seems to be associated with an increased risk of pancreatic cancer. People may experience other issues in the mouth such as dryness, salivary duct stones, and crusted lesions around the mouth.

Occult infection

Persons who have been infected with hepatitis C may appear to clear the virus but remain infected. The virus is not detectable with conventional testing but can be found with ultra-sensitive tests. The original method of detection was by demonstrating the viral genome within liver biopsies, but newer methods include an antibody test for the virus' core protein and the detection of the viral genome after first concentrating the viral particles by ultracentrifugation. A form of infection with persistently moderately elevated serum liver enzymes but without antibodies to hepatitis C has also been reported. This form is known as cryptogenic occult infection.

Several clinical pictures have been associated with this type of infection. It may be found in people with anti-hepatitis-C antibodies but with normal serum levels of liver enzymes; in antibody-negative people with ongoing elevated liver enzymes of unknown cause; in healthy populations without evidence of liver disease; and in groups at risk for HCV infection including those on hemodialysis or family members of people with occult HCV. The clinical relevance of this form of infection is under investigation. The consequences of occult infection appear to be less severe than with chronic infection but can vary from minimal to hepatocellular carcinoma.

The rate of occult infection in those apparently cured is controversial but appears to be low. 40% of those with hepatitis but with both negative hepatitis C serology and the absence of detectable viral genome in the serum have hepatitis C virus in the liver on biopsy. How commonly this occurs in children is unknown.

Virology

The hepatitis C virus (HCV) is a small, enveloped, single-stranded, positive-sense RNA virus. It is a member of the genus Hepacivirus in the family Flaviviridae. There are seven major genotypes of HCV, which are known as genotypes one to seven. The genotypes are divided into several subtypes with the number of subtypes depending on the genotype. In the United States, about 70% of cases are caused by genotype 1, 20% by genotype 2 and about 1% by each of the other genotypes. Genotype 1 is also the most common in South America and Europe.

The half life of the virus particles in the serum is around 3 hours and may be as short as 45 minutes. In an infected person, about 1012 virus particles are produced each day. In addition to replicating in the liver the virus can multiply in lymphocytes.

Transmission

Hepatitis C infection in the United States by source
 
The primary route of transmission in the developed world is intravenous drug use (IDU), while in the developing world the main methods are blood transfusions and unsafe medical procedures. The cause of transmission remains unknown in 20% of cases; however, many of these are believed to be accounted for by IDU.

Drug use

Intravenous drug use (IDU) is a major risk factor for hepatitis C in many parts of the world. Of 77 countries reviewed, 25 (including the United States) were found to have prevalences of hepatitis C in the intravenous drug user population of between 60% and 80%. Twelve countries had rates greater than 80%. It is believed that ten million intravenous drug users are infected with hepatitis C; China (1.6 million), the United States (1.5 million), and Russia (1.3 million) have the highest absolute totals. Occurrence of hepatitis C among prison inmates in the United States is 10 to 20 times that of the occurrence observed in the general population; this has been attributed to high-risk behavior in prisons such as IDU and tattooing with nonsterile equipment. Shared intranasal drug use may also be a risk factor.

Healthcare exposure

Blood transfusion, transfusion of blood products, or organ transplants without HCV screening carry significant risks of infection. The United States instituted universal screening in 1992 and Canada instituted universal screening in 1990. This decreased the risk from one in 200 units to between one in 10,000 to one in 10,000,000 per unit of blood. This low risk remains as there is a period of about 11–70 days between the potential blood donor's acquiring hepatitis C and the blood's testing positive depending on the method. Some countries do not screen for hepatitis C due to the cost.

Those who have experienced a needle stick injury from someone who was HCV positive have about a 1.8% chance of subsequently contracting the disease themselves. The risk is greater if the needle in question is hollow and the puncture wound is deep. There is a risk from mucosal exposures to blood, but this risk is low, and there is no risk if blood exposure occurs on intact skin.

Hospital equipment has also been documented as a method of transmission of hepatitis C, including reuse of needles and syringes; multiple-use medication vials; infusion bags; and improperly sterilized surgical equipment, among others. Limitations in the implementation and enforcement of stringent standard precautions in public and private medical and dental facilities are known to be the primary cause of the spread of HCV in Egypt, the country with highest rate of infection in the world.

Sexual intercourse

Sexual transmission of hepatitis C is uncommon. Studies examining the risk of HCV transmission between heterosexual partners, when one is infected and the other is not, have found very low risks. Sexual practices that involve higher levels of trauma to the anogenital mucosa, such as anal penetrative sex, or that occur when there is a concurrent sexually transmitted infection, including HIV or genital ulceration, present greater risks. The United States Department of Veterans Affairs recommends condom use to prevent hepatitis C transmission in those with multiple partners, but not those in relationships that involve only a single partner.

Body modification

Tattooing is associated with two to threefold increased risk of hepatitis C. This can be due to either improperly sterilized equipment or contamination of the dyes being used. Tattoos or piercings performed either before the mid-1980s, "underground," or nonprofessionally are of particular concern, since sterile techniques in such settings may be lacking. The risk also appears to be greater for larger tattoos. It is estimated that nearly half of prison inmates share unsterilized tattooing equipment. It is rare for tattoos in a licensed facility to be directly associated with HCV infection.

Shared personal items

Personal-care items such as razors, toothbrushes, and manicuring or pedicuring equipment can be contaminated with blood. Sharing such items can potentially lead to exposure to HCV. Appropriate caution should be taken regarding any medical condition that results in bleeding, such as cuts and sores. HCV is not spread through casual contact, such as hugging, kissing, or sharing eating or cooking utensils. Neither is it transmitted through food or water.

Mother-to-child transmission

Mother-to-child transmission of hepatitis C occurs in less than 10% of pregnancies. There are no measures that alter this risk. It is not clear when transmission occurs during pregnancy, but it may occur both during gestation and at delivery. A long labor is associated with a greater risk of transmission. There is no evidence that breastfeeding spreads HCV; however, to be cautious, an infected mother is advised to avoid breastfeeding if her nipples are cracked and bleeding, or if her viral loads are high.

Diagnosis

Serologic profile of Hepatitis C infection
 
There are a number of diagnostic tests for hepatitis C, including HCV antibody enzyme immunoassay or ELISA, recombinant immunoblot assay, and quantitative HCV RNA polymerase chain reaction (PCR). HCV RNA can be detected by PCR typically one to two weeks after infection, while antibodies can take substantially longer to form and thus be detected.

Chronic hepatitis C is defined as infection with the hepatitis C virus persisting for more than six months based on the presence of its RNA. Chronic infections are typically asymptomatic during the first few decades, and thus are most commonly discovered following the investigation of elevated liver enzyme levels or during a routine screening of high-risk individuals. Testing is not able to distinguish between acute and chronic infections. Diagnosis in the infant is difficult as maternal antibodies may persist for up to 18 months.

Serology

Hepatitis C testing typically begins with blood testing to detect the presence of antibodies to the HCV, using an enzyme immunoassay. If this test is positive, a confirmatory test is then performed to verify the immunoassay and to determine the viral load. A recombinant immunoblot assay is used to verify the immunoassay and the viral load is determined by an HCV RNA polymerase chain reaction. If there is no RNA and the immunoblot is positive, it means that the person tested had a previous infection but cleared it either with treatment or spontaneously; if the immunoblot is negative, it means that the immunoassay was wrong. It takes about 6–8 weeks following infection before the immunoassay will test positive. A number of tests are available as point of care testing which means that results are available within 30 minutes.

Liver enzymes are variable during the initial part of the infection and on average begin to rise at seven weeks after infection. The elevation of liver enzymes does not closely follow disease severity.

There are reports of negative plasma PCR for the viral genome with positive PCR for the viral genome within peripheral blood monocytes of liver cells. This condition has been termed occult HCV infection and it was first recognized in 2004.

Biopsy

Liver biopsies are used to determine the degree of liver damage present; however, there are risks from the procedure. The typical changes seen are lymphocytes within the parenchyma, lymphoid follicles in portal triad, and changes to the bile ducts. There are a number of blood tests available that try to determine the degree of hepatic fibrosis and alleviate the need for biopsy.

Screening

It is believed that only 5–50% of those infected in the United States and Canada are aware of their status. Testing is recommended for those at high risk, which includes injection drug users, those who have received blood transfusions before 1992, those who have been in jail, those on long term hemodialysis, and those with tattoos. Screening is also recommended in those with elevated liver enzymes, as this is frequently the only sign of chronic hepatitis. Routine screening is not currently recommended in the United States. In 2012, the U.S. Centers for Disease Control and Prevention (CDC) added a recommendation for a single screening test for those born between 1945 and 1965. In Canada one time screening is recommended for those born between 1945 and 1975.

Prevention

As of 2016, no approved vaccine protects against contracting hepatitis C. A combination of harm reduction strategies, such as the provision of new needles and syringes and treatment of substance use, decreases the risk of hepatitis C in intravenous drug users by about 75%. The screening of blood donors is important at a national level, as is adhering to universal precautions within healthcare facilities. In countries where there is an insufficient supply of sterile syringes, medications should be given orally rather than via injection (when possible).

Treatment

HCV induces chronic infection in 80% of infected persons. Approximately 95% of these clear with treatment. In rare cases, infection can clear without treatment. Those with chronic hepatitis C are advised to avoid alcohol and medications toxic to the liver. They should also be vaccinated against hepatitis A and hepatitis B due to the increased risk if also infected. Use of acetaminophen is generally considered safe at reduced doses. Nonsteroidal anti-inflammatory drugs (NSAIDs) are not recommended in those with advanced liver disease due to an increased risk of bleeding. Ultrasound surveillance for hepatocellular carcinoma is recommended in those with accompanying cirrhosis. Coffee consumption has been associated with a slower rate of liver scarring in those infected with HCV.

Medications

Treatment with antiviral medication is recommended in all people with proven chronic hepatitis C who are not at high risk of dying from other causes. People with the highest complication risk should be treated first, with the risk of complications based on the degree of liver scarring. The initial recommended treatment depends on the type of hepatitis C virus, if the person has received previous hepatitis C treatment, and whether or not a person has cirrhosis. Direct-acting antivirals (DAAs) may reduce the number of the infected people.

No prior treatment

  • HCV genotype 1a (no cirrhosis): 8 weeks of glecaprevir/pibrentasvir or ledipasvir/sofosbuvir (the latter for people who do not have HIV/AIDS, are not African-American, and have less than 6 million HCV viral copies per milliliter of blood) or 12 weeks of elbasvir/grazoprevir, ledipasvir/sofosbuvir, or sofosbuvir/velpatasvir. Sofosbuvir with either daclatasvir or simeprevir may also be used.
  • HCV genotype 1a (with compensated cirrhosis): 12 weeks of elbasvir/grazoprevir, glecaprevir/pibrentasvir, ledipasvir/sofosbuvir, or sofosbuvir/velpatasvir. An alternative treatment regimen of elbasvir/grazoprevir with weight-based ribavirin for 16 weeks can be used if the HCV is found to have antiviral resistance mutations against NS5A protease inhibitors.
  • HCV genotype 1b (no cirrhosis): 8 weeks of glecaprevir/pibrentasvir or ledipasvir/sofosbuvir (with the aforementioned limitations for the latter as above) or 12 weeks of elbasvir/grazoprevir, ledipasvir/sofosbuvir, or sofosbuvir/velpatasvir. Alternative regimens include 12 weeks of ombitasvir/paritaprevir/ritonavir with dasabuvir or 12 weeks of sofosbuvir with either daclatasvir or simeprevir.
  • HCV genotype 1b (with compensated cirrhosis): 12 weeks of elbasvir/grazoprevir, glecaprevir/pibrentasvir, ledipasvir/sofosbuvir, or sofosbuvir/velpatasvir. A 12-week course of paritaprevir/ritonavir/ombitasvir with dasabuvir may also be used.
  • HCV genotype 2 (no cirrhosis): 8 weeks of glecaprevir/pibrentasvir or 12 weeks of sofosbuvir/velpatasvir. Alternatively, 12 weeks of sofosbuvir/daclatasvir can be used.
  • HCV genotype 2 (with compensated cirrhosis): 12 weeks of sofosbuvir/velpatasvir or glecaprevir/pibrentasvir. An alternative regimen of sofosbuvir/daclatasvir can be used for 16–24 weeks.
  • HCV genotype 3 (no cirrhosis): 8 weeks of glecaprevir/pibrentasvir or 12 weeks of sofosbuvir/velpatasvir or sofosbuvir and daclatasvir.
  • HCV genotype 3 (with compensated cirrhosis): 12 weeks of glecaprevir/pibrentasvir, sofosbuvir/velpatasvir, or if certain antiviral mutations are present, 12 weeks of sofosbuvir/velpatasvir/voxilaprevir (when certain antiviral mutations are present), or 24 weeks of sofosbuvir and daclatasvir.
  • HCV genotype 4 (no cirrhosis): 8 weeks of glecaprevir/pibrentasvir or 12 weeks of sofosbuvir/velpatasvir, elbasvir/grazoprevir, or ledipasvir/sofosbuvir. A 12-week regimen of ombitasvir/paritaprevir/ritonavir is also acceptable in combination with weight-based ribavirin.
  • HCV genotype 4 (with compensated cirrhosis): A 12-week regimen of sofosbuvir/velpatasvir, glecaprevir/pibrentasavir, elbasvir/grazoprevir, or ledipasvir/sofosbuvir is recommended. A 12-week course of ombitasvir/paritaprevir/ritonavir with weight-based ribavirin is an acceptable alternative.
  • HCV genotype 5 or 6 (with or without compensated cirrhosis): If no cirrhosis is present, then 8 weeks of glecaprevir/pibrentasvir is recommended. If cirrhosis is present, then a 12-week course of glecaprevir/pibrentasvir, sofosbuvir/velpatasvir, or ledipasvir/sofosbuvir is warranted.
Chronic infection can be cured about 95% of the time with recommended treatment in 2017. Getting access to these treatments however can be expensive. The combination of sofosbuvir, velpatasvir, and voxilaprevir may be used in those who have previously been treated with sofosbuvir or other drugs that inhibit NS5A and were not cured.

Prior to 2011, treatments consisted of a combination of pegylated interferon alpha and ribavirin for a period of 24 or 48 weeks, depending on HCV genotype. This produces cure rates of between 70 and 80% for genotype 2 and 3, respectively, and 45 to 70% for genotypes 1 and 4. Adverse effects with these treatments were common, with half of people getting flu-like symptoms and a third experiencing emotional problems. Treatment during the first six months is more effective than once hepatitis C has become chronic. In those with chronic hepatitis B, treatment for hepatitis C results in reactivation of hepatitis B in about 25%.

Surgery

Cirrhosis due to hepatitis C is a common reason for liver transplantation though the virus usually (80–90% of cases) recurs afterwards. Infection of the graft leads to 10–30% of people developing cirrhosis within five years. Treatment with pegylated interferon and ribavirin post-transplant decreases the risk of recurrence to 70%. A 2013 review found unclear evidence regarding if antiviral medication was useful if the graft became reinfetcted.

Alternative medicine

Several alternative therapies are claimed by their proponents to be helpful for hepatitis C including milk thistle, ginseng, and colloidal silver. However, no alternative therapy has been shown to improve outcomes in hepatitis C, and no evidence exists that alternative therapies have any effect on the virus at all.

Prognosis

Disability-adjusted life year for hepatitis C in 2004 per 100,000 inhabitants 
 

The responses to treatment is measured by sustained viral response (SVR), defined as the absence of detectable RNA of the hepatitis C virus in blood serum for at least 24 weeks after discontinuing the treatment, and rapid virological response (RVR) defined as undetectable levels achieved within four weeks of treatment. Successful treatment decreases the future risk of hepatocellular carcinoma by 75%.

Prior to 2012 sustained response occurs in about 40–50% in people with HCV genotype 1 given 48 weeks of treatment. A sustained response is seen in 70–80% of people with HCV genotypes 2 and 3 with 24 weeks of treatment. A sustained response occurs about 65% in those with genotype 4 after 48 weeks of treatment. The evidence for treatment in genotype 6 disease is sparse and what evidence there is supports 48 weeks of treatment at the same doses used for genotype 1 disease.

Epidemiology

Prevalence of hepatitis C worldwide in 1999
 
It is estimated that 143 million people (2%) of people globally are living with chronic hepatitis C. About 3–4 million people are infected per year, and more than 350,000 people die yearly from hepatitis C-related diseases. During 2010 it is estimated that 16,000 people died from acute infections while 196,000 deaths occurred from liver cancer secondary to the infection. Rates have increased substantially in the 20th century due to a combination of intravenous drug abuse and reused but poorly sterilized medical equipment.

Rates are high (>3.5% population infected) in Central and East Asia, North Africa and the Middle East, they are intermediate (1.5%-3.5%) in South and Southeast Asia, sub-Saharan Africa, Andean, Central and Southern Latin America, Caribbean, Oceania, Australasia and Central, Eastern and Western Europe; and they are low (<1 .5="" america.="" america="" and="" asia-pacific="" in="" latin="" north="" p="" tropical="">

Among those chronically infected, the risk of cirrhosis after 20 years varies between studies but has been estimated at ~10–15% for men and ~1–5% for women. The reason for this difference is not known. Once cirrhosis is established, the rate of developing hepatocellular carcinoma is ~1–4% per year. Rates of new infections have decreased in the Western world since the 1990s due to improved screening of blood before transfusion.

In the United States, about 2% of people have chronic hepatitis C. In 2014, an estimated 30,500 new acute hepatitis C cases occurred (0.7 per 100,000 population), an increase from 2010–2012. The number of deaths from hepatitis C has increased to 15,800 in 2008 having overtaken HIV/AIDS as a cause of death in the USA in 2007. In 2014 it was the single greatest cause of infectious death in the United States. This mortality rate is expected to increase, as those infected by transfusion before HCV testing become apparent. In Europe the percentage of people with chronic infections has been estimated to be between 0.13 and 3.26%.

In England about 160,000 people are chronically infected. Between 2006 and 2011 28,000, about 3%, received treatment. About half of people using a needle exchange in London in 2017/8 tested positive for hepatitis C of which half were unaware of they had it. As part of a bid to eradicate hepatitis C by 2025 NHS England conducted a large procurement exercise in 2019. Merck Sharp & Dohme, Gilead Sciences, and Abbvie were awarded contracts, which, together, are worth up to £1 billion over five years.

The total number of people with this infection is higher in some countries in Africa and Asia. Countries with particularly high rates of infection include Egypt (22%), Pakistan (4.8%) and China (3.2%). It is believed that the high prevalence in Egypt is linked to a now-discontinued mass-treatment campaign for schistosomiasis, using improperly sterilized glass syringes.

History

In the mid-1970s, Harvey J. Alter, Chief of the Infectious Disease Section in the Department of Transfusion Medicine at the National Institutes of Health, and his research team demonstrated how most post-transfusion hepatitis cases were not due to hepatitis A or B viruses. Despite this discovery, international research efforts to identify the virus, initially called non-A, non-B hepatitis (NANBH), failed for the next decade. In 1987, Michael Houghton, Qui-Lim Choo, and George Kuo at Chiron Corporation, collaborating with Daniel W. Bradley at the Centers for Disease Control and Prevention, used a novel molecular cloning approach to identify the unknown organism and develop a diagnostic test. In 1988, Alter confirmed the virus by verifying its presence in a panel of NANBH specimens. In April 1989, the discovery of HCV was published in two articles in the journal Science. The discovery led to significant improvements in diagnosis and improved antiviral treatment. In 2000, Drs. Alter and Houghton were honored with the Lasker Award for Clinical Medical Research for "pioneering work leading to the discovery of the virus that causes hepatitis C and the development of screening methods that reduced the risk of blood transfusion-associated hepatitis in the U.S. from 30% in 1970 to virtually zero in 2000."

Chiron filed for several patents on the virus and its diagnosis. A competing patent application by the CDC was dropped in 1990 after Chiron paid $1.9 million to the CDC and $337,500 to Bradley. In 1994, Bradley sued Chiron, seeking to invalidate the patent, have himself included as a coinventor, and receive damages and royalty income. He dropped the suit in 1998 after losing before an appeals court.

Society and culture

World Hepatitis Day, held on July 28, is coordinated by the World Hepatitis Alliance. The economic costs of hepatitis C are significant both to the individual and to society. In the United States the average lifetime cost of the disease was estimated at 33,407 USD in 2003 with the cost of a liver transplant as of 2011 costing approximately 200,000 USD. In Canada the cost of a course of antiviral treatment is as high as 30,000 CAD in 2003, while the United States costs are between 9,200 and 17,600 in 1998 USD. In many areas of the world, people are unable to afford treatment with antivirals as they either lack insurance coverage or the insurance they have will not pay for antivirals. In the English National Health Service treatment rates for hepatitis C are higher among wealthier groups per 2010–2012 data. Spanish anaesthetist Juan Maeso infected 275 patients between 1988 and 1997 as he used the same needles to give both himself and the patients opioids. For this he was jailed.

Special populations

Children and pregnancy

Compared with adults, infection in children is much less well understood. Worldwide the prevalence of hepatitis C virus infection in pregnant women and children has been estimated to 1–8% and 0.05–5% respectively. The vertical transmission rate has been estimated to be 3–5% and there is a high rate of spontaneous clearance (25–50%) in the children. Higher rates have been reported for both vertical transmission (18%, 6–36% and 41%). and prevalence in children (15%).

In developed countries transmission around the time of birth is now the leading cause of HCV infection. In the absence of virus in the mother's blood transmission seems to be rare. Factors associated with an increased rate of infection include membrane rupture of longer than 6 hours before delivery and procedures exposing the infant to maternal blood. Cesarean sections are not recommended. Breastfeeding is considered safe if the nipples are not damaged. Infection around the time of birth in one child does not increase the risk in a subsequent pregnancy. All genotypes appear to have the same risk of transmission. 

HCV infection is frequently found in children who have previously been presumed to have non-A, non-B hepatitis and cryptogenic liver disease. The presentation in childhood may be asymptomatic or with elevated liver function tests. While infection is commonly asymptomatic both cirrhosis with liver failure and hepatocellular carcinoma may occur in childhood.

Immunosuppressed

The rate of hepatitis C in immunosuppressed people is higher. This is particularly true in those with human immunodeficiency virus infection, recipients of organ transplants, and those with hypogammaglobulinemia. Infection in these people is associated with an unusually rapid progression to cirrhosis. People with stable HIV who never received medication for HCV, may be treated with a combination of peginterferon plus ribavirin with caution to the possible side effects.

Research

As of 2011, there are about one hundred medications in development for hepatitis C. These include vaccines to treat hepatitis, immunomodulators, and cyclophilin inhibitors, among others. These potential new treatments have come about due to a better understanding of the hepatitis C virus. There are a number of vaccines under development and some have shown encouraging results.

The combination of sofosbuvir and velpatasvir in one trial (reported in 2015) resulted in cure rates of 99%. More studies are needed to investigate the role of the preventative antiviral medication against HCV recurrence after transplantation.

Animal models

One barrier to finding treatments for hepatitis C is the lack of a suitable animal model. Despite moderate success, current research highlights the need for pre-clinical testing in mammalian systems such as mouse, particularly for the development of vaccines in poorer communities. Currently, chimpanzees remain the available living system to study, yet their use has ethical concerns and regulatory restrictions. While scientists have made use of human cell culture systems such as hepatocytes, questions have been raised about their accuracy in reflecting the body's response to infection.

One aspect of hepatitis research is to reproduce infections in mammalian models. A strategy is to introduce liver tissues from humans into mice, a technique known as xenotransplantation. This is done by generating chimeric mice, and exposing the mice HCV infection. This engineering process is known to create humanized mice, and provide opportunities to study hepatitis C within the 3D architectural design of the liver and evaluating antiviral compounds. Alternatively, generating inbred mice with susceptibility to HCV would simplify the process of studying mouse models.

Russia and weapons of mass destruction

From Wikipedia, the free encyclopedia
 
Soviet Union
Russian Federation
Location of Soviet Union Russian Federation
Nuclear program start date1943
First nuclear weapon testAugust 29, 1949
First fusion weapon testAugust 12, 1953
Last nuclear testOctober 24, 1990
Largest yield test50 Mt (210 PJ) (Tsar Bomba, October 30, 1961)
Total tests715 detonations
Peak stockpile68,000 warheads (1990)
Current stockpile (usable and not)6,500
Current strategic arsenal1,600
Cumulative strategic arsenal in megatonnage663.5-801.5 (2016.est)
(Variability occurs because of uncertainty about SS-18 yields) 
Maximum missile rangeIntercontinental up to 16,000 kilometers
NPT partyYes (1968, one of five recognized powers)

According to the Federation of American Scientists, an organization that assesses nuclear weapon stockpiles, as of 2018, the Russian Federation possesses 7,850 total nuclear warheads, of which 1,600 are strategically operational. This is in large part due to the special bomber counting rules allowed by the New START treaty, which counts each strategic nuclear bomber as one warhead irrespective of the number of warheads—gravity bombs and/or cruise missiles carried by the aircraft. The figures are, by necessity, only estimates because "the exact number of nuclear weapons in each country's possession is a closely held national secret." In addition to nuclear weapons, Russia declared an arsenal of 39,967 tons of chemical weapons in 1997. The Soviet Union ratified the Geneva Protocol on April 5, 1928 with reservations. The reservations were dropped on January 18, 2001. Russia is also party to the Biological Weapons Convention and the Chemical Weapons Convention. The Soviet Union had a peak stockpile of 45,000 nuclear warheads in 1986. It is estimated that from 1949 to 1991 the Soviet Union produced approximately 55,000 nuclear warheads.

Nuclear weapons

History

Post-Soviet era

At the dissolution of the Soviet Union in 1991, Soviet nuclear weapons were deployed in four of the new republics: Russia, Ukraine, Belarus and Kazakhstan. In May 1992, these four states signed the Lisbon Protocol, agreeing to join the Treaty on the Non-Proliferation of Nuclear Weapons, with Russia the successor state to the Soviet Union as a nuclear state, and the other three states joining as non-nuclear states. 

Ukraine agreed to give up its weapons to Russia, in exchange for guarantees of Ukrainian territory from Russia, the United Kingdom, and the United States, known as the Budapest Memorandum on Security Assurances. China and France also made statements in support of the memorandum.

Nuclear arsenal of Russia

The exact number of nuclear warheads is a state secret and is therefore a matter of guesswork. The Federation of American Scientists estimates that Russia possesses 6,500 nuclear weapons, while the United States has 6,185; Russia and the U.S. each have 1,600 active deployed strategic nuclear warheads.

The RS-28 Sarmat (Russian: РС-28 Сармат; NATO reporting name: SATAN 2), is a Russian liquid-fueled, MIRV-equipped, super-heavy thermonuclear armed intercontinental ballistic missile in development by the Makeyev Rocket Design Bureau from 2009, intended to replace the previous R-36 missile. Its large payload would allow for up to 10 heavy warheads or 15 lighter ones or up to 24 hypersonic glide vehicles Yu-71, or a combination of warheads and massive amounts of countermeasures designed to defeat anti-missile systems; it was heralded by the Russian military as a response to the U.S. Prompt Global Strike.

In 2015, information emerged that Russia may be developing a new nuclear torpedo, up to 100 megatons, the Status-6 Ocean Multipurpose System, codenamed "Kanyon" by Pentagon officials. This weapon is designed to create a tsunami wave up to 500m tall that will radioactively contaminate a wide area on an enemy coasts with cobalt-60, and to be immune to anti-missile defense systems such as laser weapons and railguns that might disable an ICBM. Two potential carrier submarines, the Project 09852 Belgorod, and the Project 09851 Khabarovsk, are new boats laid down in 2012 and 2014 respectively. Status 6 appears to be a deterrent weapon of last resort. It appears to be a torpedo-shaped robotic mini-submarine, that can travel at speeds of 185 km/h (100 kn). More recent information suggests a top speed of 100 km/h (54 kn), with a range of 10,000 km (6,200 mi) and a depth maximum of 1,000 m (3,300 ft). This underwater drone is cloaked by stealth technology to elude acoustic tracking devices.

During an annual state-of-the-nation address given on March 1, 2018, President Vladimir Putin publicly claimed that Russia was now in possession of several new classes of nuclear weapons, including some with capabilities previously speculated to exist. Putin discussed several new or upgraded weapons, including an intercontinental missile known as the Avangard capable of performing sharp maneuvers while traveling at 20 times the speed of sound making it "absolutely invulnerable for any missile defense system."  Putin also discussed the existence of a nuclear powered underwater torpedo and a nuclear powered cruise missile, both with effectively unlimited range. He also discussed that Russia had tested a new class of traditional ICBM called the Sarmat, which expanded upon the range and carrying capability of the Soviet-era Satan ICBM. Animations of these weapons were shown in front of the live and televised audience, and Putin suggested that an online poll be conducted to give them official public names.

Nuclear weapons in Russian military doctrine

According to a Russian military doctrine stated in 2010, nuclear weapons could be used by Russia "in response to the use of nuclear and other types of weapons of mass destruction against it or its allies, and also in case of aggression against Russia with the use of conventional weapons when the very existence of the state is threatened". Most military analysts believe that, in this case, Russia would pursue an 'escalate to de-escalate’ strategy, initiating limited nuclear exchange to bring adversaries to the negotiating table. Russia will also threaten nuclear conflict to discourage initial escalation of any major conventional conflict.

Nuclear proliferation

After the Korean War, the Soviet Union transferred nuclear technology and weapons to the People's Republic of China as an adversary of the United States and NATO. According to Ion Mihai Pacepa, "Khrushchev's nuclear-proliferation process started with Communist China in April 1955, when the new ruler in the Kremlin consented to supply Beijing a sample atomic bomb and to help with its mass production. Subsequently, the Soviet Union built all the essentials of China's new military nuclear industry."

Russia is one of the five "Nuclear Weapons States" (NWS) under the Treaty on the Non-Proliferation of Nuclear Weapons (NPT), which Russia ratified (as the Soviet Union) in 1968. 

Following the dissolution of the Soviet Union in 1991, a number of Soviet-era nuclear warheads remained on the territories of Belarus, Ukraine, and Kazakhstan. Under the terms of the Lisbon Protocol to the NPT, and following the 1995 Trilateral Agreement between Russia, Belarus, and the USA, these were transferred to Russia, leaving Russia as the sole inheritor of the Soviet nuclear arsenal. It is estimated that the Soviet Union had approximately 45,000 nuclear weapons stockpiled at the time of its collapse.

The collapse of the Soviet Union allowed for a warming of relations with NATO. Fears of a nuclear holocaust lessened. In September 1997, the former secretary of the Russian Security Council Alexander Lebed claimed 100 "suitcase sized" nuclear weapons were unaccounted for. He said he was attempting to inventory the weapons when he was fired by President Boris Yeltsin in October 1996. Indeed, several US politicians have expressed worries and promised legislation addressing the threat.

In 2002, the United States and Russia agreed to reduce their stockpiles to not more than 2,700 warheads each in the SORT treaty. In 2003, the US rejected Russian proposals to further reduce each nation's nuclear stockpiles to 1,500. Russia, in turn, refused to discuss reduction of tactical nuclear weapons.

After U.S. President George W. Bush withdrew from the 1972 Anti-Ballistic Missile Treaty, Russia responded by building-up their nuclear capabilities, in such a way as to counterbalance U.S. capabilities.

Most analysts agree that Russia’s nuclear strategy under Putin eventually brought it into violation of the 1987 Intermediate-Range Nuclear Forces Treaty (although) this is not confirmed). Because of this, U.S. President Donald Trump announced the U.S. would no longer consider itself bound by the treaty’s provisions, raising nuclear tensions between the two powers.

There were allegations that Russia contributed to North Korean nuclear program, selling it the equipment for the safe storage and transportation of nuclear materials. Nevertheless, Russia condemned North Korean nuclear tests since then.

According to high-ranking Russian SVR defector Sergei Tretyakov, a businessman told him that he keeps his own nuclear bomb at his dacha outside Moscow.

Nuclear sabotage allegations from Russia

The highest-ranking GRU defector Stanislav Lunev described alleged Soviet plans for using tactical nuclear weapons for sabotage against the United States in the event of war. He described Soviet-made suitcase nukes identified as RA-115s (or RA-115-01s for submersible weapons) which weigh from fifty to sixty pounds (23 kg - 27 kg). These portable bombs can last for many years if wired to an electric source. "In case there is a loss of power, there is a battery backup. If the battery runs low, the weapon has a transmitter that sends a coded message – either by satellite or directly to a GRU post at a Russian embassy or consulate.".

Lunev was personally looking for hiding places for weapons caches in the Shenandoah Valley area. He said that "it is surprisingly easy to smuggle nuclear weapons into the US" either across the Mexican border or using a small transport missile that can slip though undetected when launched from a Russian airplane. Searches of the areas identified by Lunev – who admits he never planted any weapons in the US – have been conducted, "but law-enforcement officials have never found such weapons caches, with or without portable nuclear weapons" in the US.

Biological weapons

Soviet program of biological weapons was initially developed by the Ministry of Defense of the Soviet Union (between 1945 and 1973).

The Soviet Union signed the Biological Weapons Convention on April 10, 1972 and ratified the treaty on March 26, 1975. However, it subsequently augmented its biowarfare programs. After 1975, the program of biological weapons was run primarily by the "civilian" Biopreparat agency, although it also included numerous facilities run by the Soviet Ministry of Defense, Ministry of Agriculture, Ministry of Chemical Industry, Ministry of Health, and Soviet Academy of Sciences.

According to Ken Alibek, who was deputy-director of Biopreparat, the Soviet biological weapons agency, and who defected to the United States in 1992, weapons were developed in labs in isolated areas of the Soviet Union including mobilization facilities at Omutininsk, Penza and Pokrov and research facilities at Moscow, Stirzhi and Vladimir. These weapons were tested at several facilities most often at "Rebirth Island" (Vozrozhdeniya) in the Aral Sea by firing the weapons into the air above monkeys tied to posts, the monkeys would then be monitored to determine the effects. According to Alibek, although Soviet offensive program was officially ended in 1992, Russia may be still involved in the activities prohibited by BWC.

In 1993, the story about the Sverdlovsk anthrax leak was published in Russia. The incident occurred when spores of anthrax were accidentally released from a military facility in the city of Sverdlovsk (formerly, and now again, Yekaterinburg) 1,500 km (930 mi) east of Moscow on April 2, 1979. The ensuing outbreak of the disease resulted in 94 people becoming infected, 64 of whom died over a period of six weeks.

Chemical weapons

Russia signed the Chemical Weapons Convention on January 13, 1993, and ratified it on November 5, 1997. Russia declared an arsenal of 39,967 tons of chemical weapons in 1997 consisting of:
Ratification was followed by three years of inaction on chemical weapons destruction because of the August 1998 Russian financial crisis

Russia met its treaty obligations by destroying 1% of its chemical agents by the Chemical Weapons Convention's 2002 deadline, but requested technical and financial assistance and extensions on the deadlines of 2004 and 2007 due to the environmental challenges of chemical disposal. This extension procedure spelled out in the treaty has been utilized by other countries, including the United States. The extended deadline for complete destruction (April 2012) was not met. As of October 2011, Russia has destroyed 57% of its stockpile. Russia also destroyed all of its declared Category 2 (10,616 MTs) and Category 3 chemicals.

Russia has stored its chemical weapons (or the required chemicals) which it declared within the CWC at 8 locations: in Gorny (Saratov Oblast) (2.9% of the declared stockpile by mass) and Kambarka (Udmurt Republic) (15.9%) stockpiles already have been destroyed. In Shchuchye (Kurgan Oblast) (13.6%), Maradykovsky (Kirov Oblast) (17.4%) and Leonidovka (Penza Oblast) (17.2%) destruction takes place, while installations are under construction in Pochep (Bryansk Oblast) (18.8%) and Kizner (Udmurt Republic) (14.2%).

On 27 September 2017, OPCW announced that Russia had destroyed its entire chemical weapons stockpile.

Novichok agents

A range of Novichok agents were developed and tested in the 1970s and 1980s, but the intended Novichok weapons production site at the Pavlodar Chemical Plant in Soviet Kazakhstan was still under construction when it was decided to demolish the chemical weapons building in 1987 in view of the forthcoming Chemical Weapons Convention.

In March 2018, former GRU agent Sergei Skripal and his daughter were poisoned in Salisbury, United Kingdom by a chemical agent later confirmed to be Novichok. The incident raised new controversy over Russia's potential production and use of chemical weapons, with the United Kingdom accusing the Russian government or rogue Russian agents of orchestrating the attack, a claim Russia repeatedly denied.

Disposal facilities

Russia has a number of factories for destruction of its chemical weapons arsenal: Gorny in Saratov Oblast, Kambarka in Udmurtia, Leonidovka Penza Oblast, Maradykovsky in Kirov Oblast, Shchuchye in Kurgan Oblast and the latest one Pochep in the Bryansk Oblast 70 km from the border with Ukraine, built with funds from Italy in accordance with the agreement signed between the two countries. The last Russian chemical disposal facility in Kizner, Udmurtia, was opened on December 2013.

United States and weapons of mass destruction

From Wikipedia, the free encyclopedia
 
United States
Location of United States
Nuclear program start date21 October 1939
First nuclear weapon test16 July 1945
First fusion weapon test1 November 1952
Last nuclear test23 September 1992
Largest yield test15 Mt (1 March 1954)
Total tests1,054 detonations
Peak stockpile32,040 warheads (1967)
Current stockpile (usable and not)6,185 total6,185
(2019)
Current strategic arsenal1,600 methods of delivery (including ICBMs, Bombers, and including MIRVed warheads on SLBMs)
(2019)
Cumulative strategic arsenal in megatonnage≈1430 (2014)
Maximum missile range13,000 km (8,078 mi) (land)
12,000 km (7,456 mi) (sub)
NPT partyYes (1968, one of five recognized powers)

The United States is known to have possessed three types of weapons of mass destruction: nuclear weapons, chemical weapons, and biological weapons. The U.S. is the only country to have used nuclear weapons in combat, when it detonated two atomic bombs over the Japanese cities of Hiroshima and Nagasaki during World War II. It had secretly developed the earliest form of the atomic weapon during the 1940s under the title "Manhattan Project". The United States pioneered the development of both the nuclear fission and hydrogen bombs (the latter involving nuclear fusion). It was the world's first and only nuclear power for four years (1945–1949), until the Soviet Union managed to produce its own nuclear weapon. The United States has the second largest number of nuclear weapons in the world, after Russia.

Nuclear weapons

U.S. nuclear warhead stockpiles, 1945-2002.
 
Nuclear weapons have been used twice in combat: two nuclear weapons were used by the United States against Japan during World War II in the atomic bombings of Hiroshima and Nagasaki. Altogether, the two bombings killed 105,000 people and injured thousands more while devastating hundreds or thousands of military bases, factories, and cottage industries

The U.S. conducted an extensive nuclear testing program.1054 tests were conducted between 1945 and 1992. The exact number of nuclear devices detonated is unclear because some tests involved multiple devices while a few failed to explode or were designed not to create a nuclear explosion. The last nuclear test by the United States was on September 23, 1992; the U.S. has signed but not ratified the Comprehensive Nuclear-Test-Ban Treaty.

Currently, the United States nuclear arsenal is deployed in three areas:
The United States is one of the five "Nuclear Weapons States" under the Treaty on the Non-Proliferation of Nuclear Weapons, which the U.S. ratified in 1968. On October 13, 1999, the U.S. Senate rejected ratification of the Comprehensive Test Ban Treaty, having previously ratified the Partial Test Ban Treaty in 1963. The U.S. has not, however, tested a nuclear weapon since 1992, though it has tested many non-nuclear components and has developed powerful supercomputers in an attempt to duplicate the knowledge gained from testing without conducting the actual tests themselves. 

In the early 1990s, the U.S. stopped developing new nuclear weapons and now devotes most of its nuclear efforts into stockpile stewardship, maintaining and dismantling its now-aging arsenal. The administration of George W. Bush decided in 2003 to engage in research towards a new generation of small nuclear weapons, especially "earth penetrators". The budget passed by the United States Congress in 2004 eliminated funding for some of this research including the "bunker-busting or earth-penetrating" weapons. 

The exact number of nuclear weapons possessed by the United States is difficult to determine. Different treaties and organizations have different criteria for reporting nuclear weapons, especially those held in reserve, and those being dismantled or rebuilt:
  • In its Strategic Arms Reduction Treaty (START) declaration for 2003, the U.S. listed 5968 deployed warheads as defined by START rules.
  • The exact number as of September 30, 2009, was 5,113 warheads, according to a U.S. fact sheet released May 3, 2010.
In 2002, the United States and Russia agreed in the SORT treaty to reduce their deployed stockpiles to not more than 2,200 warheads each. In 2003, the U.S. rejected Russian proposals to further reduce both nation's nuclear stockpiles to 1,500 each. In 2007, for the first time in 15 years, the United States built new warheads. These replaced some older warheads as part of the Minuteman III upgrade program. 2007 also saw the first Minuteman III missiles removed from service as part of the drawdown. Overall, stockpiles and deployment systems continue to decline in number under the terms of the New START treaty. 

In 2014, Bulletin of the Atomic Scientists released a report, stating that there are a total of 2,530 warheads kept in reserve, and 2,120 actively deployed. Of the warheads actively deployed, the number of strategic warheads rests at 1,920 (subtracting 200 tactical B61s as part of Nato nuclear weapon sharing arrangements). The amount of warheads being actively disabled rests at about 2,700 warheads, which brings the total United States inventory to about 7,400 warheads.

Land-based ICBMs

A Minuteman III ICBM test launch.
 
The U.S. Air Force currently operates 400 Minuteman III ICBMs, located primarily in the northern Rocky Mountain states and the Dakotas. Peacekeeper missiles were phased out of the Air Force inventory in 2005. All USAF Minuteman II missiles were destroyed in accordance with the START treaty and their launch silos imploded and buried then sold to the public under the START II. The U.S. goal under the SORT treaty was to reduce from 1,600 warheads deployed on over 500 missiles in 2003 to 500 warheads on 450 missiles in 2012. The first Minuteman III were removed under this plan in 2007 while, at the same time, the warheads deployed on Minuteman IIIs began to be upgraded from smaller W62s to larger W87s from decommissioned Peacekeeper missiles.

Air-based delivery systems

The U.S. Air Force also operates a strategic nuclear bomber fleet. The bomber force consists of 36 nuclear-armed B-52 Stratofortresses, and 20 B-2 Spirits. All 64 B-1s were retrofitted to operate in a solely conventional mode by 2007 and thus don't count as nuclear platforms.

In addition to this, the U.S. military can also deploy smaller tactical nuclear weapons either through cruise missiles or with conventional fighter-bombers. The U.S. maintains about 400 nuclear gravity bombs capable of use by F-15, F-16, and F-35. Some 350 of these bombs are deployed at seven airbases in six European NATO countries; of these, 180 tactical B61 nuclear bombs fall under a nuclear sharing arrangement.

Sea-based Ballistic Missiles

The U.S. Navy currently has 18 Ohio-class submarines deployed, of which 14 are ballistic missile submarines. Each submarine is equipped with a maximum complement of 24 Trident II missiles. Approximately 12 U.S. attack submarines were equipped to launch nuclear Tomahawk missiles, but these weapons were removed from service by 2013.

The number of Deployed and Non-Deployed SLBMs on the Ohio-Class SSBNs as of 2018 is 280, of which 203 SLBMs are deployed.

Biological weapons

The United States offensive biological weapons program was instigated by President Franklin Roosevelt and the U.S. Secretary of War in October 1941. Research occurred at several sites. A production facility was built at Terre Haute, Indiana but testing with a benign agent demonstrated contamination of the facility so no production occurred during World War II. A more advanced production facility was constructed in Pine Bluff, Arkansas, which began producing biological agents in 1954. Fort Detrick, Maryland later became a production facility as well as a research site. The U.S. developed anti-personnel and anti-crop biological weapons. Several deployment systems were developed including aerial spray tanks, aerosol spray canisters, grenades, rocket warheads and cluster bombs.

E120 biological bomblet, developed before the U.S. ratified the Biological Weapons Convention.
 
In mid-1969, the UK and the Warsaw Pact, separately, introduced proposals to the UN to ban biological weapons, which would lead to a treaty in 1972. The U.S. cancelled its offensive biological weapons program by executive order in November 1969 (microorganisms) and February 1970 (toxins) and ordered the destruction of all offensive biological weapons, which occurred between May 1971 and February 1973. The U.S. ratified the Geneva Protocol on January 22, 1975. The U.S. ratified the Biological Weapons Convention (BWC) which came into effect in March 1975.

Negotiations for a legally binding verification protocol to the BWC proceeded for years. In 2001, negotiations ended when the Bush administration rejected an effort by other signatories to create a protocol for verification, arguing that it could be abused to interfere with legitimate biological research. 

The U.S. Army Medical Research Institute of Infectious Diseases, located in Fort Detrick, Maryland, produces small quantities of biological agents, for use in biological weapons defense research. According to the U.S. government, this research is performed in full accordance with the BWC.

In September 2001, shortly after the September 11 terrorist attacks on the United States, there was a series of mysterious anthrax attacks aimed at U.S. media offices and the U.S. Senate which killed five people. The anthrax used in the attacks was the Ames strain, which was first studied at Fort Detrick and then distributed to other labs around the world.

Chemical weapons

In World War I, the U.S. had its own chemical weapons program, which produced its own chemical munitions, including phosgene and mustard gas. The U.S. only created about 4% of the total chemical weapons produced for that war and just over 1% of the era's most effective weapon, mustard gas. (U.S. troops suffered less than 6% of gas casualties.) Although the U.S. had begun a large-scale production of Lewisite, for use in an offensive planned for early 1919, Lewisite was not deployed during World War I. The United States also created a special unit, the 1st Gas Regiment, which used phosgene in attacks after being deployed to France.

Chemical weapons were not used by the Allies or Germany during World War II for military purposes, but such weapons were deployed to Europe from the United States. In 1943, German bombers attacked the port of Bari in Southern Italy, sinking several American ships – among them John Harvey, which was carrying mustard gas. The presence of the gas was highly classified, and, according to the U.S. military account, "Sixty-nine deaths were attributed in whole or in part to the mustard gas, most of them American merchant seamen" out of 628 mustard gas military casualties. The affair was kept secret at the time and for many years. After the war, the U.S. both participated in arms control talks involving chemical weapons and continued to stockpile them, eventually exceeding 30,000 tons of material. 

Honest John missile warhead cutaway, showing M134 Sarin bomblets (photo c. 1960)
 
After the war, all of the former Allies pursued further research on the three new nerve agents developed by the Nazis: tabun, sarin, and soman. Over the following decades, thousands of American military volunteers were exposed to chemical agents during Cold War testing programs, as well as in accidents. (In 1968, one such accident killed approximately 6,400 sheep when an agent drifted out of Dugway Proving Ground during a test.) The U.S. also investigated a wide range of possible nonlethal, psychobehavioral chemical incapacitating agents including psychedelic indoles such as LSD and marijuana derivatives, as well as several glycolate anticholinergics. One of the anticholinergic compounds, 3-quinuclidinyl benzilate, was assigned the NATO code BZ and was weaponized at the beginning of the 1960s for possible battlefield use. Alleged use of chemical agents by the U.S. in the Korean (1950–53) conflict has never been substantiated.

In late 1969, President Richard Nixon unilaterally renounced the first use of chemical weapons (as well as all methods of biological warfare). He issued a unilateral decree halting production and transport of chemical weapons which remains in effect. From 1967 to 1970 in Operation CHASE, the U.S. disposed of chemical weapons by sinking ships laden with the weapons in the deep Atlantic. The U.S. began to research safer disposal methods for chemical weapons in the 1970s, destroying several thousand tons of mustard gas by incineration and nearly 4,200 tons of nerve agent by chemical neutralization.

The U.S. entered the Geneva Protocol in 1975 (the same time it ratified the Biological Weapons Convention). This was the first operative international treaty on chemical weapons to which the U.S. was party. Stockpile reductions began in the 1980s, with the removal of some outdated munitions and destruction of the entire stock of BZ beginning in 1988. In 1990, destruction of chemical agents stored on Johnston Atoll in the Pacific began, seven years before the Chemical Weapons Convention (CWC) came into effect. In 1986, President Ronald Reagan began removal of the U.S. stockpile of chemical weapons from Germany. In 1991, President George H.W. Bush unilaterally committed the U.S. to destroying all chemical weapons and renounced the right to chemical weapon retaliation. 

In 1993, the U.S. signed the CWC, which required the destruction of all chemical weapon agents, dispersal systems, chemical weapons production facilities by 2012. Both Russia and U.S. missed the CWC's extended deadline of April 2012 to destroy all of their chemical weapons. The United States destroyed 89.75% of the original stockpile of nearly 31,100 metric tons (30,609 long tons) of nerve and mustard agents under the terms of the treaty. Chemical weapons destruction resumed in 2015 with expected completion by 2023. The country's last stockpile is at the Blue Grass Army Depot in Kentucky.

Introduction to entropy

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