HOME MEDICATIONS PROGRAM SUPPLEMENTS ABOUT US CONTACT
Already in Klonopin Clonazepam Withdrawal click
here
If you
want to taper off the Klonopin and you are not sure where to start, you can
click here and read the bestselling book, How to Get Off Psychoactive Drugs
Safely or send Jim Harper an email at
Jim@theroadback.org and he will guide you through the process of Klonopin
withdrawal.
Klonopin withdrawal step by step procedure. Klonopin withdrawal. Withdrawal from
Klonopin no longer needs to be grueling and suffering from the Klonopin
withdrawal side effects can be a thing of the past. You are now on The Road Back
web site, we are a non-profit, located in the United States, offer assistance
for free and most importantly we show you what you can do right now for Klonopin
withdrawal without the need to purchase a book.
Klonopin Withdrawal - Anxiety? Insomnia?
Of
course you do.You likely would prefer to cut to the chase and find out what you
can do to get relief quickly.
Neuro
Day is formulated for the daytime anxiety and most other daytime side effects.
Neuro
Night for sleep and body aches.
JNK
Formula helps bring a gene back to balance the Klonopin has altered.
Go to
the manufacturers web site -
Click here
and purchase JNK Formula, Neuro Day and Neuro Night as a package.
The
web site you are on now, The Road Back, offers information on how to get off
Klonopin and reduce Klonopin withdrawal side effects. Many of you taking
Klonopin were prescribed Klonopin for anxiety, general anxiety disorder, panic
attacks, and possibly for other reasons.
The
Road Back is a member of California Association of Alcoholism & Drug Abuse
Counselors (CAADAC). Since 1999, The Road Back has helped thousands of people
off Klonopin and has helped as many people that wanted to stay on Klonopin but
reduce the side effects of taking this medication. The Road Back is the largest
outpatient drug withdrawal program in the world. We are based in the United
States.
Spend
a minute or two and read an e-mail we received November 10, 2014.
“Jim,
here is my testimonial. Feel free to use however you wish. God bless you!
WARNING: KLONIPIN IS A VERY ADDICTIVE AND DANGEROUS DRUG SIDE EFFECTS can be
serious and harmful to overall health. WITHDRAWAL from this drug is dangerous
and might very well kill you.
This
is what any physician should be required to advise patients upon prescribing
Klonopin. I began my journey to Hell a little over 6 years ago while going
through a nasty divorce. I was experiencing major anxiety, panic attacks, and
insomnia. These symptoms did improve. However, over the years I developed
hypertension and steadily gained weight which I had never had a problem with. I
began taking Lisinopril for the hypertension.
I made
the decision to go off of the Klonopin after seeing my gynecologist and
discussing these issues with her. She said that she felt the K was the culprit.
I asked how to taper, she told me to talk to my family doctor who prescribed it
to me. I was not told of the horrible withdrawal so I didn't think it would be a
big deal. I began tapering....and did a complete taper within a month. I had
been taking 1 mg 3X daily for 6+ years.
At
first, I did not attribute my symptoms to the withdrawal. It was subtle at
first, smells and the taste of food was very strange. Hands and feet numb and
tingling. Unable to carry a train of thought and to complete a task. I googled
withdrawal from Klonopin. I was shocked at what I read. I prayed that I would
not experience any of it.....and really did not think this would happen to "me".
Little did I know that I had just begun my descent into Hell.
I do
not feel that I can adequately convey the nightmare. You just about have to go
through it to know what it is like. There are exceptions, as Jim is proof of. I
thank God for his dedication to overcoming addiction and The Road Back. I will
get into this a little later.
Here
is a list of what I experienced, not in order and not to the degree of each
symptom, there is really no way to do so: major anxiety and panic attacks,
insomnia, hot/cold spells, severe sweating, no appetite, sensitivity to noise/
light/ movement, pain in extremities, blurred vision, ringing in ears, fullness
in head, vertigo, high bp even on lisinopril, increased heart rate, confusion,
disorientation, de-realization, depersonalization, detachment. I was completely
unable to function.
About
two weeks into this horror, my daughter visited and started researching online.
She found The Road Back program. But when you are living a minute-to-minute
nightmare it is a very long time. And I was not certain it would even work. I
was at the end of my rope. I had not slept in 4 consecutive days and nights. My
heart rate was 130+ constantly. I felt like I was going to die. My husband
thought that since I had read about these withdrawal symptoms that somehow, I
should miraculously be "alright", bc it was "normal" and I would eventually be
okay. He told me to "get a grip". I began to cry, uncontrollably. And
scream...it seemed as though it was not even coming from me. I did not even feel
human, I felt like an alien. I could not take anymore.
My
husband drove me to the ER. I was terrified that I would be committed to the
psyche ward. I feared that the doctor would not understand (who could???)!
Thankfully I was wrong. After I had somehow been talking for quite some time, he
finally looked me in the eye. I did not think I had gotten through to him. He
disclosed that his son had been addicted to K and was hospitalized for seizures.
I was relieved and terrified at the same time. He reassured me that I was most
likely past the seizure stage. He said that kicking the K would be the hardest
thing I have ever done in my life but that it would be so worth it. He did ask
me if I wanted to go back on the K, that the majority of ppl could not make it
through withdrawal and went back on the drug. I will admit that I had thought
about it......I somehow found the courage to say NO. He was concerned about my
bp which was 157/124 P132 upon entering hospital. But he did not want to address
it just yet as he felt it was a result of withdrawal. He prescribed a 20 day of
Lunesta for sleep. I actually slept for the first time in days. Thank God for
this doctor.
I
thought that maybe since I had gotten some sleep that my symptoms would improve.
I was wrong. I thought about the supplements and began an agonizing wait. I
would sit outside and wait for the delivery, afraid that I would miss it. I was
a bit skeptical as I had the misconception that anything that wasn't prescribed
by a doctor was worthless. But yet I was desperate, and this man Jim Harper
really seemed to know his stuff. I finally received my supplements and had to
restrain myself to only take the recommended amount.
I had
corresponded with Jim/The Road Back on occasion. This was my lifeline. He
suggested keeping a journal to monitor my reactions and I did. I am very
thankful for this as now that I am better it is a little difficult for me to
remember how debilitated I really was.
After
only a few days I increased to 2 capsules 3X daily. On about day five, I began
to catch glimpses of "Jill".
Very
brief but still........it was a start. I also began taking the JNK capsules
daily, as well as Omega 3, vitamin E and biotin. It was a slow and steady
progression at first, but praise God I am happy to report that I am feeling
human again. I have control again! I know without a doubt that these supplements
work! It seems like years ago that I first contacted Jim. Hard to believe it has
only been about three months. Most with this degree of withdrawal report at
least a year. I do not think I could have endured that. Occasionally I have a
bad day, and I found that even 1 glass of wine would set me back. I avoid all
alcohol. My bp and heart rate have returned to normal! I no longer take Lunesta
and I am able to sleep. I am enjoying the things that brought me joy years ago.
I am discovering new and exciting things about myself.
I want
to encourage anyone going through withdrawal of Klonopin or other Benzo drugs to
give The Road Back a try. The information and support is FREE. The supplements
saved my life. I read some reviews about the supplements being expensive.
Hello???????? I would have paid anything to be better, even rehab. The ER doctor
told me that his son had been to rehab several times to no avail. I cannot
confirm or deny rehab treatment as I have not had it. But I can tell you that
the supplements are a mere fraction of the cost of rehab. I will continue with
the supplements until I feel that I am completely well.
I hope
that my experience will help others that find themselves in this hellish
nightmare. I could never thank Jim Harper enough. God bless him and The Road
Back program.”
Jill
A/North Carolina
If you
are already reducing Klonopin we know you are looking for relief from the
Klonopin withdrawal side effects and you want relief fast. If you have already
stopped Klonopin, the need of assistance is no different and relief needs to
come quickly for you. You are not alone with these feelings and Klonopin
withdrawal symptoms.
You
can click The Program located on the top navigation line and read all chapters
of How to Get Off Psychoactive Drugs Safely for free.
Clonazepam Brand name (Klonopin and Clonazepam
Klonopin
Withdrawal
Klonopin
Withdrawal
Klonopin
Withdrawal
Klonopin
Withdrawal
Pharmacology
Clonazepam's pharmacological profile is similar to other anxiolytic/sedative
benzodiazepines. Its basic anticonvulsive properties are also similar to those
of other diazepines. Clonazepam is capable of suppressing the spike and wave
discharge in absence seizures (petit mal) and decreasing the frequency,
amplitude, duration and spread of discharge in minor motor seizures.
Clonazepam is well absorbed orally with maximum blood concentrations occurring
in 1 to 2 hours. Clonazepam is metabolized by the liver to inactive metabolites,
which are excreted mainly in the urine. Less than 0.5% of a dose is excreted in
the urine unchanged and from 9 to 27% of a dose may be excreted in the feces.
The half-life of the parent compound varies from approximately 18 to 50 hours.
Indications
Alone
or as an adjunct in the management of myoclonic and akinetic seizures and petit
mal variant (Lennox-Gastaut syndrome). May also be of some value in patients
with absence spells (petit mal) who have failed to respond to succinimides.
Up to
nearly 33% of the patients in some studies have shown a loss of anticonvulsant
activity, often within the first 3 months of clonazepam administration. In some
cases, dosage adjustment may re-establish efficacy.
Contraindications
Significant liver disease, narrow angle glaucoma, sensitivity to
benzodiazepines.
Warnings
Pregnancy:
Recent
reports indicate an association between the use of anticonvulsant drugs and an
elevated incidence of birth defects in children born to epileptic women taking
such medication during pregnancy. The incidence of congenital malformations in
the general population is regarded to be approximately 2%; in children of
treated epileptic women this incidence may be increased 2 to 3 fold. The
increase is largely due to specific defects, e.g., congenital malformations of
the heart, and cleft lip and/or palate.
Nevertheless, the great majority of mothers receiving anticonvulsant medications
deliver normal infants.
Data
are more extensive with respect to phenytoin and phenobarbital, but these drugs
are also the most commonly prescribed anticonvulsants. Some reports indicate a
possible similar association with the use of other anticonvulsants, including
trimethadione and paramethadione. However, the possibility also exists that
other factors, e.g., genetic predisposition or the epileptic condition itself
may contribute to or may be mainly responsible for the higher incidence of birth
defects.
Anticonvulsants should not be discontinued in patients in whom the drug is
administered to prevent major seizures, because of the strong possibility of
precipitating status epilepticus with attendant hypoxia and risk to both the
mother and the unborn child. With regard to drugs given for minor seizures, the
risk of discontinuing medication prior to or during pregnancy should be weighed
against the risk of congenital defects in the particular case and with the
particular family history.
Epileptic women of childbearing age should be encouraged to seek professional
counsel and should report the onset of pregnancy promptly to their physician.
Where the necessity for continued use of antiepileptic medication is in doubt,
appropriate consultation might be indicated.
In a
reproductive study in rabbits, clonazepam administration was associated with an
increased incidence of cleft palate and other anomalies at 2 dose
concentrations. Accordingly, clonazepam should be used in women of childbearing
potential only when the expected benefits to the patient warrant the possible
risk to a fetus.
Lactation:
Mothers receiving clonazepam should not breast feed their infants.
Children: Because of the possibility that adverse effects on childhood physical
or mental development could become apparent only after years, a risk-benefit
consideration of the long-term use of clonazepam is important in pediatric
patients.
Precautions
Although simultaneous administration of several anticonvulsants may be
considered with clonazepam, such combined therapy may result in an increase of
central depressant adverse effects. In addition, the dosage of each drug may be
required to be adjusted to obtain the optimum effect.
Abrupt
withdrawal of clonazepam particularly in those patients on long-term, high dose
therapy, may precipitate status epilepticus. Therefore, as with any other
anticonvulsants, gradual withdrawal is essential when discontinuing clonazepam.
While clonazepam is being gradually withdrawn, the simultaneous substitution of
incremental doses of another anticonvulsant may be indicated.
A
paradoxical increase in seizure activity or the appearance of new seizure types
has occurred in a very few patients during clonazepam treatment. When used in
patients in whom several different types of seizures coexist, clonazepam may
increase the incidence or precipitate the onset of generalized tonic-clonic
seizures (grand mal). These phenomena may require the addition of appropriate
anticonvulsants or an increase in their dosages. The concomitant use of valproic
acid and clonazepam may produce absence status.
Occupational Hazards:
Caution patients receiving clonazepam against engaging in hazardous occupations
requiring complete mental alertness, such as operating machinery or driving a
motor vehicle.They also should be warned against the concomitant use of alcohol
and other CNS depressant drugs.
The
CNS depressant action of benzodiazepines may be potentiated by other drugs such
as alcohol, narcotics, barbiturates, nonbarbiturate hypnotics, anxiolytics,
phenothiazines, thioxanthene and butyrophenone antipsychotic agents, MAO
inhibitors and tricyclic antidepressants.
Benzodiazepines have produced habituation, dependence and withdrawal symptoms
similar to those noted with barbiturates and alcohol. Therefore, patients who
may be prone to increasing the dose of drugs on their own initiative should be
under careful monitoring when receiving clonazepam.
Periodic liver function tests and blood counts are recommended during long-term
clonazepam therapy.
Clonazepam and its metabolites are excreted by the kidneys; to avoid excessive
accumulation, exercise caution in administering the drug to patients with
impaired renal function.
Hypersecretion in the upper respiratory passages has at times been a troublesome
adverse reaction during clonazepam therapy, especially in small mentally
retarded children who ordinarily have difficulty handling secretions. Treatment
with clonazepam should be instituted with caution in patients with chronic
respiratory diseases.