Очень ранний клинический ответ при лечении ингибитором янус-киназ тофацитинибом у больных активным ревматоидным артритом: динамика боли и элементов центральной сенситизации

Janus kinase (JK) inhibitors block the intracellular signaling pathways that are responsible for the synthesis of proinflammatory cytokines and mediators, which in turn cause the activation of pain receptors and central sensitization (CS). It is suggested that JK inhibitors can rapidly eliminate pain and reduce the severity of CS.Objective: to evaluate the effect of the JK inhibitor tofacitinib (TOFA) on the intensity of pain and the signs of CS in patients with active rheumatoid arthritis (RA) at 7 and 28 days after therapy initiation.Patients and methods. A study group consisted of 39 patients (79.5% female) (mean age 50.9±11.1 years) with RA (DAS28 5.8±0.6). Of these, 89.7% were seropositive for rheumatoid factor; 82.0% took methotrexate and 18.0% received leflunomide. All the patients were prescribed TOFA 5 mg twice daily due to the inefficacy or intolerance of biological agents. The investigators estimated pain intensity using a Brief Pain Inventory (BPI), rated the presence of a neuropathic pain component (NPC) with the PainDETECT questionnaire, and assessed the signs of CS with the Central Sensitization Inventory (CSI) during the first 4 weeks after TOFA administration.Results and discussion. The patients initially experienced moderate or severe pain (the mean scores of 5.33±2.51 on the numerical rating scale (NRS) included in BPI); 53.8% had signs of CS (CSI scores of ≥40); 17.9% had signs of a NPC (PainDETECT scores of >18). Already on day 7 after the start of TOFA administration, there was a statistically significant decrease in the mean NRS pain intensity scores to 4.06±2.2 (p=0.01) and by 29.4±17.9%, as shown by the patient's assessment of the analgesic effect of therapy (BPI), as well as the severity of CS, namely a decrease in the mean NRS pain score to 35.9±11.2 (p=0.01). On 28 days, the effect became better: there was a reduction in the level of NRS pain to 2.32±1.57 (p<0.001), in pain according to the patient's assessment of the analgesic effect of therapy to 43.6±29.6%; in the median PainDETECT score to 2.5 [0; 8.7] (p<0.001); and in CSI scores to an average of 26.4±13.9 (p <0.001). No serious adverse reactions were noted.TOFA has a rapid analgesic effect, which allows it to be considered as a chooser for pathogenetic therapy in patients with active RA and severe pain, especially in the presence of CS signs and secondary fibromyalgia. Undoubtedly, large-scale, long-term controlled studies with a wider range of estimated parameters are required to clarify the therapeutic potential of TOFA in this patient category. The limitation of this investigation was its open observer design pattern.Conclusion. The use of the JK inhibitor TOFA can achieve a rapid analgesic effect, inter alia due to its effect on CS and NPC.Ингибиторы янус-киназ (ЯК) блокируют внутриклеточные сигнальные пути, отвечающие за синтез провоспалительных цитокинов и медиаторов, которые, в свою очередь, вызывают активацию болевых рецепторов и развитие центральной сенситизации (ЦС). Предполагается, что ингибиторы ЯК могут быстро устранять боль и уменьшать выраженность ЦС.Цель исследования – оценить влияние ингибитора ЯК тофацитиниба (ТОФА) на выраженность боли и признаки ЦС у больных активным ревматоидным артритом (РА) через 7 и 28 дней после начала терапии.Пациенты и методы. Исследуемую группу составили 39 больных РА (средний возраст 50,9±11,1 года, 79,5% женщин), DAS28 – 5,8±0,6. Из них 89,7% были серопозитивными по ревматоидному фактору, 82,0% получали метотрексат и 18,0% – лефлуномид. Всем пациентам был назначен ТОФА 5 мг 2 раза в день в связи с неэффективностью или непереносимостью генно-инженерных биологических препаратов. Оценивались выраженность боли с помощью опросника BPI (Brief Pain Inventory), наличие невропатического компонента боли (НКБ) с помощью опросника PainDETECT и признаков ЦС с помощью опросника CSI (Central Sensitization Inventory) в первые 4 нед после назначения ТОФА.Результаты и обсуждение. Пациенты исходно испытывали умеренную или выраженную боль (в среднем 5,33±2,51 по числовой рейтинговой шкале – ЧРШ, включенной в BPI), 53,8% имели признаки ЦС (CSI ≥40), 17,9% – признаки НКБ (PainDETECT >18). Уже через 7 дней после начала приема ТОФА отмечалось статистически значимое снижение интенсивности боли в среднем до 4,06±2,2 по ЧРШ (р=0,01) и на 29,4±17,9% по оценке анальгетического эффекта терапии пациентом (BPI), а также выраженности ЦС – уменьшение значения CSI в среднем до 35,9±11,2 (р=0,01). Через 28 дней эффект усилился: наблюдалось снижение уровня боли по ЧРШ до 2,32±1,57 (р<0,001), боли по оценке анальгетического эффекта терапии пациентом до 43,6±29,6%, медианы значения PainDETECT до 2,5 [0; 8,7] (р<0,001), показателя CSI в среднем до 26,4±13,9 (р<0,001). Серьезных неблагоприятных реакций не отмечено. ТОФА обладает быстрым анальгетическим эффектом, что позволяет рассматривать его как средство выбора при проведении патогенетической терапии у больных активным РА с выраженной болью, особенно при наличии признаков ЦС и вторичной фибромиалгии. Несомненно, требуются большие по масштабу длительные контролируемые исследования с более широким кругом оцениваемых параметров для уточнения лечебного потенциала ТОФА у этой категории пациентов. Ограничением настоящего исследования явился его открытый наблюдательный характер.Заключение. Использование ингибитора ЯК ТОФА позволяет достичь быстрого анальгетического эффекта, в том числе за счет влияния на ЦС и НКБ

Destruction of bonds between soil particles in the process of water erosion

It is known that tensile strength of soil samples is by three orders of magnitude greater than the shear stresses on the bottom of slope streams responsible for the detachment and transport of soil particles by water current. C.E. Mirtskhulava believed that detachment of soil particles by water current occurs due to the fatigue destruction of bonds between soil particles.Taking this fact into account, tensile strength is lower by two orders of magnitude. M.A. Nearing had an opinion that detachment of soil particles occurs in the points of separation of vortices from the bottom of the stream, where the shear stress is by two orders of magnitude higher than the average. These approaches did not explain overcoming by slope streams of the cohesion forces between soil particles. Studies of the influence of water temperature on the washout rate of model samples have shown that the soil erosion is highly dependent on the water temperature, which is close to the Van’t Hoff’s rule. This means that destruction of bonds between soil particles is probably the result of interaction between the soil solid phase and water molecules. Experiments have also shown that destruction of bonds between soil particles in the sample of chernozem monoaggregate soil occurs under a layer of still water. Upon the start of the water flow, particles that lost bond with the rest of the soil body immediately break away. The number of particles with disrupted bonds grows with the duration of the sample exposure to still water, although with some flattening. Experiments confirm the validity of the hypothesis of non-hydraulic nature of forces that disrupt inter-aggregate bonds during water erosion

Azidothymidine "clicked" into 1,2,3-Triazoles: First Report on Carbonic Anhydrase-Telomerase Dual-Hybrid Inhibitors

Cancer cells rely on the enzyme telomerase (EC 2.7.7.49) to promote cellular immortality. Telomerase inhibitors (i.e., azidothymidine) can represent promising antitumor agents, although showing high toxicity when administered alone. Better outcomes were observed within a multipharmacological approach instead. In this context, we exploited the validated antitumor targets carbonic anhydrases (CAs; EC 4.2.1.1) IX and XII to attain the first proof of concept on CA-telomerase dual-hybrid inhibitors. Compounds 1b, 7b, 8b, and 11b showed good in vitro inhibition potency against the CAs IX and XII, with KI values in the low nanomolar range, and strong antitelomerase activity in PC-3 and HT-29 cells (IC50 values ranging from 5.2 to 9.1 μM). High-resolution X-ray crystallography on selected derivatives in the adduct with hCA II as a model study allowed to determine their binding modes and thus to set the structural determinants necessary for further development of compounds selectively targeting the tumoral cells

Azidothymidine "clicked" into 1,2,3-Triazoles: First Report on Carbonic Anhydrase-Telomerase Dual-Hybrid Inhibitors

Cancer cells rely on the enzyme telomerase (EC 2.7.7.49) to promote cellular immortality. Telomerase inhibitors (i.e., azidothymidine) can represent promising antitumor agents, although showing high toxicity when administered alone. Better outcomes were observed within a multipharmacological approach instead. In this context, we exploited the validated antitumor targets carbonic anhydrases (CAs; EC 4.2.1.1) IX and XII to attain the first proof of concept on CA-telomerase dual-hybrid inhibitors. Compounds 1b, 7b, 8b, and 11b showed good in vitro inhibition potency against the CAs IX and XII, with KI values in the low nanomolar range, and strong antitelomerase activity in PC-3 and HT-29 cells (IC50 values ranging from 5.2 to 9.1 μM). High-resolution X-ray crystallography on selected derivatives in the adduct with hCA II as a model study allowed to determine their binding modes and thus to set the structural determinants necessary for further development of compounds selectively targeting the tumoral cells. Copyright © 2020 American Chemical Society