| Current
Clinical Pharmacology
ISSN: 1574-8847
Current Clinical
Pharmacology
Volume 1, Number 3, September 2006
Contents
Hypericin Lights Up the Way for the Potential
Treatment of Nasopharyngeal Cancer by Photodynamic Therapy
Pp. 217-222
M. Olivo, H.-Y. Du and B.-H. Bay
[Abstract]
Sorafenib (BAY 43-9006): Review of Clinical Development
Pp. 223-228
R. Ng and E.X. Chen
[Abstract]
Nuclear Imaging of Inflammation in Neurologic
and Psychiatric Disorders Pp. 229-242
E.F.J. de Vries, R.A. Dierckx and H.C. Klein
[Abstract]
Pharmacologic Treatment of Rapid Ejaculation:
Levels of Evidence-Based Review Pp. 243-254
I.A. Abdel-Hamid
[Abstract]
The Relevance of Microdialysis for Clinical Oncology
Pp. 255-263
J.J.E.M. Kitzen, J. Verweij, E.A.C. Wiemer and W.J. Loos
[Abstract]
Chronopharmacology and Antimicrobial Therapeutics
Pp. 265-275
M. Rebuelto
[Abstract]
Drug Susceptibility of the Mycobacterium
Genus: In Vitro Tests and Clinical Implications
Pp. 277-289
J.C. Rodríguez, E. García-Pachon, M. Ruiz
and G. Royo
[Abstract]
Genetic and Environmental Influences on Therapeutic
and Toxicity Outcomes: Studies with CYP2A6 Pp. 291-309
S. Satarug, W. Tassaneeyakul, K. Na-Bangchang, J.R. Cashman
and M.R. Moore
[Abstract]
Clinical Pharmacokinetics of Irinotecan-Based
Chemotherapy in Colorectal Cancer Patients Pp. 311-323
A. Di Paolo, G. Bocci, R. Danesi and M. Del Tacca
[Abstract]
Abstracts
[Back to top]
Hypericin Lights Up the Way for the Potential Treatment
of Nasopharyngeal Cancer by Photodynamic Therapy
M. Olivo, H.-Y. Du and B.-H. Bay
Photodynamic therapy (PDT) involves the administration of
a photosensitizer followed by light irradiation with a specific
wavelength, giving rise to irreversible tissue destruction.
Hypericin, a herbal extract derived from Hypericum perforatum
or St. John’s Wort, has minimal toxicity but exhibits
potent photo-damaging effects in the presence of light. Hypericin
is known to generate a high yield of singlet oxygen and other
reactive oxygen species that are associated with photo-oxidative
cellular damage. The application of PDT with hypericin for
the treatment of cancers such as recurrent mesothelioma and
skin cancer has been validated in clinical trials. This mini-review
focuses on the investigative studies of hypericin as a potential
photodynamic agent in the treatment of nasopharyngeal cancer
(NPC) in in vitro and in vivo models. NPC
is an enigmatic tumor with a multifactorial etiology and a
high incidence in the populations of Southern China.
[Back to top]
Sorafenib (BAY 43-9006): Review of Clinical Development
R. Ng and E.X. Chen
Sorafenib (BAY 43-9006) is a novel oral bis-aryl urea compound
originally developed as an inhibitor to RAF kinase for its
anti-proliferative property. It also inhibits receptor tyrosine
kinases of multiple pro-angiogenic factors such as VEGFR-2/3,
Flt-3/ and PDGFR-β.
The combination of both its anti-proliferative and anti-angiogenic
properties makes sorafenib an attractive agent in cancer treatment.
Phase I studies demonstrated that sorafenib was well tolerated,
and the recommended phase II dose was 400 mg twice daily continuously.
Common toxicities included skin toxicity (rash and hand-foot
syndrome), gastrointestinal toxicities (nausea and diarrhea)
and fatigue. Anti-tumor activities were observed in multiple
tumors types including renal cell carcinoma and hepatocellular
carcinoma. Randomized phase III studies in these tumor types
are ongoing, and results are eagerly waited.
[Back to top]
Nuclear Imaging of Inflammation in Neurologic
and Psychiatric Disorders
E.F.J. de Vries, R.A. Dierckx and H.C. Klein
Cerebral inflammation is a common phenomenon during the progression
of neurodegenerative diseases. In general, neurodegenerative
diseases have unpredictable clinical courses and timely effective
treatment is not available. For effective clinical trials
on new drugs, suitable surrogate markers to monitor disease
progression are required. The extent of cerebral inflammation
could be such a surrogate marker. Nuclear imaging techniques,
like positron emission tomography (PET) and single photon
emission computed tomography (SPECT), have been applied to
monitor inflammatory processes in patients. Neuroinflammation
is accompanied by a variety of physiological changes, such
as changes in cerebral glucose metabolism and perfusion, cyclooxygenase-2
overexpression and microglia activation. Nuclear imaging has
utilized these physiological changes to visualize the inflammatory
process in various chronic or acute neurodegenerative diseases.
Expression of the peripheral benzodiazepine receptor in activated
microglia proved a suitable specific marker to detect neuroinflammation.
Currently, radiolabeled COX-2 inhibitors are under investigation
for this purpose. The causative of neuroinflammation is often
unknown, but the herpes simplex virus (HSV), for example,
has been implicated in several neurodegenerative diseases.
Recently, antiviral agents and antibiotics have been prepared
that might be applicable to discriminate specific viral or
bacterial infections. These radiolabeled compounds could also
be used to monitor the drug pharmacokinetics noninvasively
with PET. This review summarizes the progress that has been
made in nuclear imaging of neuroinflammation in neuropsychiatric
diseases.
[Back to top]
Pharmacologic Treatment of Rapid Ejaculation:
Levels of Evidence-Based Review
I.A. Abdel-Hamid
Rapid (premature) ejaculation (RE) is defined as persistent
or recurrent ejaculation with minimal sexual stimulation before,
upon, or shortly after penetration and before it is wished
by the man or his partner. RE is the most frequently encountered
sexual complaint of men and couples. Estimates suggest that
as many as one third of all sexually active men suffer from
RE. RE has been treated with various modalities. These include
behavioral therapy, topical applications, oral pharmacotherapy
and intracavernosal vasoactive drug injection. The success
rates of these modalities are variable, however, to date an
approved treatment does not exist. In this article, we review
the evidence surrounding the pharmacological management of
RE. The search included (i) a MEDLINE search from 1980 through
August 2005 limited to English-language medical literature;
(ii) relevant abstracts from 2003, 2004, and 2005; and (iii)
a pipeline search for therapeutics in development. The review
does not include behavioral therapy. The distinct feature
of this review is that the level of evidence supporting each
treatment will be discussed in details. Results showed that
there is consistent evidence which supports the daily use
of paroxetine, clomipramine, sertraline and fluoxetine for
the treatment of RE. There is no strong evidence suggesting
the use of these previous drugs on an as-needed basis. There
is strong evidence to suggest the use of dapoxetine on an
as-needed in RE. Available evidence indicates that topical
anesthetic agents such as prilocaine-lidocaine and SS-cream
appears to be effective in treatment of RE. There is no strong
evidence to suggest that PDEI5 could prolong IELT in RE when
used on-demand. In conclusion, based on literature data, although
some drugs may be effective in treatment of RE, more extended
multi-center prospective double-blind, placebo-controlled
stopwatch studies on the benefits of SSRIs, SNRIs and PDEI5
in RE are required.
[Back to top]
The Relevance of Microdialysis for Clinical Oncology
J.J.E.M. Kitzen, J. Verweij, E.A.C. Wiemer and W.J. Loos
Conventional pharmacokinetic trials in oncology measure the
total amount of drug and its metabolites in the plasma of
patients. These total drug concentrations are then correlated
with clinical parameters such as toxicity and/or drug efficacy.
However, total drug concentrations in plasma are often not
directly related to tumor or tissue concentrations and the
kinetics in (tumor) tissue may be very different from the
kinetics of the drug in plasma. As only the unbound fraction
of drugs can passively diffuse or can be actively transported
across the cell membrane of endothelial cells and penetrate
the tissues and tumor cells, binding of drugs to plasma components
may, in part, be responsible for the variability in clinical
outcomes. Also, variation in binding to cellular components
may be important. As an overall consequence, in in vivo
models high inter-individual variabilities of drug concentrations
in the tumor have been observed, which affected drug activity.
Many current cancer drug-therapies aim for a clinical benefit
at the edge of acceptable toxicity, without paying attention
to (variability in) plasma and tumor or tissue pharmacokinetics.
This review discusses the potential applicability of microdialysis,
a minimally invasive method used to determine the unbound
fraction of drugs in blood or in the interstitial fluid of
tissues, in clinical oncology. Although faced with some methodological
challenges, the technique offers many advantages over others,
and enables direct tumor assessment for pharmacokinetics and
even pharmacodynamics.
[Back to top]
Chronopharmacology and Antimicrobial Therapeutics
M. Rebuelto
Chronobiology studies the phenomenon of rhythmicity in living
organisms. Circadian rhythms are genetically determined and
are regulated by external synchronizers (i.e. light/day cycle).
Several biological processes involved in the pharmacokinetics
and pharmacodynamics of drugs are subject to circadian variations.
Chronopharmacology studies how biological rhythms impact on
drug pharmacokinetic (chronokinetics), pharmacodynamics (chronoesthesy)
and toxicity and determines whether time of day administration
modifies drug’s pharmacological characteristics. Chronotherapy
applies chronopharmacological studies to clinical treatments,
determining the best biological time for its dosing, i.e.
when beneficial effects are maximal and incidence and /or
intensity of related side-effects and toxicity are minimal.
Significant variations in the pharmacokinetics and toxicity
of antibiotics (aminoglycosides, beta-lactams and fluoroquinolones)
related to administration time are well known. The aims of
this review are to discuss, briefly, the currently accepted
model of the circadian system that substantiates endogenous
rhythmicity and to provide an update on the knowledge of circadian
rhythms applied to drugs used as medicines, with a special
mention to the possible impact on antimicrobial treatments.
It is concluded that the dosing time of an antimicrobial agent
might be clinically relevant in some treatments, thus, clinicians
should be aware that the dosing time might affect the clinical
response of a drug.
He thought of himself, frying bacon and eggs in his
own kitchen at home –for he could feel inside that it
was high time for some meal or other, but that only made him
miserable.
The Hobbit, J.R.R. Tolkien
[Back to top]
Drug Susceptibility of the Mycobacterium
Genus: In Vitro Tests and Clinical Implications
J.C. Rodríguez, E. García-Pachon, M. Ruiz
and G. Royo
This review describes the mechanisms of drug resistance of
the most clinically relevant mycobacteria and the methods
that have been used for studying drug susceptibility (pnenotype,
genotype and in vivo tests) and it describes the
more important resistance mechanisms to the drugs.
Also, this review describes the relationship between microbiological
and pharmacological data and the importance of latency –stationary
phase- in mycobacteria.
Current clinical guidelines on the treatment of tuberculosis
(populations of Mycobacterium tuberculosis within
the host, drugs and duration, importance of HIV infection
in the treatment of tuberculosis, and treatment of latent
tuberculosis) and other diseases caused by mycobacteria (specially
associated a Mycobacterium kansasii, Mycobacterium avium
complex, Mycobacterium fortuitum and Mycobacterium
chelonei) are commented in view of drug resistance information,
including the more commonly accepted treatments to these diseases.
In addition, the impact of pharmacological studies in predicting
response to therapy is reviewed.
Finally, it describes the new methods of susceptibility testing
and the new antituberculous drugs.
[Back to top]
Genetic and Environmental Influences on Therapeutic
and Toxicity Outcomes: Studies with CYP2A6
S. Satarug, W. Tassaneeyakul, K. Na-Bangchang, J.R. Cashman
and M.R. Moore
The idea that the liver enzyme cytochrome P450 2A6 (CYP2A6),
known also as nicotine C-oxidase, is one of the determinants
of smoking addiction and smoking behavior is primarily based
on its role in nicotine metabolism and disposition. The results
of studies linking the CYP2A6 genetic polymorphism
with smoking dependence and smoking behavior however remain
controversial. The most likely causes of the controversies
appeared to be consideration given to a few allelic variants
coupled with the uses of the CYP2A6 alleles lacking
in vivo phenotypic validation. In the present review,
we summarize research findings on biological significance
of CYP2A6 and gene polymorphisms together with a discussion
on CYP2A6 inhibitors that hold the promise of uses in smoking
cessation. In addition, we provide the pheno-type/genotype
information derived from our systematic investigation on the
relationship between CYP2A6 genotypes, smoking habits
and coumarin metabolism phenotypes in a group of 393 normal
adults (197 women and 196 men), 16 to 60 years of age, whose
exposure to cadmium and lead were also determined, enabling
us to assess the CYP2A6 phenotypic variability associated
with CYP2A6 genotypes and environmental exposure.
The results indicate that the phenotype of CYP2A6 enzyme in
liver is an outcome of interactions between the CYP2A6
gene, cadmium, nicotine and possibly its metabolites.
[Back to top]
Clinical Pharmacokinetics of Irinotecan-Based
Chemotherapy in Colorectal Cancer Patients
A. Di Paolo, G. Bocci, R. Danesi and M. Del Tacca
Irinotecan (CPT-11) significantly improves the efficacy of
colorectal cancer treatment, demonstrating a superior efficacy
with respect to leucovorin-modulated 5-fluorouracil (5-FU),
also in fluoropyrimidine-resistant neoplasms. Preclinical
studies demonstrated the inhibition of topoisomerase I by
CPT-11 active metabolite 7-ethyl-10-hydroxycamptothecin (SN-38),
and the possible synergistic interaction with other drugs
effective against colorectal cancer, including 5-FU and oxaliplatin.
Because of the occurrence of toxicities due to the large interpatient
variability in drug metabolism, irinotecan is a candidate
for therapeutic drug monitoring and pharmacokinetic optimisation.
New schedules of drug administration (i.e. prolonged infusion)
have led to improved cytotoxic effect of irinotecan, which
resulted in improved overall survival and time to relapse
together with reduced toxicity in comparison with 5-FU-based
regimens. Furthermore, the analysis of the conversion of irinotecan
into SN-38 by carboxylesterase, the detoxification of irinotecan
and SN-38 by CYP3A4 and UDP-glucuronosyl transferases, and
the activity of excretory systems (i.e., cMOAT, P-gp and MRP)
seems able to predict the interindividual variability in pharmacokinetics
and pharmacodynamics, being possible to predict untolerable
toxicities. Finally, pharmacogenetics may elucidate drug interaction
and gene expression modulation by irinotecan, while pharmacokinetic/pharmacodynamic
models represent a valuable approach to further define the
pharmacologic profile of irinotecan and improve its therapeutic
index.
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