Temporary transvenous cardiac pacing in a dog with diltiazem intoxication
Journal of Veterinary Emergency and Critical Care 18(1) 2008, pp 75–80
Temporary transvenous cardiac pacing in a dogwith diltiazem intoxication
Rebecca S. Syring, DVM, DACVECC, Merilee F. Costello, DVM, DACVECC and Robert H. Poppenga, DVM, PhD, DABVT
Objective: This case report presents the clinical findings of a dog with diltiazem intoxication and theutilization of temporary transvenous pacing for management of high-grade second-degree atrioventricular(AV) block with associated bradycardia and hypotension. Case summary: A nine-year-old spayed female Basset Hound, who ingested between 95 and 109 mg/kg ofsustained-release diltiazem exhibited clinical signs of cardiac arrhythmias, bradycardia, hypotension, mentaldepression and gastrointestinal (GI) upset. Bradycardia was present initially, then was followed by high-gradesecond-degree AV block with ventricular escape. Traditional medications to treat calcium channel blocker(CCB) intoxication, including atropine, calcium gluconate, dopamine and glucagon were initially successful inmanaging the cardiac rhythm disturbances and hypotension. Twenty-two hours post-ingestion, however, thedog became refractory to these medications following sedation for GI decontamination and a temporarytransvenous pacemaker was placed. The dog was paced for 19 hours. Transvenous pacing effectivelyincreased heart rate, which increased blood pressure into an acceptable range. The dog was successfullydischarged from the hospital following treatment. New or unique information provided: The use of a temporary pacemaker should be considered anacceptable treatment for bradycardia, AV block and hypotension associated with CCB intoxication whenconventional medical therapy fails.
(J Vet Emerg Crit Care 2008; 18(1): 75–80) doi: 10.1111/j.1476-4431.2007.00269.x
Keywords: AV block, bradycardia, calcium channel antagonist, calcium channel blocker, hypotension, pace-maker
contained 300 mg sustained-release diltiazem cap-sules.b The owners estimated that the dog had ingest-
ed 7–8 capsules (95–109 mg/kg). The dog had no overt
A nine-year-old spayed female Basset Hound, weigh-
abnormal clinical signs at that time and she ate a meal
ing 22 kg, was referred for treatment following inges-
shortly thereafter. One and one-half hours after the
tion of the owner’s diltiazem. This dog had been
owners noted the ingestion, the dog was let outside into
diagnosed with unilateral laryngeal paralysis and
the fenced backyard where she was found a few min-
pneumonia based upon a positive transtracheal wash
utes later, collapsed and unresponsive. She was taken
culture one month previously, for which she was
immediately to the local emergency veterinary hospital.
receiving oral enrofloxacina therapy.
At presentation to the local veterinarian, she was
Four hours before referral, the owners returned home
laterally recumbent and bradycardic (heart rate range
to find that the dog had chewed open a pill vial that
30–50 b.p.m.). Intravenous (IV) isotonic crystalloidsolution (rate unknown) and atropine (0.01 mg/kg,
From the Section of Critical Care, Department of Clinical Studies –
IV) were administered. After noting no response to
Philadelphia, School of Veterinary Medicine, University of Pennsylvania,
the initial dose of atropine, a second dose (0.01 mg/kg,
Philadelphia, PA (Syring, Costello) and California Animal Health and FoodSafety Laboratory, School of Veterinary Medicine, University of California
IV) of atropine was administered, wherein the heart
rate normalized and increased to 100 b.p.m. At that
Address correspondence and reprint requests to:
time, an electrocardiogram (ECG) revealed second-
Dr. Rebecca S. Syring, Room 2066, VHUP, 3900 Delancey Street, Philadel-
degree atrioventricular (AV) block with a ventricular
phia, PA 19104-6010. E-mail [email protected]
escape rhythm. Calcium gluconate (22.7 mg/kg, IV)
& Veterinary Emergency and Critical Care Society 2008
was administered over 10–15 minutes. Following this
An IV bolus of glucagoni (0.04 mg/kg) was admin-
treatment, the heart rate increased to approximately
istered. Within five minutes of administration, the car-
160–180 b.p.m., and the dog was referred for ongoing
diac rhythm converted to a normal sinus rhythm and
the heart rate increased to 130 b.p.m. With this change
At presentation to the emergency room, the dog
in heart rate and rhythm, the mean arterial blood pres-
was mentally dull and recumbent. The heart rate was
sure increased to 89 mmHg. As there was a positive
bradycardic (50 b.p.m.) with adequate peripheral puls-
response to the glucagon bolus, a glucagon CRI
es. The mucous membranes were pink with a capillary
was initiated at 0.04 mg/kg/hr because glucagon has
refill time o2 seconds. The respiratory rate and effort
only a 3–6-minute duration of action when given as
were normal, with notable inspiratory stridor. Abdom-
inal palpation revealed a tense abdomen and elicited
An arterial blood gas was obtained that revealed
unproductive retching. No other abnormalities were
significant hypoxia (PaO2 5 58 mmHg, at an inspired
found on the remainder of the physical examination.
oxygen concentration [FiO2] of 0.21). Radiographs
Emergency blood screening revealed hemoconcen-
revealed marked alveolar infiltrates in the right crani-
tration (PCV 60%) but no other significant abnormal-
al and middle lung lobes, consistent with aspiration
ities. Second-degree AV block with a junctional rhythm
pneumonia. Decreased gastric transit time was also
and occasional ventricular escape beats persisted on the
present since the ingesta, which had been noted on
ECG. Arterial blood pressure was not measured at the
radiographs 12 hours earlier, was still visible in the
time of initial presentation. The only notable finding on
stomach. Metoclopramidej (1 mg/kg/day, CRI) and
abdominal radiographs was a distended stomach con-
ranitidinek (1 mg/kg, IV, q 12 h) were instituted for
signs of decreased gastric motility.
An IV balanced electrolyte solutionc was adminis-
Gastrointestinal (GI) decontamination (approximate-
tered at 4 mL/kg/hr. One dose of prochlorperazined
ly 20 hours post-ingestion of diltiazem) was thought
(0.2 mg/kg, IM) was administered for persistent
to be worthwhile because the ingested drug was a
unproductive retching, and enrofloxacina (10 mg/kg,
sustained-release formulation, there was evidence of
IV, q 24 h) was continued as prescribed previously for
delayed gastric emptying, and the dog had not vomited
ongoing treatment of bacterial pneumonia.
productively (despite retching). Once the aforemen-
Within two hours of presentation, the blood pressure
tioned drugs provided a more stable heart rate, rhythm
was judged to be inadequate based on subjective palpa-
and blood pressure, general anesthesia was induced to
tion of arterial pulses. At that time, indirect measure of
perform gastric decontamination with a protected air-
arterial blood pressure by Dopplere was attempted and
way given the dog’s decreased mentation and history
was determined to be hypotensive. A constant rate infu-
of laryngeal paralysis. General anesthesia was induced
sion (CRI) of dopaminef was instituted at 5 mg/kg/min.
with etomidatel (0.3 mg/kg, IV) and midazolamm
At this dose, systolic blood pressure increased to
(0.5 mg/kg, IV) and maintained with intermittent
50 mmHg. A 500 mL IV bolus of a balanced electrolyte
boluses of etomidate (0.2 mg/kg, IV to effect). Gastric
solutionc was administered over 30 minutes in an effort
lavage was performed and activated charcoaln with
to improve perfusion. The dopamine dose was titrated
magnesium citrate was administered via a large bore
upwards from 5 to 10 mg/kg/min as needed to main-
orogastric tube. At that time an endotracheal lavage
tain systolic blood pressure as measured by Doppler
was performed and ticarcillin/clavulanateo (50 mg/kg,
above 100 mmHg. During the following eight hours, the
IV, q 6 h) was added to increase the antimicrobial spec-
dog’s heart rate ranged from 50 to 100 b.p.m. An ad-
trum pending results of culture and sensitivity testing.
ditional dose of atropineg (0.02 mg/kg, IV) was admin-
Initially, the glucagon CRI was effective at maintain-
istered; however, the heart rate never exceeded
ing a normal heart rate, rhythm and blood pressure, but
during general anesthesia, the dog gradually became
The following morning the dog was transferred to
more refractory to this therapy. First-degree AV block
the intensive care unit. She remained mentally dull and
returned, which progressed to a high-grade second-de-
recumbent. The dog was placed on a continuous
gree AV block. At this time the heart rate remained
ECG, which revealed persistent high-grade second-
between 45 and 50 b.p.m. with a MAP of 55 mmHg.
degree AV block with ventricular escape beats. A 11 in:
Repeated bolus doses of atropine (0.02 mg/kg, IV), 10%
22-gauge catheterh was percutaneously placed in a
calcium gluconate (9–13.6 mL/kg, IV) and glucagon
dorsal pedal artery for continuous direct arterial
(0.08 mg/kg, IV) were administered but found to have
blood pressure monitoring. Despite 10 mg/kg/min of
limited to no effect. Progressive bradycardia and
dopamine, she remained hypotensive, with a mean ar-
refractory hypotension that persisted approximately
one hour beyond the last dose of etomidate were the
& Veterinary Emergency and Critical Care Society 2008, doi: 10.1111/j.1476-4431.2007.00269.x
Transvenous pacing for diltiazem toxicity
primary reasons contributing to the decision to place a
increased in parallel with the frequency of their use.3 In
human medicine, 9650 cases of CCB ingestion were re-
A 6 Fr, 5.5 cm introducerp was inserted percutane-
ported in 2003. Of these reported cases, 1481 were
ously into the right jugular vein, through which a 6 Fr
deemed moderate to severe intoxications, with 57
bipolar pacing wireq was inserted into the right ventri-
deaths reported.4 In veterinary medicine, 390 cases of
cle. Ventricular capture was successful without the
CCB overdose were reported to the American Society
need for fluoroscopic guidance. The pacing wire was
for the Prevention of Cruelty to Animals National An-
attached to an external pulse generatorr and pro-
imal Poison Control Center between 1995 and 2000.5
grammed to pace the ventricle at a heart rate of
CCBs act at voltage sensitive slow L-type calcium
80 b.p.m. in a ventricular demand mode (VVI). At this
channels, inhibiting intracellular influx of calcium.
heart rate, the mean arterial blood pressure was be-
Limiting intracellular calcium inhibits both actin–myo-
sin cross-linking in blood vessels and excitation–con-
Nineteen hours after placement of the pacemaker (41
traction coupling in the myocardium. In addition,
hours post-ingestion) the spontaneous heart rate and
inhibition of intracellular calcium suppresses automati-
rhythm had returned to normal, such that the pace-
city at the sinoatrial and AV nodes.6–8 These actions
maker was suppressed from firing. The dog was dis-
result in varying degrees of vasodilation, negative ino-
connected from the external pulse generator and, when
tropy, decreased automaticity and suppressed AV con-
it was determined that the cardiac rhythm was stable,
duction, depending upon the type of CCB used.8
the pacing wire was removed. Throughout the duration
Diltiazem, a CCB in the benzothiazepine family, is
of pacing and after discontinuation of transvenous pac-
used clinically in both human and veterinary medicine.
ing, no additional medical therapy was needed to
The benzothiazepine family is reported to have pro-
maintain heart rate, rhythm or blood pressure.
found depressant effects on cardiac automaticity and
Stored serum samples were submitted for evaluation
conduction and moderate effects on vascular tone.6–8
of diltiazem concentrations by high-performance liquid
The dog in this report ingested between 95 and
chromatography.2 The samples had been collected ap-
109 mg/kg of a sustained-release formulation of diltia-
proximately 18 and 48 hours after the latest possible
zem. The therapeutic dose published for short-acting
exposure to the diltiazem (time 0 being the time when
diltiazem in the canine species ranges from 0.5 to
the owners found the empty pill vial at home).
1.5 mg/kg, orally, every eight hours.9 There is little
Diltiazem was quantified at 1300 ng/mL (1.30 p.p.m.)
data regarding the use of sustained-release formula-
in the sample 18 hours post-exposure but was unde-
tions in dogs and it is important to recognize that dos-
tectable in the 48-hour sample. The lower limit of de-
ing varies depending on the formulation of the
tection for this assay was 250 ng/mL (0.25 p.p.m.).
sustained-release product. For instance, a dosage of
The dog remained hospitalized for four days after
1.5–6.0 mg/kg every 12–24 hours has been recommend-
discontinuation of transvenous pacing (6 days after the
ed in dogs for one extended-release formulation10,t but
initial intoxication), primarily for supportive oxygen
the dosage recommended for sustained-release prod-
therapy and medical management of aspiration pneu-
uctu ingested by the dog reported here is 10 mg/kg,
monia. Escherichia coli sensitive to cefixime was cultured
orally, once daily. Based upon this dose, the dog in this
and the dog was discharged on oral cefpodoximes
report ingested at least 9.5 times the lower end of the
(10 mg/kg, PO, q 12 h). At a follow-up examination
therapeutic dose. The lowest reported oral LD50 for
two weeks after discharge, the dog was doing well and
diltiazem is 50 mg/kg in dogs.11,v In a retrospective
there was radiographic resolution of the pneumonia.
human study of CCB intoxication, the mean toxic doseof diltiazem was 2167 mg (approximately 30 mg/kg). The study did not differentiate short-acting from sus-
tained-release formulations when reporting toxic doses;
Calcium channel blockers (CCBs) are common medica-
however, almost half of the intoxications reported in-
tions used to treat both humans and animals with a
volved sustained-release formulations.3 Therefore, the
variety of cardiac and vascular disorders. There are
dose that this dog ingested was substantially higher
three different families of CCB and at least 10 different
than that reported in the human study.
types of CCB commercially available. The therapeutic
Traditional short-acting formulations of diltiazem are
effect depends primarily upon the drug family, with
rapidly cleared by first-order kinetics following oral
some agents (e.g., amlodipine) mostly causing vasodi-
administration, with a half-life of 3–5 hours.v However,
lation, while others (e.g., verapamil or diltiazem) have
sustained-release formulations cause a slow, continual
mixed effects on both the systemic vasculature and
release of the drug, which prolongs its half-life. The
heart. The incidence of human CCB intoxications has
product that this dog ingested is reported to reach
& Veterinary Emergency and Critical Care Society 2008, doi: 10.1111/j.1476-4431.2007.00269.x
detectable plasma concentrations within two hours,
insulin administration. Discussion of these therapies
with peak concentrations occurring 10–14 hours after
is beyond the scope of this report and can be reviewed
administration of a therapeutic dose.v Its elimination
in detail elsewhere.5,7,19 Treatment with various com-
half-life is reported to be 5–8 hours following thera-
binations of the aforementioned drugs has failed to
peutic dosing.v The pharmacokinetics of sustained-re-
yield consistent responses to these therapies in case re-
ports of human intoxications.3 In this dog, all these
investigated in dogs. However, the product that this
agents were used, with the exception of insulin, and
dog ingested has been shown to have a terminal half-
many were initially successful in maintaining heart rate
life of 7.6 hours and 36% bioavailability following once
and blood pressure. However, over the course of the
daily oral dosing at 10 mg/kg in healthy cats.12
first 24 hours, the dog became refractory to their ad-
While the half-lives of short-acting and sustained-re-
lease formulations of diltiazem are established for ther-
The dose of glucagon that was used in this dog (0.04–
0.08 mg/kg, IV bolus; CRI 0.04 mg/kg/hr) is lower than
supratherapeutic doses may differ. One study reports
that considered to be appropriate in humans (0.15 mg/kg,
half-lives of 5–10 hours following toxic doses of short-
IV bolus; CRI 0.05–0.10 mg/kg/hr) for treatment of
acting diltiazem, which is longer than reported for
CCB overdose.1 However, the dose administered was
therapeutic doses.13 Isolated case reports demonstrate
higher than doses published (0.05 mg/kg, IV bolus; CRI
that the elimination half-life can be dramatically longer
0.6–0.9 mg/kg/hr) for treatment of hypoglycemia in
and extremely variable following ingestion of supra-
dogs.20 Although the dose of glucagon used in this dog
therapeutic doses of diltiazem.14–16 A retrospective
was lower than recommended, a positive but transient
study of a CCB intoxication in humans reported that
therapeutic effect was noted. It is possible that use of a
the onset of clinical signs may be delayed by 6–12 hours
higher dose may have resulted in longer term efficacy;
following ingestion of a toxic dose of sustained-release
however, this would have been cost prohibitive if used
for as many hours as the dog required pacing.
Serum concentrations of diltiazem were quantified at
Because the dog in this case report had been retching,
1300 ng/mL (1.3 p.p.m.) 18 hours post-intoxication in
GI decontamination was not initially attempted. Gastric
this dog and below the range of detection 48 hours
lavage and administration of activated charcoal was not
post-intoxication. Therapeutic serum concentrations of
performed until approximately 20 hours after ingestion.
diltiazem in humans are reported to range from 50 to
Optimally, GI decontamination should have been per-
200 ng/mL (0.05–0.20 p.p.m.).v Therapeutic serum con-
formed within four hours of intoxication. However, in
centrations of diltiazem are not published for dogs, but
massive overdoses, sustained-release formulations can
should approximate those concentrations recommend-
form concretions within the GI tract that can persist for
ed for humans.17 The serum concentration measured 18
days.21 Therefore, based upon radiographic evidence of
hours post-ingestion represents a value 6.5 times above
ingesta persisting within the stomach the following day
the high end of the therapeutic range. Because serum
and the progression of the dog’s clinical signs, we felt
concentrations were not obtained more frequently dur-
that the dog would benefit from GI decontamination
ing the first two days following intoxication, it is diffi-
even 20 hours post-intoxication. Although repeated
cult to predict the peak serum concentration for this
doses of charcoal have not proven effective in cases of
dog. However, it is likely that the concentration ob-
short-acting diltiazem intoxication,13 repeated or de-
tained 18 hours post-ingestion was lower than the peak
layed administration of activated charcoal may help
serum concentration. A serum concentration as high as
limit further systemic absorption of sustained-release
6090 ng/mL has been documented in a human who
formulations.21 Extracorporeal removal, such as hemo-
survived acute intoxication with short-acting diltia-
dialysis, might enhance drug elimination, but such in-
zem.15,17 Reports of sustained-release intoxication are
terventions are unlikely to alter clinical outcome and
less prevalent in the literature, however a serum con-
centration as high as 3171 ng/mL was reported in a
A temporary transvenous pacemaker was inserted in
person who survived intoxication.14 In humans, plasma
this dog because of persistent bradycardia, AV block
concentrations of CCB do not appear to correlate with
and hypotension despite standard medical therapy.
A temporary pacemaker was selected because thearrhythmia was expected to be transient in nature,
Treatments for toxicity and novel information
negating the need for long-term pacing. Alternative
There are numerous reported treatments for CCB in-
routes of temporary pacing include transesophageal
toxication including calcium supplementation, para-
and transthoracic, although the use of transesophageal
sympatholytic agents, vasopressors, glucagon and
pacing has only recently been described in veterinary
& Veterinary Emergency and Critical Care Society 2008, doi: 10.1111/j.1476-4431.2007.00269.x
Transvenous pacing for diltiazem toxicity
medicine.w Transthoracic pacing was not used in this
pacing seems to be more common with overdoses of
patient because heavy sedation or general anesthesia is
verapamil,26–30 while most positive responses to pacing
often required to minimize skeletal muscle activity and
involve diltiazem overdoses.3,7,15,16,31–36 Verapamil,
alleviate pain.22 If the transvenous pacemaker could not
which is in a different family of CCB, is known to
be placed with ease, the dog could have been paced
exert more profound effects on vasomotor tone, ino-
externally with transthoracic paddles under anesthesia
tropy and cardiac conduction compared to diltiazem.21
while a transvenous pacemaker could be placed.
Thus, it is possible that ventricular pacing to a higher
The diltiazem overdose likely decreased cardiac out-
heart rate is less likely to compensate for the more
put in this dog by altering both heart rate and stroke
profound vasodilation and impairment in contractility
volume. A decreased heart rate was noted secondary to
AV blockade. While not directly measured by invasive
The fact that diltiazem was undetectable in this dog’s
cardiac output monitoring, stroke volume may also
serum 48 hours post-ingestion corresponds with the
have been decreased in this dog given the negative
clinical signs. The need for pacemaker support until 41
inotropic properties of diltiazem. By pacing the dog’s
hours post-intoxication corresponds with the metabo-
ventricle to a higher heart rate, cardiac output was in-
creased, which subsequently increased systemic bloodpressure, despite having no effect on inotropy or vaso-motor tone.
It is important to note that the dog became resistant
This report outlines the use of temporary transvenous
to medical therapy during general anesthesia. Anes-
pacing as an adjunct to conventional medical therapy in
thesia may have played a role in this dog’s clinical de-
a case of severe diltiazem intoxication in a dog. When
terioration by directly altering cardiac function and
traditional therapies, such as atropine, calcium, gluc-
vasomotor tone or by blunting the physiologic response
agon and other vasopressors fail to maintain blood
to such changes. Etomidate and midalozam, the only
pressure and perfusion, temporary pacing should be
anesthetics used, are reported to have minimal effects
considered as a means to improve cardiac output.
on the cardiovascular system and are preferred in car-diovascular instability.23,24 Additionally, the doses ofetomidate used to maintain anesthesia in this dog
(0.2 mg/kg) were much lower than published doses for
The authors graciously thank Margie Cummings in the
Laboratory of Large Animal Pathology and Toxicology
The use of prochlorperazine as an antiemetic early in
at the University of Pennsylvania for her assistance in
the course of this intoxication was contraindicated.
determining serum diltiazem concentrations.
Prochlorperazine acts primarily by a-2 antagonism,which can impair vasoconstriction, adding to thehypotensive effects seen with diltiazem. In addition it
has mild anticholinergic effects which could contribute
Baytril, Bayer Health Care LLC, Shawnee Mission, KA.
Cardizem-CD, Biovail Pharmaceuticals Incorporated, Morrisville, NC.
The pacemaker was placed in a ventricular demand
Normosol-R, Hospira Inc., Lake Forest, IL.
Compazine, GlaxoSmithKline, Research Triangle Park, NC.
mode. In this mode, if the spontaneous rate of the heart
Ultrasonic Doppler Flow Detector, Model 811-BL, Parks Medical
is slower than the set rate of the pacemaker, the pace-
Dopamine HCl, American Regent Inc., Shirley, NY.
maker will discharge and trigger a depolarization.
Atropine SA, The Butler Company, Columbus, OH.
However, if the spontaneous rate exceeds that set for
BD Insyte, Becton Dickinson, Sandy, UT.
the pacemaker, the pacemaker will sense this depolar-
Glucagon, Bedford Laboratories, Bedford, OH.
Reglan, SICOR Pharmaceuticals Inc., Irvine, CA.
ization and be temporarily suppressed. This is a supe-
rior mode of ventricular pacing, because it prevents
Amidate, Itospira Inc., Lake Forest, IL.
Midazolam, Baxter Healthcare Corp., Deerfield, IL.
depolarization of the ventricle during repolarization,
Actidose, Paddock Laboratories, Minneapolis, MN.
which could predispose to fibrillation.25 Performing
brief pacemaker cessation trials may have been helpful
Avanti1, Cordis Corporation, Miami, FL.
in this dog to determine if the pacemaker could have
Temporary pacemaker placement is occasionally
Dilacor XR, Watson Pharmaceuticals Inc., Corona, CA.
used in human CCB intoxication. Similar to other rec-
North American Companion Animal Formulary, Sixth Edition, 2004,
ommended therapeutic interventions, the clinical re-
published online at http://www.vin.com/Members/Drug/NACA.plx?ID=257.
sponse to pacing is variable. The lack of response to
Product monograph, Cardizem CD, Biovail Laboratories Incorporated.
& Veterinary Emergency and Critical Care Society 2008, doi: 10.1111/j.1476-4431.2007.00269.x
Sanders RA, Green HW III, Hogan DF, et al. Efficacy of transesophageal
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Tom Stade STAR OF BBC ONEʼS LIVE AT THE APOLLO & MICHAEL MCINTYREʼS COMEDY ROADSHOW CH4ʼS STAND-UP FOR THE WEEK & DAVEʼS ONE NIGHT STAND Since arriving in the UK, Canadian émigré Tom Stade has steadily earned a reputation as one of the most original and exciting stand-up talents around. He instantly made a splash on the UK circuit with his magnetic stage presence, i
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