The anticancer activity of propolis

Propolis and its compounds have been the subject of many studies due to their antimicrobial and antiinflammatory activity; however, it is now known that they also possess antitumor properties. This review aims to summarize the results of studies on the mechanism of activity of propolis and its active compounds such as CAPE and chrysin in the apoptotic process, and their influence on the proliferation of cancer cells. Our review shows that propolis and its presented compounds induce apoptosis pathways in cancer cells. The antiproliferative effects of propolis, CAPE or chrysin in cancer cells are the result of the suppression of complexes of cyclins, as well as cell cycle arrest. The results of in vitro and in vivo studies suggest that propolis, CAPE and chrysin may inhibit tumor cell progression and may be useful as potential chemotherapeutic or chemopreventive anticancer drugs

Problem niedożywienia u chorych na nowotwory

The problem of nutrition disorders affects most patients with cancer. Prevention and treatment of malnutrition is dependent on the stage of the disease and the patient’s requirements. Doctor’s task is the assessment of nutrition status, treatment of malnutrition, and monitoring the effectiveness and safety of the treatment. It is worth remembering that patient can derive great benefits from an appropriate nutrition and from professional nutritionist care. Effective treatment can be carried out in the hospital as well as at patient’s home. Prevention and treatment of nutrition disorders can significantly improve the patient’s condition and the course of oncological treatment and best supportive care. Therefore, the problem of an appropriate nutrition should be considered in every patient with cancer.Problem zaburzeń odżywiania dotyczy większości chorych na nowotwory. Do zadań lekarza należy ocena stanu odżywienia, leczenie niedożywienia oraz monitorowanie efektywności i przebiegu terapii, w zależności od etapu choroby i potrzeb pacjenta. Warto pamiętać, że pacjent może odnieść dużą korzyść również z opieki dietetyka. Efektywne leczenie może być prowadzone w szpitalu i w domu chorego. Zapobieganie i leczenie zaburzeń odżywiania może w znaczący sposób poprawić stan pacjenta i przebieg leczenia onkologicznego oraz wspomagać leczenie objawowe, dlatego problem ten powinien być rozważony u każdego chorego na nowotwór

Propolis changes the anticancer activity of temozolomide in U87MG human glioblastoma cell line

BACKGROUND: Propolis is a honey bee product which contains many active compounds, such as CAPE or chrysin, and has many beneficial activities. Recently, its anti-tumor properties have been discussed. We have tested whether the ethanolic extract of propolis (EEP) interferes with temozolomide (TMZ) to inhibit U87MG cell line growth. METHODS: The U87MG glioblastoma cell line was exposed to TMZ (10-100 μM), EEP (10-100 μg/ml) or a mixture of TMZ and EEP during 24, 48 or 72 hours. The cell division was examined by the H(3)-thymidine incorporation, while the western blot method was used for detection of p65 subunit of NF-κB and ELISA test to measure the concentration of its p50 subunit in the nucleus. RESULTS: We have found that both, TMZ and EEP administrated alone, had a dose- and time-dependent inhibitory effect on the U87MG cell line growth, which was manifested by gradual reduction of cell viability and alterations in proliferation rate. The anti-tumor effect of TMZ (20 μM) was enhanced by EEP, which was especially well observed after a short time of exposition, where simultaneous usage of TMZ and EEP resulted in a higher degree of growth inhibition than each biological factor used separately. In addition, cells treated with TMZ presented no changes in NF-κB activity in prolonged time of treatment and EEP only slightly reduced the nuclear translocation of this transcription factor. In turn, the combined incubation with TMZ and EEP led to an approximately double reduction of NF-κB nuclear localization. CONCLUSIONS: We conclude that EEP presents cytotoxic properties and may cooperate with TMZ synergistically enhancing its growth inhibiting activity against glioblastoma U87MG cell line. This phenomenon may be at least partially mediated by a reduced activity of NF-κB

Czy wszystkie preparaty toksyny botulinowej typu A są takie same? Porównanie trzech preparatów toksyny botulinowej typu A w zarejestrowanych wskazaniach w neurologii

W ostatnim czasie lista klinicznych zastosowań toksyny botulinowej typu A (BTX-A) znacznie się wydłużyła. Substancja ta stała się narzędziem w rękach neurologów, lekarzy rehabilitacji, urologów, proktologów, migrenologów czy kosmetologów. Zwiększyła się także liczba produkowanych preparatów BTX-A. Obecnie na rynku dostępne są preparaty: Botox, Dysport i Xeomin. Mają one podobny mechanizm działania, aczkolwiek różnią się istotnie budową chemiczną, siłą działania, migracją poza miejsce podania, skutecznością i profilem działań niepożądanych. Te odrębności mogą sprawiać trudności w ich zamiennym stosowaniu przez niedoświadczonego lekarza. Rodzą także pytania o ich równowartość ekonomiczną. Autorzy dokonali przeglądu prac i porównali dostępne preparaty w zarejestrowanych w Polsce wskazaniach neurologicznych. Preparaty te powinny być traktowane jako odrębne leki, a ich zastosowanie kliniczne oparte o dane z badań klinicznych dotyczących poszczególnych preparatów

Magnetic particles with polymeric shells bearing cholesterol moieties sensitize breast cancer cells to low doses of doxorubicin

One of the promising strategies for improvement of cancer treatment is application of a combination therapy. The aim of this study was to investigate the anticancer activity of nanoformulations containing doxorubicin and iron oxide particles covered with polymeric shells bearing cholesterol moieties. It was postulated that due to high affinity to cell membranes, particles comprising poly(cholesteryl acrylate) can sensitize cancer cells to doxorubicin chemotherapy. The performed analyses revealed that the developed systems are effective against the human breast cancer cell lines MCF-7 and MDA-MB-231 even at low doses of the active compound applied (0.5 µM). Additionally, high compatibility and lack of toxicity of the tested materials against human red blood cells, immune (monocytic THP-1) cells, and cardiomyocyte H9C2(2-1) cells was demonstrated. Synergistic effects observed upon administration of doxorubicin with polymer–iron oxide hybrids comprising poly(cholesteryl acrylate) may provide an opportunity to limit toxicity of the drug and to improve its therapeutic efficiency at the same time

Are botulinum toxin type A preparations really the same medication? : a comparison of three botulinum toxin A formulations in labelled neurological indications

W ostatnim czasie lista klinicznych zastosowań toksyny botulinowej typu A (BTX-A) znacznie się wydłużyła. Substancja ta stała się narzędziem w rękach neurologów, lekarzy rehabilitacji, urologów, proktologów, migrenologów czy kosmetologów. Zwiększyła się także liczba produkowanych preparatów BTX-A. Obecnie na rynku dostępne są preparaty: Botox, Dysport i Xeomin. Mają one podobny mechanizm działania, aczkolwiek różnią się istotnie budową chemiczną, siłą działania, migracją poza miejsce podania, skutecznością i profilem działań niepożądanych. Te odrębności mogą sprawiać trudności w ich zamiennym stosowaniu przez niedoświadczonego lekarza. Rodzą także pytania o ich równowartość ekonomiczną. Autorzy dokonali przeglądu prac i porównali dostępne preparaty w zarejestrowanych w Polsce wskazaniach neurologicznych. Preparaty te powinny być traktowane jako odrębne leki, a ich zastosowanie kliniczne oparte o dane z badań klinicznych dotyczących poszczególnych preparatów.Recently, the list of clinical applications of botulinum toxin type A (BTX-A) enlarged. This medication is used not only by neurologists, but also by medical rehabilitation specialists, urologists, proctologists, and migraine and aesthetic medicine specialists. Currently, there are three commercially available BTX-A preparations available: Botox, Dysport and Xeomin. They have similar mechanisms of action but their chemical formulation, clinical potency, migration and diffusion as well as safety profile seem to be different. This may result in pro­blems of bioequivalence, not only clinical but also economic ones. The authors reviewed the available clinical and labora­tory studies on neurological indications labelled in Poland. Each BTX-A formulation should be treated as a different medication and used cautiously according to the individual range of dosages established in clinical trials

"Heterobasidion annosum" induces apoptosis in DLD-1 cells and decreases colon cancer growth in In vivo model

Application of substances from medicinal mushrooms is one of the interesting approaches to improve cancer therapy. In this study, we commenced a new attempt in the field of Heterobasidion annosum (Fr.) Bref. sensu lato to further extend our knowledge on this basidiomycete fungus. For this purpose, analysis of the active substances of Heterobasidion annosum methanolic extract and also its influence on colorectal cancer in terms of in vitro and in vivo experiments were performed. In vivo studies on mice were conducted to verify its acute toxicity and to further affirm its anticancer potential. Results indicated that all the most common substances of best known medicinal mushrooms that are also responsible for their biological activity are present in tested extracts. In vitro tests showed a high hemocompatibility and a significant decrease in viability and proliferation of DLD-1 cells in a concentration-dependent manner of Heterobasidion annosum extract. The studies performed on xenograft model of mice showed lower tendency of tumor growth in the group of mice receiving Heterobasidion annosum extract as well as mild or moderate toxicity. Obtained results suggest beneficial potential of Heterobasidion annosum against colon cancer as cytotoxic agent or as adjuvant anticancer therapy

Botulinum toxin type-A preparations are not the same medications — clinical studies (Part 2)

The growing number of Botulinum neurotoxin type A (BoNT/A) preparations on the market has resulted in a search for pharmacological, clinical and pharmacoeconomic differences. Patients are occasionally switched from one botulinum toxin formulation to another.The aim of this paper was to review studies that have made direct comparisons of the three major BoNT/A preparations presently on the market: ona-, abo- and incobotulinumtoxinA. We also review the single medication Class I pivotal and occasionally Class II-IV studies, as well as recommendations and guidelines to show how effective doses have been adopted in well-established indications such as blepharospasm, hemifacial spasm, cervical dystonia and adult spasticity.Neither direct head-to-head studies nor single medication studies between all preparations allow the formation of universal conversion ratios. All preparations should be treated as distinct medications with respect to their summary of product characteristics when used in everyday practice

Botulinum toxin type-A preparations are not the same medications — basic science (Part 1)

Botulinum neurotoxin type A (BoNT/A) formulations are widely used in clinical practice. Although they share a common mechanism of action resulting in presynaptic block in acetylocholine release, their structure and pharmacological properties demonstrate some similarities and many differences. Bioequivalence has been discussed since the onset of the clinical use of BoNT/A. In this review, we provide an update on the studies and compare the molecular structure, mechanisms of action, diffusion and spread, as well as immunogenicity and dose equivalence of onabotulinumtoxinA, abobotulinumtoxinA and incobotulinumtoxinA