Cocaine Research Report
Cocaine Research Report
Cocaine Research Report
Table of Contents
Cocaine Research Report
What is Cocaine?
Why are cocaine users at risk for contracting HIV/AIDS and hepatitis?
Glossary
References
Cocaine Research Report
Describes the latest research findings on cocaine, exploring the scope of abuse in the U.S., its
potential long- and short-term health effects, maternal cocaine use, and treatment approaches.
All materials appearing in the ?Research Reports series are in the public domain and may be
reproduced without permission from NIDA. Citation of the source is appreciated.
What is Cocaine?
Cocaine is a powerfully addictive
stimulant drug. For thousands of
years, people in South America
have chewed and ingested coca
leaves (Erythroxylon coca), the
source of cocaine, for their
stimulant effects.1, 2 The purified
chemical, cocaine hydrochloride, was isolated from the plant more than 100 years ago. In the early
1900s, purified cocaine was the main active ingredient in many tonics and elixirs developed to treat a
wide variety of illnesses. Before the development of synthetic local anesthetic, surgeons used cocaine
1
to block pain. However, research has since shown that cocaine is a powerfully addictive substance
that can alter brain structure and function if used repeatedly.
Photo by ©iStock.com/Rafal Cichawa
Today, cocaine is a Schedule II drug, which means that it has high potential for abuse but can be
administered by a doctor for legitimate medical uses, such as local anesthesia for some eye, ear, and
throat surgeries. Dealers often dilute (or “cut”) it with non-psychoactive substances such as
cornstarch, talcum powder, flour, or baking soda to increase their profits. They may also adulterate
cocaine with other drugs like procaine (a chemically related local anesthetic) or amphetamine (another
, 2
psychoactive stimulant).2 3 Some users combine cocaine with heroin.
People abuse two chemical forms of cocaine: the water-soluble hydrochloride salt and the water-
insoluble cocaine base (or freebase). Users inject or snort the hydrochloride salt, which is a powder.
The base form of cocaine is created by processing the drug with ammonia or sodium bicarbonate
(baking soda) and water, then heating it to remove the hydrochloride to produce a smokable
substance.
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Users primarily administer cocaine orally, intranasally, Photo by DEA/ Cocaine
Photo by DEA
Page 4
In the normal communication process, dopamine is released by a neuron into the synapse (the small
gap between two neurons), where it binds to specialized proteins called dopamine receptors on the
neighboring neuron. By this process, dopamine acts as a chemical messenger, carrying a signal from
neuron to neuron. Another specialized protein called a transporter removes dopamine from the
8
synapse to be recycled for further use.
Drugs of abuse can interfere with this normal communication process. For example, cocaine acts by
binding to the dopamine transporter, blocking the removal of dopamine from the synapse. Dopamine
then accumulates in the synapse to produce an amplified signal to the receiving neurons. This is what
causes the euphoria commonly experienced immediately after taking the drug (see the video "Brain
Reward: Understanding How the Brain Responds to Natural Rewards and Drugs of Abuse").
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Image by NIDA
Page 6
receptor proteins—in the reward pathway, particularly the nucleus accumbens. The glutamate system
may be an opportune target for anti-addiction medication development, with the goal of reversing the
9
cocaine-induced neuroadaptations that contribute to the drive to use the drug.
Although addiction researchers have focused on adaptations in the brain’s reward system, drugs also
affect the brain pathways that respond to stress. Stress can contribute to cocaine relapse, and cocaine
11
use disorders frequently co-occur with stress-related disorders. The stress circuits of the brain are
distinct from the reward pathway, but research indicates that there are important ways that they
overlap. The ventral tegmental area seems to act as a critical integration site in the brain that relays
information about both stress and drug cues to other areas of the brain, including ones that drive
11
cocaine seeking. Animals that have received cocaine repeatedly are more likely to seek the drug in
11
response to stress, and the more of the drug they have taken, the more stress affects this behavior.
Research suggests that cocaine elevates stress hormones, inducing neuroadaptations that further
11
increase sensitivity to the drug and cues associated with it.
Volkow ND, Want G-J, Fowler JS, Tomasi D, Teland F. Addiction: beyond dopamine reward circuitry. Proc Natl
Acad Sci USA. 2011;108(37):15037-15042.
Page 7
Chronic cocaine exposure affects many other areas of the brain too. For example, animal research
indicates that cocaine diminishes functioning in the orbitofrontal cortex (OFC), which appears to
underlie the poor decision-making, inability to adapt to negative consequences of drug use, and lack of
12
self-insight shown by people addicted to cocaine. A study using optogenetic technology, which uses
light to activate specific, genetically-modified neurons, found that stimulating the OFC restores
adaptive learning in animals. This intriguing result suggests that strengthening OFC activity may be a
good therapeutic approach to improve insight and awareness of the consequences of drug use among
13
people addicted to cocaine.
The duration of cocaine’s euphoric effects depend upon the route of administration. The faster the
drug is absorbed, the more intense the resulting high, but also the shorter its duration. Snorting
cocaine produces a relatively slow onset of the high, but it may last from 15 to 30 minutes. In contrast,
15
the high from smoking is more immediate but may last only 5 to 10 minutes.
Short-term physiological effects of cocaine use include constricted blood vessels; dilated pupils; and
16
increased body temperature, heart rate, and blood pressure. Large amounts of cocaine may intensify
the user’s high but can also lead to bizarre, erratic, and violent behavior. Some cocaine users report
2
feelings of restlessness, irritability, anxiety, panic, and paranoia. Users may also experience tremors,
2
vertigo, and muscle twitches.
Severe medical complications can occur with cocaine use. Some of the most frequent are
cardiovascular effects, including disturbances in heart rhythm and heart attacks; neurological effects,
including headaches, seizures, strokes, and coma; and gastrointestinal complications, including
7
abdominal pain and nausea. In rare instances, sudden death can occur on the first use of cocaine or
2
unexpectedly thereafter. Cocaine-related deaths are often a result of cardiac arrest or seizures (see "
Page 8
National Overdose Deaths: Number of Deaths from Cocaine"). Many cocaine users also use alcohol,
and this combination can be particularly dangerous. The two substances react to produce
17
cocaethylene, which may potentiate the toxic effects of cocaine and alcohol on the heart. The
combination of cocaine and heroin is also very dangerous. Users combine these drugs because the
stimulating effects of cocaine are offset by the sedating effects of heroin; however, this can lead to
taking a high dose of heroin without initially realizing it. Because cocaine's effects wear off sooner, this
can lead to a heroin overdose, in which the user's respiration dangerously slows down or stops,
possibly fatally.
With regular use, tolerance may develop so that higher doses, more frequent use of cocaine, or both
,
are needed to produce the same level of pleasure and relief from withdrawal experienced initially.10 18
At the same time, users can also develop sensitization, in which less cocaine is needed to produce
7
anxiety, convulsions, or other toxic effects. Tolerance to cocaine reward and sensitization to cocaine
toxicity can increase the risk of overdose in a regular user.
Users take cocaine in binges, in which cocaine is used repeatedly and at increasingly higher doses.
This can lead to increased irritability, restlessness, panic attacks, paranoia, and even a full-blown
2
psychosis, in which the individual loses touch with reality and experiences auditory hallucinations.
With increasing doses or higher frequency of use, the risk of adverse psychological or physiological
,
effects increases.2 7 Animal research suggests that binging on cocaine during adolescence enhances
19
sensitivity to the rewarding effects of cocaine and MDMA (Ecstasy or Molly). Thus, binge use of
cocaine during adolescence may further increase vulnerability to continued use of the drug among
some people.
Page 9
Specific routes of cocaine administration can produce their own adverse effects. Regularly snorting
cocaine can lead to loss of sense of smell, nosebleeds, problems with swallowing, hoarseness, and an
15
overall irritation of the nasal septum leading to a chronically inflamed, runny nose. Smoking crack
,
23
cocaine damages the lungs and can worsen asthma. People who inject cocaine have puncture
7
marks called tracks, most commonly in their forearms, and they are at risk of contracting infectious
diseases like HIV and hepatitis C (see "Why Are Cocaine Users at Risk for Contracting HIV and
Hepatitis?"). They also may experience allergic reactions, either to the drug itself or to additives in
cocaine, which in severe cases can result in death.
Cocaine damages many other organs in the body. It reduces blood flow in the gastrointestinal tract,
7
which can lead to tears and ulcerations. Many chronic cocaine users lose their appetite and
experience significant weight loss and malnourishment. Cocaine has significant and well-recognized
, ,
toxic effects on the heart and cardiovascular system.7 16 20 Chest pain that feels like a heart attack is
,
common and sends many cocaine users to the emergency room.7 20 Cocaine use is linked with
16
increased risk of stroke, as well as inflammation of the heart muscle, deterioration of the ability of the
20
heart to contract, and aortic ruptures.
In addition to the increased risk for stroke and seizures, other neurological problems can occur with
,
long-term cocaine use.7 18 There have been reports of intracerebral hemorrhage, or bleeding within the
,
brain, and balloon-like bulges in the walls of cerebral blood vessels.7 18 Movement disorders, including
7
Parkinson’s disease, may also occur after many years of cocaine use. Generally, studies suggest that
a wide range of cognitive functions are impaired with long-term cocaine use—such as sustaining
attention, impulse inhibition, memory, making decisions involving rewards or punishments, and
14
performing motor tasks.
Former cocaine users are at high risk for relapse, even following long periods of abstinence. Research
indicates that during periods of abstinence, the memory of the cocaine experience or exposure to cues
21
associated with drug use can trigger strong cravings, which can lead to relapse.
Page 10
Drug intoxication and addiction can compromise judgment and decision-making and potentially lead to
risky sexual behavior, including trading sex for drugs, and needle sharing. This increases a cocaine
22
user’s risk for contracting infectious diseases such as HIV and hepatitis C (HCV). There are no
vaccines to prevent HIV or HCV infections.
Studies that examine patterns of HIV infection and progression have demonstrated that cocaine use
23 24
accelerates HIV infection. Research indicates that cocaine impairs immune cell function, promotes
replication of the HIV virus, and potentiates the damaging effects of HIV on different types of cells in
23
the brain and spinal cord, resulting in further damage. Studies also suggest that cocaine use
accelerates the development of NeuroAIDS, neurological conditions associated with HIV infection.
23
Symptoms of NeuroAIDS include memory loss, movement problems, and vision impairment.
Cocaine users with HIV often have advanced progression of the disease, with increased viral load and
accelerated decreases in CD4+ cell counts. Infection with HIV increases risk for co-infection with HCV,
24
a virus that affects the liver. Co-infection can lead to serious illnesses—including problems with the
immune system and neurologic conditions. Liver complications are very common, with many co-
22
infected individuals dying of chronic liver disease and cancer. Although the link between injection
drug use and HIV/HCV is well established, more studies are needed to understand the molecular
24
mechanisms underlying this increased risk of co-infection in non-injecting substance users.
The interaction of substance use, HIV, and hepatitis may accelerate disease progression. For
example, HIV speeds the course of HCV infection by accelerating the progression of hepatitis-
24
associated liver disease. Research has linked HIV/HCV co-infection with increased mortality when
24
compared to either infection alone. Substance use and co-infection likely negatively influence HIV
24
disease progression and the ability of the body to marshal an immune response.
Patients with HIV/HCV co-infection can benefit from substance abuse treatment and antiretroviral
therapies, when closely monitored.22 Antiretroviral treatment is not effective for everyone and can
have significant side effects, necessitating close medical supervision. Testing for HIV and HCV is
recommended for any individual who has ever injected drugs, since the disease is highly transmissible
via injection.
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Most women who are addicted to cocaine are of childbearing age. Estimates suggest that about 5
25
percent of pregnant women use one or more addictive substances, and there are around 750,000
26
cocaine-exposed pregnancies every year. Although women may be reluctant to report substance
use patterns because of social stigma and fear of losing custody of their children, they should be
aware that drug use while pregnant is associated with specific risks that may be reduced with
appropriate care.
Cocaine use during pregnancy is associated with maternal migraines and seizures, premature
25
membrane rupture, and separation of the placental lining from the uterus prior to delivery. Pregnancy
is accompanied by normal cardiovascular changes, and cocaine use exacerbates these—sometimes
leading to serious problems with high blood pressure (hypertensive crises), spontaneous miscarriage,
26
preterm labor, and difficult delivery. Cocaine-using pregnant women must receive appropriate
25
medical and psychological care—including addiction treatment—to reduce these risks.
Sex-specific addiction treatment and comprehensive services—including prenatal care, mental health
counseling, vocational/employment assistance, and parenting skills training—can promote drug
27
abstinence and other positive health behaviors. Motivational incentives/contingency management
(see "Behavioral Interventions") as an adjunct to other addiction treatment is a particularly promising
28
strategy to engage women in prenatal care and counseling for substance use.
It is difficult to estimate the full extent of the consequences of maternal drug use and to determine the
specific hazard of a particular drug to the unborn child. This is because multiple factors—such as the
amount and number of all drugs used, including nicotine or alcohol; extent of prenatal care; exposure
to violence in the environment; socioeconomic conditions; maternal nutrition; other health conditions;
and exposure to sexually transmitted diseases—can all interact to influence maternal and child
, ,
outcomes.26 29 30 Similarly, parenting styles, quality of care during early childhood, exposure to
,
violence, and continued parental drug use are strong environmental factors influencing outcomes.31 32
Babies born to mothers who use cocaine during pregnancy are often prematurely delivered, have low
birth weights and smaller head circumferences, and are shorter in length than babies born to mothers
, ,
who do not use cocaine.26 29 30 Dire predictions of reduced intelligence and social skills in babies born
to mothers who used crack cocaine while pregnant during the 1980s were grossly exaggerated.
However, the fact that most of these children do not show serious overt deficits should not be
Page 12
overinterpreted to indicate that there is no cause for concern.
Using sophisticated technologies, scientists are now finding that exposure to cocaine during fetal
,
development may lead to subtle, yet significant, later deficits in some children.31 32 These include
behavior problems (e.g., difficulties with self-regulation) and deficits in some aspects of cognitive
performance, information processing, and sustained attention to tasks—abilities that are important for
,
the realization of a child’s full potential.32 33 Some deficits persist into the later years, with prenatally
34
exposed adolescents showing increased risk for subtle problems with language and memory. Brain
scans in teens suggests that at-rest functioning of some brain regions—including areas involved in
35
attention, planning, and language—may differ from that of non-exposed peers. More research is
needed on the long-term effects of prenatal cocaine exposure.
Pharmacological Approaches
Presently, there are no medications approved by the U.S. Food and Drug Administration to treat
cocaine addiction, though researchers are exploring a variety of neurobiological targets. Past research
has primarily focused on dopamine, but scientists have also found that cocaine use induces changes
in the brain related to other neurotransmitters—including serotonin, gamma-aminobutyric acid (GABA),
37
norepinephrine, and glutamate. Researchers are currently testing medications that act at the
dopamine D3 receptor, a subtype of dopamine receptor that is abundant in the emotion and reward
38
centers of the brain. Other research is testing compounds (e.g., N-acetylcysteine) that restore the
balance between excitatory (glutamate) and inhibitory (GABA) neurotransmission, which is disrupted
Page 13
39
by long-term cocaine use. Research in animals is also looking at medications (e.g., lorcaserin) that
40
act at serotonin receptors.
Several medications marketed for other diseases show promise in reducing cocaine use within
controlled clinical trials. Among these, disulfiram, which is used to treat alcoholism, has shown the
most promise. Scientists do not yet know exactly how disulfiram reduces cocaine use, though its
effects may be related to its ability to inhibit an enzyme that converts dopamine to norepinephrine.
However, disulfiram does not work for everyone. Pharmacogenetic studies are revealing variants in
the gene that encodes the DBH enzyme and seems to influence disulfiram’s effectiveness in reducing
41–43
cocaine use. Knowing a patient’s DBH genotype could help predict whether disulfiram would be
41–43
an effective pharmacotherapy for cocaine dependence in that person.
Finally, researchers have developed and conducted early tests on a cocaine vaccine that could help
reduce the risk of relapse. The vaccine stimulates the immune system to create cocaine-specific
44
antibodies that bind to cocaine, preventing it from getting into the brain. In addition to showing the
vaccine’s safety, a clinical trial found that patients who attained high antibody levels significantly
45
reduced cocaine use. However, only 38 percent of the vaccinated subjects attained sufficient
45
antibody levels and for only 2 months.
Researchers are working to improve the cocaine vaccine by enhancing the strength of binding to
,
cocaine and its ability to elicit antibodies.44 46 New vaccine technologies, including gene transfer to
boost the specificity and level of antibodies produced or enhance the metabolism of cocaine, may also
47
improve the effectiveness of this treatment. A pharmacogenetics study with a small number of
patients suggests that individuals with a particular genotype respond well to the cocaine vaccine—an
48
intriguing finding that requires more research.
In addition to treatments for addiction, researchers are developing medical interventions to address
the acute emergencies that result from cocaine overdose. One approach being explored is the use of
genetically engineered human enzymes involved in the breakdown of cocaine, which would
49
counter the behavioral and toxic effects of a cocaine overdose. Currently, researchers are testing
49
and refining these enzymes in animal research, with the ultimate goal of moving to clinical trials.
Behavioral Interventions
Page 14
Many behavioral treatments for cocaine addiction have proven to be effective in both residential and
outpatient settings. Indeed, behavioral therapies are often the only available and effective treatments
for many drug problems, including stimulant addictions. However, the integration of behavioral and
50
pharmacological treatments may ultimately prove to be the most effective approach.
One form of behavioral therapy that is showing positive results in people with cocaine use disorders is
contingency management (CM), also called motivational incentives. Programs use a voucher or prize-
based system that rewards patients who abstain from cocaine and other drugs. On the basis of drug-
free urine tests, the patients earn points, or chips, which can be exchanged for items that encourage
healthy living, such as a gym membership, movie tickets, or dinner at a local restaurant. CM may be
,
particularly useful for helping patients achieve initial abstinence from cocaine and stay in treatment.39
50–52
This approach has recently been shown to be practical and effective in community treatment
51
programs.
Research indicates that CM benefits diverse populations of cocaine users. For example, studies show
that cocaine-dependent pregnant women and women with young children who participated in a CM
program as an adjunct to other substance use disorder treatment were able to stay abstinent longer
28
than those who received an equivalent amount of vouchers with no behavioral requirements.
Patients participating in CM treatment for cocaine use who also experienced psychiatric
symptoms—such as depression, emotional distress, and hostility—showed a significant reduction in
53
these problems, probably related to reductions in cocaine use.
Cognitive-behavioral therapy (CBT) is an effective approach for preventing relapse. This approach
helps patients develop critical skills that support long-term abstinence—including the ability to
recognize the situations in which they are most likely to use cocaine, avoid these situations, and cope
more effectively with a range of problems associated with drug use. This therapy can also be used in
50
conjunction with other treatments, thereby maximizing the benefits of both.
Recently, researchers developed a computerized form of CBT (CBT4CBT) that patients use in a
54–56
private room of a clinic. This interactive multimedia program closely follows the key lessons and
skill-development activities of in-person CBT in a series of modules. Movies present examples and
information that support the development of coping skills; quizzes, games, and homework
54–56
assignments reinforce the lessons and provide opportunities to practice skills. Studies have shown
Page 15
54
that adding CBT4CBT to weekly counseling boosted abstinence and increased treatment success
55
rates up to 6 months after treatment.
Regardless of the specific type of substance use disorder treatment, it is important that patients
receive services that match all of their treatment needs. For example, an unemployed patient would
benefit from vocational rehabilitation or career counseling along with addiction treatment. Patients with
marital problems may need couples counseling. Once inpatient treatment ends, ongoing support—also
called aftercare—can help people avoid relapse. Research indicates that people who are committed to
abstinence, engage in self-help behaviors, and believe that they have the ability to refrain from using
59
cocaine (self-efficacy) are more likely to abstain. Aftercare serves to reinforce these traits and
address problems that may increase vulnerability to relapse, including depression and declining self-
59
efficacy.
Scientists have found promising results from telephone-based counseling as a low-cost method to
deliver aftercare. For example, people who misused stimulants who participated in seven sessions of
telephone counseling showed decreasing drug use during the first 3 months, whereas those who did
60
not receive calls increased their use. Voucher incentives can boost patients' willingness to participate
61
in telephone aftercare, doubling the number of sessions received according to one study.
Page 16
Two cutting-edge areas of science, genetics and brain imaging, are significantly advancing our
understanding of cocaine addiction.
Researchers estimate that genetics contributes 42 to 79 percent of the risk for cocaine use and
63
dependence. Of course, with a complex disease such as addiction, many different genes are
involved, and their expression can be influenced by the environment. There appears to be significant
overlap in the genes that put people at risk for all addictive substances, perhaps indicating a common
63
biological pathway for addiction regardless of the drug.
In genome-wide association studies (GWAS), researchers examine whether certain gene variants are
more frequently found in people with a substance use disorder, which eventually might help identify
,
those at increased risk for drug addiction.64 65 Identifying genes linked to addiction is only the first step.
Candidate-gene research examines the links between substance use and specific genes that encode
proteins that appear to be related to addiction. For example, researchers have found connections
between various aspects of cocaine addiction and the genes that encode for particular dopamine
63
receptors and the enzymes that break down this neurotransmitter.
Because environmental factors typically shape the impact of genes on disease risk, researchers must
63
also identify how particular gene-by-environment interactions influence the course of addiction.
Research in the field of epigenetics is uncovering how the environment induces long-term changes in
66
gene expression—influencing the pattern of gene expression—without altering the DNA sequence.
In animal research, scientists are determining how long-term cocaine exposure changes gene
expression in the brain, particularly in the reward pathway. Studies have linked specific cocaine-
67
induced epigenetic changes to neuroadaptations and behavioral hallmarks of addiction, such as
,
66 67
sensitivity to cocaine’s rewarding effects. The epigenetic changes induced by cocaine can be
68
passed to the next generation, even if the drug exposure does not occur prenatally. Although much
more genetic and epigenetic research is needed, understanding addiction at the molecular level offers
great promise for improving diagnosis, for example by discovering biomarkers for disease severity or
66
treatment response.
Although more research is needed, brain-imaging might be used to detect biomarkers for drug
addiction vulnerability, as these technologies have yielded insights into the processes underlying
Page 17
69
craving and how medications may quell the brain’s response to cocaine cues. A relatively new
neuroimaging technology called default-mode or resting-state functional magnetic resonance imaging
(rs-fMRI) reveals brain activity when people are alert but not performing a particular task; researchers
use this technique to compare functional brain networks of people who have used cocaine for a long
time and those who have not. These studies suggest that there is reduced connectivity between
70–72 73
various brain circuits and between the two hemispheres among people with cocaine
dependence. Researchers have also correlated reduced connectivity between particular brain circuits
71 72
with important addiction-related behaviors, including risk for relapse and impulsivity.
Neuroimaging technologies are also documenting how the brains of cocaine users may recover after
periods of abstinence. For example, these techniques indicate that years of cocaine use are
associated with reduced grey matter in particular brain regions. However, people who maintained
cocaine abstinence for approximately 9 months showed grey matter levels similar to or greater than
74
those of people who had never used the drug. Further analysis indicated that the increased grey
matter occurred in regions other than the ones altered by cocaine use, suggesting that the
neurobiological changes involved in recovery are more complex than simply reversing the changes
74
related to addiction. The researchers also found that increased grey matter volume in brain regions
74
involved with behavioral control were associated with longer duration of abstinence.
fMRI technologies have also revealed that abstinence from cocaine has important, restorative effects
on the brain. Although current cocaine users demonstrated reduced brain activity in a brain circuit that
mediates response inhibition during a motor control task, individuals who had attained abstinence for
an average of 8 months showed similar patterns of activation and levels of performance to those who
75
had never used the drug. The results suggest that abstinence helps restore the functioning of this
brain circuit.
Researchers are engaged in several large-scale, collaborative projects to map the human
connectome, which is the brain’s network of interconnected circuits. For example, the National
Institutes of Health supports the Human Connectome Project to generate maps of the developing,
adult, and aging brain. By having a map of the typical brain, scientists will further understand how
neural functioning differs in behavioral disorders—knowledge that will drive improved diagnostics and
treatments.
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Glossary
Addiction: A chronic, relapsing disease characterized by compulsive drug seeking and use and by
long-lasting changes in the brain.
Anesthetic: An agent that causes insensitivity to pain and is used for surgeries and other medical
procedures.
Coca: The plant, Erythroxylon, from which cocaine is derived. Also refers to the leaves of this plant.
Dopamine: A brain chemical, classified as a neurotransmitter, found in regions of the brain that
regulate movement, emotion, motivation, and pleasure.
Freebase: A solid, water-insoluble, and smokable form of cocaine that is produced when its
hydrochloride salt form is processed with ammonia or sodium bicarbonate and water, then heated to
remove the hydrochloride. (Also, see "crack.")
Frontal cortex: The front part of the brain involved with reasoning, planning, problem-solving, and
other higher cognitive functions.
Gamma-aminobutyric acid (GABA): The main inhibitory neurotransmitter in the central nervous
system. GABA provides the needed counterbalance to the actions of other systems, particularly the
excitatory neurotransmitter glutamate.
Glutamate: An excitatory neurotransmitter found throughout the brain, that influences the reward
system and is involved in learning and memory among other functions.
Hydrochloride salt: A powdered, water-soluble form of cocaine that can be injected or snorted.
Page 19
Nucleus accumbens: A brain region involved in motivation and reward. Nearly all drugs of abuse
directly or indirectly increase dopamine in the nucleus accumbens, contributing to their addictive
properties.
Rush: A surge of pleasure (euphoria) that rapidly follows administration of some drugs.
Stimulant: A class of drugs that enhances the activity of monamines (such as dopamine) in the brain,
increasing arousal, heart rate, blood pressure, and respiration, and decreasing appetite; includes
some medications used to treat attention-deficit hyperactivity disorder (e.g., methylphenidate and
amphetamines), as well as cocaine and methamphetamine.
Tolerance: A condition in which higher doses of a drug are required to produce the same effect
achieved during initial use.
Page 20
NIDA websites and webpages
www.nida.nih.gov/drugs-abuse/cocaine
www.researchstudies.drugabuse.gov
www.irp.drugabuse.gov
Other websites
Information about marijuana is also available through the following websites:
This publication is available for your use and may be reproduced in its entirety without permission from NIDA.
Citation of the source is appreciated, using the following language: Source: National Institute on Drug Abuse;
National Institutes of Health; U.S. Department of Health and Human Services.
References
1. Calatayud J, González A. History of the development and evolution of local anesthesia since the
coca leaf. Anesthesiology. 2003;98(6):1503-1508.
2. Goldstein RA, DesLauriers C, Burda AM. Cocaine: history, social implications, and toxicity–a
review. Dis–Mon DM. 2009;55(1):6-38. doi:10.1016/j.disamonth.2008.10.002.
3. Drent M, Wijnen P, Bast A. Interstitial lung damage due to cocaine abuse: pathogenesis,
pharmacogenomics and therapy. Curr Med Chem. 2012;19(33):5607-5611.
Page 21
4. Center for Behavioral Health Statistics and Quality (CBHSQ). Behavioral Health Trends in the
United States: Results from the 2014 National Survey on Drug Use and Health. Rockville, MD:
Substance Abuse and Mental Health Services Administration; 2015. HHS Publication No. SMA 15-
4927, NSDUH Series H-50.
5. Johnston L, O’Malley P, Miech R, Bachman J, Schulenberg J. Monitoring the Future National
Survey Results on Drug Use: 1975-2015: Overview: Key Findings on Adolescent Drug Use. Ann
Arbor, MI: Institute for Social Research, The University of Michigan; 2015.
6. Center for Behavioral Health Statistics and Quality (CBHSQ). Drug Abuse Warning Network: 2011:
Selected Tables of National Estimates of Drug-Related Emergency Department Visits. Rockville,
MD: Substance Abuse and Mental Health Services Administration; 2013.
7. Riezzo I, Fiore C, De Carlo D, et al. Side effects of cocaine abuse: multiorgan toxicity and
pathological consequences. Curr Med Chem. 2012;19(33):5624-5646.
8. Baik J-H. Dopamine signaling in reward-related behaviors. Front Neural Circuits. 2013;7.
doi:10.3389/fncir.2013.00152.
9. Schmidt HD, Pierce RC. Cocaine-induced neuroadaptations in glutamate transmission: potential
therapeutic targets for craving and addiction. Ann N Y Acad Sci. 2010;1187:35-75.
doi:10.1111/j.1749-6632.2009.05144.x.
10. Wolf ME. The Bermuda Triangle of cocaine-induced neuroadaptations. Trends Neurosci.
2010;33(9):391-398. doi:10.1016/j.tins.2010.06.003.
11. Mantsch JR, Vranjkovic O, Twining RC, Gasser PJ, McReynolds JR, Blacktop JM. Neurobiological
mechanisms that contribute to stress-related cocaine use. Neuropharmacology. 2014;76, Part
B:383-394. doi:10.1016/j.neuropharm.2013.07.021.
12. Lucantonio F, Stalnaker TA, Shaham Y, Niv Y, Schoenbaum G. The impact of orbitofrontal
dysfunction on cocaine addiction. Nat Neurosci. 2012;15(3):358-366. doi:10.1038/nn.3014.
13. Lucantonio F, Takahashi YK, Hoffman AF, et al. Orbitofrontal activation restores insight lost after
cocaine use. Nat Neurosci. 2014;17(8):1092-1099. doi:10.1038/nn.3763.
14. Spronk DB, van Wel JHP, Ramaekers JG, Verkes RJ. Characterizing the cognitive effects of
cocaine: a comprehensive review. Neurosci Biobehav Rev. 2013;37(8):1838-1859.
doi:10.1016/j.neubiorev.2013.07.003.
15. Advokat C, Comaty J, Julien R. Julien’s Primer of Drug Action. 13th ed. New York, NY: Worth
Publishers; 2014.
Page 22
16. Fonseca AC, Ferro JM. Drug abuse and stroke. Curr Neurol Neurosci Rep. 2013;13(2):325.
doi:10.1007/s11910-012-0325-0.
17. Pennings EJM, Leccese AP, Wolff FA de. Effects of concurrent use of alcohol and cocaine. Addict
Abingdon Engl. 2002;97(7):773-783.
18. Büttner A. Neuropathological alterations in cocaine abuse. Curr Med Chem. 2012;19(33):5597-
5600.
19. Mateos-García A, Roger-Sánchez C, Rodriguez-Arias M, et al. Higher sensitivity to the conditioned
rewarding effects of cocaine and MDMA in High-Novelty-Seekers mice exposed to a cocaine binge
during adolescence. Psychopharmacology (Berl). 2015;232(1):101-113. doi:10.1007/s00213-014-
3642-y.
20. Maraj S, Figueredo VM, Lynn Morris D. Cocaine and the heart. Clin Cardiol. 2010;33(5):264-269.
doi:10.1002/clc.20746.
21. Sinha R. The clinical neurobiology of drug craving. Curr Opin Neurobiol. 2013;23(4):649-654.
doi:10.1016/j.conb.2013.05.001.
22. Khalsa JH, Elkashef A. Interventions for HIV and hepatitis C virus infections in recreational drug
users. Clin Infect Dis. 2010;50(11):1505-1511. doi:10.1086/652447.
23. Buch S, Yao H, Guo M, et al. Cocaine and HIV-1 interplay in CNS: cellular and molecular
mechanisms. Curr HIV Res. 2012;10(5):425-428.
24. Parikh N, Nonnemacher MR, Pirrone V, Block T, Mehta A, Wigdahl B. Substance abuse, HIV-1 and
hepatitis. Curr HIV Res. 2012;10(7):557-571.
25. Wendell AD. Overview and epidemiology of substance abuse in pregnancy. Clin Obstet Gynecol.
2013;56(1):91-96. doi:10.1097/GRF.0b013e31827feeb9.
26. Cain MA, Bornick P, Whiteman V. The maternal, fetal, and neonatal effects of cocaine exposure in
pregnancy. Clin Obstet Gynecol. 2013;56(1):124-132. doi:10.1097/GRF.0b013e31827ae167.
27. Hull L, May J, Farrell-Moore D, Svikis DS. Treatment of cocaine abuse during pregnancy:
translating research to clinical practice. Curr Psychiatry Rep. 2010;12(5):454-461.
doi:10.1007/s11920-010-0138-2.
28. Schottenfeld RS, Moore B, Pantalon MV. Contingency management with community reinforcement
approach or twelve-step facilitation drug counseling for cocaine dependent pregnant women or
women with young children. Drug Alcohol Depend. 2011;118(1):48-55.
doi:10.1016/j.drugalcdep.2011.02.019.
Page 23
29. Behnke M, Smith VC, Abuse C on S, Newborn C on FA. Prenatal substance abuse: short- and
long-term effects on the exposed fetus. Pediatrics. 2013;131(3):e1009-e1024.
doi:10.1542/peds.2012-3931.
30. Gouin K, Murphy K, Shah PS, Knowledge Synthesis group on Determinants of Low Birth Weight
and Preterm Births. Effects of cocaine use during pregnancy on low birthweight and preterm birth:
systematic review and metaanalyses. Am J Obstet Gynecol. 2011;204(4):340.e1-e12.
doi:10.1016/j.ajog.2010.11.013.
31. Lambert BL, Bauer CR. Developmental and behavioral consequences of prenatal cocaine
exposure: a review. J Perinatol Off J Calif Perinat Assoc. 2012;32(11):819-828.
doi:10.1038/jp.2012.90.
32. Lester BM, Lagasse LL. Children of addicted women. J Addict Dis. 2010;29(2):259-276.
doi:10.1080/10550881003684921.
33. Ackerman JP, Riggins T, Black MM. A review of the effects of prenatal cocaine exposure among
school-aged children. Pediatrics. 2010;125(3):554-565. doi:10.1542/peds.2009-0637.
34. Buckingham-Howes S, Berger SS, Scaletti LA, Black MM. Systematic review of prenatal cocaine
exposure and adolescent development. Pediatrics. 2013;131(6):e1917-e1936.
doi:10.1542/peds.2012-0945.
35. Li K, Zhu D, Guo L, et al. Connectomics signatures of prenatal cocaine exposure affected
adolescent brains. Hum Brain Mapp. 2013;34(10):2494-2510. doi:10.1002/hbm.22082.
36. Center for Behavioral Health Statistics and Quality (CBHSQ). Treatment Episode Data Set (TEDS):
2003-2013. National Admissions to Substance Abuse Treatment Services. Rockville, MD:
Substance Abuse and Mental Health Services Administration; 2015. BHSIS Series S-75, HHS
Publication No. (SMA) 15-4934.
37. Shorter D, Domingo CB, Kosten TR. Emerging drugs for the treatment of cocaine use disorder: a
review of neurobiological targets and pharmacotherapy. Expert Opin Emerg Drugs. 2015;20(1):15-
29. doi:10.1517/14728214.2015.985203.
38. Karila L, Reynaud M, Aubin H-J, et al. Pharmacological treatments for cocaine dependence: is
there something new? Curr Pharm Des. 2011;17(14):1359-1368.
39. Kampman KM. What’s new in the treatment of cocaine addiction? Curr Psychiatry Rep.
2010;12(5):441-447. doi:10.1007/s11920-010-0143-5.
40. Harvey-Lewis C, Li Z, Higgins GA, Fletcher PJ. The 5-HT2C receptor agonist lorcaserin reduces
cocaine self-administration, reinstatement of cocaine-seeking and cocaine induced locomotor
Page 24
activity. Neuropharmacology. 2016;101:237-245. doi:10.1016/j.neuropharm.2015.09.028.
41. Shorter D, Nielsen DA, Huang W, Harding MJ, Hamon SC, Kosten TR. Pharmacogenetic
randomized trial for cocaine abuse: disulfiram and ?1A-adrenoceptor gene variation. Eur
Neuropsychopharmacol J Eur Coll Neuropsychopharmacol. 2013;23(11):1401-1407.
doi:10.1016/j.euroneuro.2013.05.014.
42. Spellicy CJ, Kosten TR, Hamon SC, Harding MJ, Nielsen DA. ANKK1 and DRD2
pharmacogenetics of disulfiram treatment for cocaine abuse. Pharmacogenet Genomics.
2013;23(7):333-340. doi:10.1097/FPC.0b013e328361c39d.
43. Kosten TR, Wu G, Huang W, et al. Pharmacogenetic randomized trial for cocaine abuse: disulfiram
and dopamine ?-hydroxylase. Biol Psychiatry. 2013;73(3):219-224.
doi:10.1016/j.biopsych.2012.07.011.
44. Kosten TR, Domingo CB. Can you vaccinate against substance abuse? Expert Opin Biol Ther.
2013;13(8):1093-1097. doi:10.1517/14712598.2013.791278.
45. Martell BA, Orson FM, Poling J, et al. Cocaine vaccine for the treatment of cocaine dependence in
methadone-maintained patients: a randomized, double-blind, placebo-controlled efficacy trial. Arch
Gen Psychiatry. 2009;66(10):1116-1123. doi:10.1001/archgenpsychiatry.2009.128.
46. Cai X, Tsuchikama K, Janda KD. Modulating cocaine vaccine potency through hapten fluorination.
J Am Chem Soc. 2013;135(8):2971-2974. doi:10.1021/ja400356g.
47. Brimijoin S, Shen X, Orson F, Kosten T. Prospects, promise and problems on the road to effective
vaccines and related therapies for substance abuse. Expert Rev Vaccines. 2013;12(3):323-332.
doi:10.1586/erv.13.1.
48. Nielsen DA, Hamon SC, Kosten TR. The ?-opioid receptor gene as a predictor of response in a
cocaine vaccine clinical trial. Psychiatr Genet. 2013;23(6):225-232.
doi:10.1097/YPG.0000000000000008.
49. Schindler CW, Goldberg SR. Accelerating cocaine metabolism as an approach to the treatment of
cocaine abuse and toxicity. Future Med Chem. 2012;4(2):163-175. doi:10.4155/fmc.11.181.
50. Penberthy JK, Ait-Daoud N, Vaughan M, Fanning T. Review of treatment for cocaine dependence.
Curr Drug Abuse Rev. 2010;3(1):49-62.
51. Petry NM, Barry D, Alessi SM, Rounsaville BJ, Carroll KM. A randomized trial adapting contingency
management targets based on initial abstinence status of cocaine-dependent patients. J Consult
Clin Psychol. 2012;80(2):276-285. doi:10.1037/a0026883.
Page 25
52. Schierenberg A, van Amsterdam J, van den Brink W, Goudriaan AE. Efficacy of contingency
management for cocaine dependence treatment: a review of the evidence. Curr Drug Abuse Rev.
2012;5(4):320-331.
53. Petry NM, Alessi SM, Rash CJ. Contingency management treatments decrease psychiatric
symptoms. J Consult Clin Psychol. 2013;81(5):926-931. doi:10.1037/a0032499.
54. Carroll KM, Ball SA, Martino S, et al. Computer-assisted delivery of cognitive-behavioral therapy for
addiction: a randomized trial of CBT4CBT. Am J Psychiatry. 2008;165(7):881-888.
doi:10.1176/appi.ajp.2008.07111835.
55. Carroll KM, Ball SA, Martino S, Nich C, Babuscio TA, Rounsaville BJ. Enduring effects of a
computer-assisted training program for cognitive behavioral therapy: a 6-month follow-up of
CBT4CBT. Drug Alcohol Depend. 2009;100(1-2):178-181. doi:10.1016/j.drugalcdep.2008.09.015.
56. Carroll KM, Kiluk BD, Nich C, et al. Computer-assisted delivery of cognitive-behavioral therapy:
efficacy and durability of CBT4CBT among cocaine-dependent individuals maintained on
methadone. Am J Psychiatry. 2014;171(4):436-444. doi:10.1176/appi.ajp.2013.13070987.
57. Vanderplasschen W, Colpaert K, Autrique M, et al. Therapeutic communities for addictions: a
review of their effectiveness from a recovery-oriented perspective. Sci World J. 2013;2013,
2013:e427817. doi:10.1155/2013/427817.
58. Leon GD. Is the therapeutic community an evidence based treatment? What the evidence says.
Ther Communities Int Jdournal Ther Support Organ. 2010;31(2):104-128.
59. McKay JR, Van Horn D, Rennert L, Drapkin M, Ivey M, Koppenhaver J. Factors in sustained
recovery from cocaine dependence. J Subst Abuse Treat. 2013;45(2):163-172.
doi:10.1016/j.jsat.2013.02.007.
60. Farabee D, Cousins SJ, Brecht M-L, et al. A comparison of four telephone-based counseling styles
for recovering stimulant users. Psychol Addict Behav. 2013;27(1):223-229. doi:10.1037/a0029572.
61. Van Horn DHA, Drapkin M, Ivey M, et al. Voucher incentives increase treatment participation in
telephone-based continuing care for cocaine dependence. Drug Alcohol Depend. 2011;114(2-
3):225-228. doi:10.1016/j.drugalcdep.2010.09.007.
62. Donovan DM, Daley DC, Brigham GS, et al. Stimulant abuser groups to engage in 12-step: a
multisite trial in the National Institute on Drug Abuse Clinical Trials Network. J Subst Abuse Treat.
2013;44(1):103-114. doi:10.1016/j.jsat.2012.04.004.
63. Agrawal A, Verweij KJH, Gillespie NA, et al. The genetics of addiction-a translational perspective.
Transl Psychiatry. 2012;2:e140. doi:10.1038/tp.2012.54.
Page 26
64. Drgon T, Zhang P-W, Johnson C, et al. Genome wide association for addiction: replicated results
and comparisons of two analytic approaches. PloS One. 2010;5(1):e8832.
doi:10.1371/journal.pone.0008832.
65. Kreek MJ, Levran O, Reed B, Schlussman SD, Zhou Y, Butelman ER. Opiate addiction and
cocaine addiction: underlying molecular neurobiology and genetics. J Clin Invest.
2012;122(10):3387-3393. doi:10.1172/JCI60390.
66. Nestler EJ. Epigenetic mechanisms of drug addiction. Neuropharmacology. 2014;76 Pt B:259-268.
doi:10.1016/j.neuropharm.2013.04.004.
67. Schmidt HD, McGinty JF, West AE, Sadri-Vakili G. Epigenetics and psychostimulant addiction.
Cold Spring Harb Perspect Med. 2013;3(3):a012047. doi:10.1101/cshperspect.a012047.
68. Vassoler FM, Sadri-Vakili G. Mechanisms of transgenerational inheritance of addictive-like
behaviors. Neuroscience. 2014;264:198-206. doi:10.1016/j.neuroscience.2013.07.064.
69. Young KA, Franklin TR, Roberts DCS, et al. Nipping cue reactivity in the bud: baclofen prevents
limbic activation elicited by subliminal drug cues. J Neurosci Off J Soc Neurosci. 2014;34(14):5038-
5043. doi:10.1523/JNEUROSCI.4977-13.2014.
70. Gu H, Salmeron BJ, Ross TJ, et al. Mesocorticolimbic circuits are impaired in chronic cocaine
users as demonstrated by resting-state functional connectivity. NeuroImage. 2010;53(2):593-601.
doi:10.1016/j.neuroimage.2010.06.066.
71. McHugh MJ, Demers CH, Salmeron BJ, Devous MD, Stein EA, Adinoff B. Cortico-amygdala
coupling as a marker of early relapse risk in cocaine-addicted individuals. Front Psychiatry.
2014;5:16. doi:10.3389/fpsyt.2014.00016.
72. Wisner KM, Patzelt EH, Lim KO, MacDonald AW. An intrinsic connectivity network approach to
insula-derived dysfunctions among cocaine users. Am J Drug Alcohol Abuse. 2013;39(6):403-413.
doi:10.3109/00952990.2013.848211.
73. Kelly C, Zuo X-N, Gotimer K, et al. Reduced interhemispheric resting state functional connectivity in
cocaine addiction. Biol Psychiatry. 2011;69(7):684-692. doi:10.1016/j.biopsych.2010.11.022.
74. Connolly CG, Bell RP, Foxe JJ, Garavan H. Dissociated grey matter changes with prolonged
addiction and extended abstinence in cocaine users. PLoS ONE. 2013;8(3):e59645.
doi:10.1371/journal.pone.0059645.
75. Bell RP, Foxe JJ, Ross LA, Garavan H. Intact inhibitory control processes in abstinent drug
abusers (I): a functional neuroimaging study in former cocaine addicts. Neuropharmacology.
2014;82:143-150. doi:10.1016/j.neuropharm.2013.02.018.
Page 27