Your search keyword '"kallikrein"' showing total 8,705 results

1. Prolonging the circulatory half-life of C1 esterase inhibitor via albumin fusion.

Author

Sivananthan, Sangavi, Bhakta, Varsha, Chaechi Tehrani, Negin, and Sheffield, William P.

Subjects

*SERUM albumin, *PICHIA pastoris, *INTRAVENOUS injections, *ALBUMINS, *KALLIKREIN

Abstract

Hereditary Angioedema (HAE) is an autosomal dominant disease characterized by episodic swelling, arising from genetic deficiency in C1-esterase inhibitor (C1INH), a regulator of several proteases including activated Plasma kallikrein (Pka). Many existing C1INH treatments exhibit short circulatory half-lives, precluding prophylactic use. Hexahistidine-tagged truncated C1INH (trC1INH lacking residues 1–97) with Mutated N-linked Glycosylation Sites N216Q/N231Q/N330Q (H6-trC1INH(MGS)), its murine serum albumin (MSA) fusion variant (H6-trC1INH(MGS)-MSA), and H6-MSA were expressed in Pichia pastoris and purified via nickel-chelate chromatography. Following intravenous injection in mice, the mean terminal half-life of H6-trC1INH(MGS)-MSA was significantly increased versus that of H6-trC1INH(MGS), by 3-fold, while remaining ~35% less than that of H6-MSA. The extended half-life was achieved with minimal, but significant, reduction in the mean second order rate constant of Pka inhibition of H6-trC1INH(MGS)-MSA by 33% relative to that of H6-trC1INH(MGS). Our results validate albumin fusion as a viable strategy for half-life extension of a natural inhibitor and suggest that H6-trC1INH(MGS)-MSA is worthy of investigation in a murine model of HAE. [ABSTRACT FROM AUTHOR]

Published

2024

2. Berotralstat for hereditary angioedema with C1 inhibitor deficiency: a practical guide for clinicians.

Author

Adatia, Adil and Magerl, Markus

Subjects

ORAL medication, CLINICAL trials, CONGENITAL disorders, NOCEBOS, LIVER enzymes, APIXABAN, DABIGATRAN

Abstract

The article "Berotralstat for hereditary angioedema with C1 inhibitor deficiency: a practical guide for clinicians" discusses the use of berotralstat as a treatment option for hereditary angioedema due to C1 inhibitor deficiency. Berotralstat is an oral medication that inhibits plasma kallikrein and has been shown to reduce swelling attacks in patients. The article provides information on the drug's pharmacology, clinical efficacy, side effects, drug interactions, and guidance on transitioning patients to berotralstat from other long-term prophylaxis treatments. It emphasizes the importance of individualized care and monitoring for optimal patient outcomes. [Extracted from the article]

Published

2024

3. Plasma Kallikrein as a Forgotten Clotting Factor.

Author

Kearney, Katherine J., Spronk, Henri M.H., Emsley, Jonas, Key, Nigel S., and Philippou, Helen

Subjects

*BLOOD coagulation factor IX, *BLOOD coagulation, *BLOOD coagulation factors, *KALLIKREIN, *COAGULATION

Abstract

For decades, it was considered that plasma kallikrein's (PKa) sole function within the coagulation cascade is the activation of factor (F)XII. Until recently, the two key known activators of FIX within the coagulation cascade were activated FXI(a) and the tissue factor–FVII(a) complex. Simultaneously, and using independent experimental approaches, three groups identified a new branch of the coagulation cascade, whereby PKa can directly activate FIX. These key studies identified that (1) FIX or FIXa can bind with high affinity to either prekallikrein (PK) or PKa; (2) in human plasma, PKa can dose dependently trigger thrombin generation and clot formation independent of FXI; (3) in FXI knockout murine models treated with intrinsic pathway agonists, PKa activity results in increased formation of FIXa:AT complexes, indicating direct activation of FIX by PKa in vivo. These findings suggest that there is both a canonical (FXIa-dependent) and non-canonical (PKa-dependent) pathway of FIX activation. These three recent studies are described within this review, alongside historical data that hinted at the existence of this novel role of PKa as a coagulation clotting factor. The implications of direct PKa cleavage of FIX remain to be determined physiologically, pathophysiologically, and in the context of next-generation anticoagulants in development. [ABSTRACT FROM AUTHOR]

Published

2024

4. Reducing Brain Edema Using Berotralstat, an Inhibitor of Bradykinin, Repurposed as Treatment Adjunct in Glioblastoma.

Author

Kast, Richard E.

Subjects

*DRUG approval, *CEREBRAL edema, *BRADYKININ, *GLIOBLASTOMA multiforme, *KALLIKREIN

Abstract

Glioblastomas synthesize, bear receptors for, and respond to bradykinin, triggering migration and proliferation. Since centrifugal migration into uninvolved surrounding brain tissue occurs early in the course of glioblastoma, this attribute defeats local treatment attempts and is the primary reason current treatments almost always fail. Stopping bradykinin-triggered migration would be a step closer to control of this disease. The recent approval and marketing of an oral plasma kallikrein inhibitor, berotralstat (Orladeyo™), and pending FDA approval of a similar drug, sebetralstat, now offers a potential method for reducing local bradykinin production at sites of bradykinin-mediated glioblastoma migration. Both drugs are approved for treating hereditary angioedema. They are ideal for repurposing as a treatment adjunct in glioblastoma. Furthermore, it has been established that peritumoral edema, a common problem during the clinical course of glioblastoma, is generated in large part by locally produced bradykinin via kallikrein action. Both brain edema and the consequent use of corticosteroids both shorten survival in glioblastoma. Therefore, by (i) migration inhibition, (ii) growth inhibition, (iii) edema reduction, and (iv) the potential for less use of corticosteroids, berotralstat may be of service in treatment of glioblastoma, slowing disease progression. This paper recounts the details and past research on bradykinin in glioblastoma and the rationale of treating it with berotralstat. [ABSTRACT FROM AUTHOR]

Published

2024

5. The Contrasting Effects of Bothrops lanceolatus and Bothrops atrox Venom on Procoagulant Activity and Thrombus Stability under Blood Flow Conditions.

Author

Radouani, Fatima, Jalta, Prisca, Rapon, Caroline, Lezin, Chloe, Branford, Chelsea, Florentin, Jonathan, Gutierrez, Jose Maria, Resiere, Dabor, Neviere, Remi, and Pierre-Louis, Olivier

Subjects

*FER-de-lance, *DISSEMINATED intravascular coagulation, *BLOOD coagulation factors, *BLOOD coagulation, *SHEARING force, *FIBRIN

Abstract

Background: Consumption coagulopathy and hemorrhagic syndrome are the typical features of Bothrops sp. snake envenoming. In contrast, B. lanceolatus envenoming can induce thrombotic complications. Our aim was to test whether crude B. lanceolatus and B. atrox venoms would display procoagulant activity and induce thrombus formation under flow conditions. Methods and Principal Findings: Fibrin formation in human plasma was observed for B. lanceolatus venom at 250–1000 ng/mL concentrations, which also induced clot formation in purified human fibrinogen, indicating thrombin-like activity. The degradation of fibrinogen confirmed the fibrinogenolytic activity of B. lanceolatus venom. B. lanceolatus venom displayed consistent thrombin-like and kallikrein-like activity increases in plasma conditions. The well-known procoagulant B. atrox venom activated plasmatic coagulation factors in vitro and induced firm thrombus formation under high shear rate conditions. In contrast, B. lanceolatus venom induced the formation of fragile thrombi that could not resist shear stress. Conclusions: Our results suggest that crude B. lanceolatus venom displays amidolytic activity and can activate the coagulation cascade, leading to prothrombin activation. B. lanceolatus venom induces the formation of an unstable thrombus under flow conditions, which can be prevented by the specific monovalent antivenom Bothrofav®. [ABSTRACT FROM AUTHOR]

Published

2024

6. Extension of the circulatory half-life of recombinant ecallantide via albumin fusion without loss of anti-kallikrein activity.

Author

Al-Adimi, Ghofran, Bhakta, Varsha, Eltringham-Smith, Louise J., Shirobokov, Valerie, and Sheffield, William P.

Subjects

*CHIMERIC proteins, *ALBUMINS, *SERUM albumin, *PICHIA pastoris, *KALLIKREIN, *BLOOD coagulation factor VIII

Abstract

Ecallantide comprises Kunitz Domain 1 of Tissue Factor Pathway Inhibitor, mutated at seven amino acid positions to inhibit plasma kallikrein (PK). It is used to treat acute hereditary angioedema (HAE). We appended hexahistidine tags to the N- or C-terminus of recombinant Ecallantide (rEcall) and expressed and purified the resulting proteins, with or without fusion to human serum albumin (HSA), using Pichia pastoris. The inhibitory constant (K i) of rEcall-H6 or H6-rEcall for PK was not increased by albumin fusion. When 125I-labelled rEcall proteins were injected intravenously into mice, the area under the clearance curve (AUC) was significantly increased, 3.4- and 3.6-fold, for fusion proteins H6-rEcall-HSA and HSA-rEcall-H6 versus their unfused counterparts but remained 2- to 3-fold less than that of HSA-H6. The terminal half-life of H6-rEcall-HSA and HSA-H6 did not differ, although that of HSA-rEcall-H6 was significantly shorter than either other protein. Receptor Associated Protein (RAP), a Low-density lipoprotein Receptor-related Protein (LRP1) antagonist, competed H6-rEcall-HSA clearance more effectively than intravenous immunoglobulin (IVIg), a neonatal Fc receptor (FcRn) antagonist. HSA fusion decreases rEcall clearance in vivo, but LRP1-mediated clearance remains more important than FcRn-mediated recycling for rEcall fusion proteins. The properties of H6-rEcall-HSA warrant investigation in a murine model of HAE. • Ecallantide is a small protein engineered to inhibit plasma kallikrein. • Overactive kallikrein production leads to Hereditary Angioedema (HAE). • Ecallantide does not stay in circulation long enough for prophylactic use. • Ecallantide-albumin fusion proteins circulate longer than ecallantide. • Ecallantide-albumin fusion protein clearance involves a scavenger receptor. [ABSTRACT FROM AUTHOR]

Published

2024

7. Investigation of a Serine Protease Inhibitor Active in the Infectious Stage of the Human Liver Fluke Opisthorchis viverrini.

Author

Salang, Rosnanee, Phadungsil, Wansika, Geadkaew-Krenc, Amornrat, and Grams, Rudi

Subjects

OPISTHORCHIS viverrini, SERINE proteinases, LIVER flukes, REVERSE transcriptase, PROTEASE inhibitors

Abstract

Serine protease inhibitors (serpins) participate in the regulation of inflammation, blood coagulation, and complement activation in humans. This research aimed to identify and characterize such inhibitors of the human liver fluke Opisthorchis viverrini. Parasite proteins that might contribute to the modulation of host physiology are of particular interest, especially as chronic opisthorchiasis increases the risk of developing biliary cancer. BLAST was used to find hypothetical serpins predicted from the parasite genome data. RNA extraction and reverse transcriptase PCR were used to isolate a serpin cDNA and to determine developmental transcript abundance. The evolutionary relation to other trematode serpins was revealed by phylogenetic analysis. Recombinant serpin was expressed in Escherichia coli and used to test the immunoreactivity of human opisthorchiasis sera and the inhibition of human serine proteases. A substantial serpin family with high sequence divergence among the members was found in the genus Opisthorchis. A serpin, different from previously analyzed trematode serpins, was cloned. The transcript was only detected in metacercariae and newly excysted juveniles. Human opisthorchiasis sera showed statistically significant reactivity to recombinant serpin. The serpin caused moderate inhibition of thrombin and low inhibition of kallikrein and chymotrypsin. This parasite serpin could be further evaluated as a diagnostic tool for early infection. Kallikrein and thrombin are involved in fibrinolysis; therefore, further research should explore the effects of the parasite serpin on this process. [ABSTRACT FROM AUTHOR]

Published

2024

8. Centralized care model for hereditary angioedema overcomes geographical barriers.

Author

Holmes, Ashley, Srinivasan, Cindy, Borle, Jack, Blain, Heather, Ritchie, Bruce, and Adatia, Adil

Subjects

RURAL medicine, POISSON regression, ANGIONEUROTIC edema, ODDS ratio, LOGISTIC regression analysis

Abstract

Hereditary angioedema due to C1 inhibitor deficiency (HAE) is a rare inborn error of immunity that presents with episodic swelling. Management is multifaceted and includes on-demand treatment of swelling episodes, short-term prophylaxis to prevent swelling episodes from procedures, and long-term prophylaxis (LTP) to prevent angioedema on an ongoing basis. All approved on-demand therapies are parenteral, necessitating patient training for home administration, particularly intravenous C1 inhibitor. These complexities can result in care gaps for rural HAE patients. We conducted a cross-sectional study at our Angioedema Center of Reference and Excellence to assess the care provided to urban and rural patients. The proportion of patients receiving LTP, proportion of patients diagnosed as children, and disease control measured using the Angioedema Control Test (AECT) were collected. Logistic and Poisson regression models adjusted for age and sex were used to compare the two groups. The proportion using LTP was similar at 62% and 61% in urban and rural patients, respectively (odds ratio [OR] 1.01 (CI 95% 0.34-2.99)). Among urban patients, 52% were diagnosed as children compared to 60% among rural residents (1.43 (0.37-5.56)). The mean (IQR) AECT score was 14.0 (8.5-15.5) in urban patients and 13.0 (10.0-14.0) in rural patients (Poisson β -0.001 (-0.23-0.23). These data indicate that rural patients received similar high-quality care. We attribute these findings to the centralized care model employed in which HAE patients in the region are seen at a single comprehensive care clinic. [ABSTRACT FROM AUTHOR]

Published

2024

9. Single-cell transcriptome profiling highlights the importance of telocyte, kallikrein genes, and alternative splicing in mouse testes aging.

Author

Guo, Wuyier, Zhang, Ziyan, Kang, Jiahui, Gao, Yajing, Qian, Peipei, and Xie, Gangcai

Subjects

*ALTERNATIVE RNA splicing, *KALLIKREIN, *TESTIS, *LEYDIG cells, *GERM cells, *SPERMATOGENESIS, *RNA splicing

Abstract

Advancing healthcare for elderly men requires a deeper understanding of testicular aging processes. In this study, we conducted transcriptomic profiling of 43,323 testicular single cells from young and old mice, shedding light on 1032 telocytes—an underexplored testicular cell type in previous research. Our study unveiled 916 age-related differentially expressed genes (age-DEGs), with telocytes emerging as the cell type harboring the highest count of age-DEGs. Of particular interest, four genes (Klk1b21, Klk1b22, Klk1b24, Klk1b27) from the Kallikrein family, specifically expressed in Leydig cells, displayed down-regulation in aged testes. Moreover, cell-type-level splicing analyses unveiled 1838 age-related alternative splicing (AS) events. While we confirmed the presence of more age-DEGs in somatic cells compared to germ cells, unexpectedly, more age-related AS events were identified in germ cells. Further experimental validation highlighted 4930555F03Rik, a non-coding RNA gene exhibiting significant age-related AS changes. Our study represents the first age-related single-cell transcriptomic investigation of testicular telocytes and Kallikrein genes in Leydig cells, as well as the first delineation of cell-type-level AS dynamics during testicular aging in mice. [ABSTRACT FROM AUTHOR]

Published

2024

10. Delayed plasma kallikrein inhibition fosters post-stroke recovery by reducing thrombo-inflammation.

Author

Haupeltshofer, Steffen, Mencl, Stine, Szepanowski, Rebecca D., Hansmann, Christina, Casas, Ana I., Abberger, Hanna, Hansen, Wiebke, Blusch, Alina, Deuschl, Cornelius, Forsting, Michael, Hermann, Dirk M., Langhauser, Friederike, and Kleinschnitz, Christoph

Subjects

*KALLIKREIN, *BLOOD-brain barrier, *ISCHEMIC stroke, *CEREBRAL ischemia, *CARDIOVASCULAR system

Abstract

Activation of the kallikrein-kinin system promotes vascular leakage, inflammation, and neurodegeneration in ischemic stroke. Inhibition of plasma kallikrein (PK) – a key component of the KKS – in the acute phase of ischemic stroke has been reported to reduce thrombosis, inflammation, and damage to the blood-brain barrier. However, the role of PK during the recovery phase after cerebral ischemia is unknown. To this end, we evaluated the effect of subacute PK inhibition starting from day 3 on the recovery process after transient middle artery occlusion (tMCAO). Our study demonstrated a protective effect of PK inhibition by reducing infarct volume and improving functional outcome at day 7 after tMCAO. In addition, we observed reduced thrombus formation in cerebral microvessels, fewer infiltrated immune cells, and an improvement in blood-brain barrier integrity. This protective effect was facilitated by promoting tight junction reintegration, reducing detrimental matrix metalloproteinases, and upregulating regenerative angiogenic markers. Our findings suggest that PK inhibition in the subacute phase might be a promising approach to accelerate the post-stroke recovery process. [ABSTRACT FROM AUTHOR]

Published

2024

11. Sebetralstat: A Rapidly Acting Oral Plasma Kallikrein Inhibitor for the On-Demand Treatment of Hereditary Angioedema.

Author

Feener, Edward P., Davie, Rebecca L., Murugesan, Nivetha, Pethen, Stephen J., Hampton, Sally L., Smith, Michael D., Audhya, Paul K., and Yea, Chris M.

Subjects

*KALLIKREIN, *ANGIONEUROTIC edema, *ORAL drug administration, *CLINICAL trials, *SERINE proteinases, *URTICARIA

Abstract

Sebetralstat is a novel, potent, and selective oral plasma kallikrein inhibitor drug candidate in clinical development for the on-demand treatment of hereditary angioedema (HAE). Upon binding, sebetralstat induces a conformational change in the active site of plasma kallikrein, which contributes to its high potency (Ki 3 nM) and selectivity (>1500 fold) against other serine proteases. Its physiochemical properties promote both rapid dissolution in the stomach and rapid absorption in the upper intestine that contribute to its fast and efficient absorption. A single oral administration of sebetralstat rapidly provides near-complete inhibition of plasma kallikrein and blockade of high-molecular-weight kininogen cleavage as early as 15 min, which drives its clinical efficacy. In a phase 2 clinical trial, sebetralstat significantly reduced the time to beginning of symptom relief (p < 0.0001) with median times of 1.6 h (95% CI: 1.5–3.0) with sebetralstat versus 9.0 h (4.0–17.2) with placebo. KONFIDENT (NCT05259917) is a phase 3 clinical trial assessing the on-demand use of sebetralstat for HAE. If successful, this trial could support the approval of sebetralstat as the first noninvasive, on-demand treatment option to rapidly halt HAE attacks and provide fast symptom relief. [ABSTRACT FROM AUTHOR]

Published

2024

12. Exploring Periodontal Conditions, Salivary Markers, and Systemic Inflammation in Patients with Cardiovascular Diseases.

Author

Caloian, Carmen Silvia, Șurlin, Petra, Ciurea, Andreea, Pop, Dana, Caloian, Bogdan, Leucuța, Daniel Corneliu, Țigu, Adrian Bogdan, Rasperini, Giulio, Micu, Iulia Cristina, Stanomir, Alina, Soancă, Andrada, and Roman, Alexandra

Subjects

CARDIOVASCULAR diseases, PERIODONTITIS, ARRHYTHMIA, INFLAMMATION, BLOOD proteins, KALLIKREIN, C-reactive protein

Abstract

(1) Background: This cross-sectional investigation appreciated the role of serum C-reactive protein (CRP), several hematologic-cell markers, and salivary inflammation-related molecules [calprotectin (S100A8/A9), interleukin-1β (IL-1β), kallikrein] to predict periodontitis in patients with atherosclerotic cardiovascular disease (ACVD), arrhythmia, or both. Also, we appreciated the relationship between the inflammatory burden and periodontal destruction with the type of cardiac pathology. (2) Methods: Demographic, behavioral characteristics, periodontal indicators, blood parameters, and saliva samples were collected. (3) Results: All 148 patients exhibited stage II or III/IV periodontitis. Stage III/IV cases exhibited significantly increased S100A8/A9 levels (p = 0.004). A positive correlation between S100A8/A9 and IL-1β [0.35 (<0.001)], kallikrein [0.55 (<0.001)], and CRP [0.28 (<0.001)] was observed. Patients with complex cardiac involvement had a significantly higher number of sites with attachment loss ≥ 5 mm [19 (3–30)] compared to individuals with only arrhythmia [9 (3.25–18)] or ACVD [5 (1–12)] [0.048♦ {0.162/0.496/0.14}]. (4) Conclusions: Severe, extensive attachment loss may be indicative of patients with complex cardiac conditions, which underscores the essential role of periodontal status in relation to systemic diseases. The correlations between the rising trends of the inflammatory parameters suggest a potential interconnection between oral and systemic inflammation. [ABSTRACT FROM AUTHOR]

Published

2024

13. Berotralstat for hereditary angioedema with C1 inhibitor deficiency: a practical guide for clinicians

Author

Adil Adatia and Markus Magerl

Subjects

hereditary angioedema, C1 inhibitor, kallikrein, berotralstat, immunodeficiency, Immunologic diseases. Allergy, RC581-607

Published

2024

14. BioCryst begins enrollment for Phase 1 trial evaluating BCX17725

Subjects

BioCryst Pharmaceuticals Inc. -- Product development, Kallikrein, Pharmaceutical industry -- Product development, Business, News, opinion and commentary

Abstract

BioCryst Pharmaceuticals announced the enrollment of the first participant in a Phase 1 trial evaluating BCX17725, a potent and selective investigational kallikrein 5, or KLK5, inhibitor designed to provide best-in-class [...]

Published

2024

15. Kinin-kallikrein system: New perspectives in heart failure.

Author

Mohammadi, Keivan, Shafie, Davood, Ghomashi, Newsha, Abdolizadeh, Ali, and Sadeghpour, Majid

Subjects

HEART failure, PEPTIDES, RENIN-angiotensin system, BLOOD pressure, KININS, KALLIKREIN, ALDOSTERONE antagonists

Abstract

Heart failure (HF) is a pervasive clinical challenge characterized by compromised cardiac function and reduced quality of life. The kinin-kallikrein system (KSS), a multifaceted peptide cascade, has garnered substantial attention due to its potential role in HF. Through activation of B1 and/or B2 receptors and downstream signaling, kinins modulate various physiological processes, including inflammation, coagulation, pain, blood pressure control, and vascular permeability. Notably, aberrations in KKS components have been linked to HF risk. The elevation of vasodilatory bradykinin (BK) due to kallikrein activity reduces preload and afterload, while concurrently fostering sodium reabsorption inhibition. However, kallikrein's conversion of prorenin to renin leads to angiotensinsII upregulation, resulting in vasoconstriction and fluid retention, alongside increased immune cell activity that fuels inflammation and cardiac remodeling. Importantly, prolonged KKS activation resulting from volume overload and tissue stretch contributes to cardiac collagen loss. The conventional renin-angiotensin-aldosterone system (RAAS) inhibitors used in HF management may inadvertently intensify KKS activity, exacerbating collagen depletion and cardiac remodeling. It is crucial to balance the KKS's role in acute cardiac damage, which may temporarily enhance function and metabolic parameters against its detrimental long-term effects. Thus, KKS blockade emerges as a promising strategy to impede HF progression. By attenuating the link between immune system function and tissue damage, KKS inhibition can potentially reduce cardiac remodeling and alleviate HF symptoms. However, the nuanced roles of BK in various acute conditions necessitate further investigation into the sustained benefits of kallikrein inhibitors in patients with chronic HF. [ABSTRACT FROM AUTHOR]

Published

2024

16. Centralized care model for hereditary angioedema overcomes geographical barriers

Author

Ashley Holmes, Cindy Srinivasan, Jack Borle, Heather Blain, Bruce Ritchie, and Adil Adatia

Subjects

hereditary angioedema, SERPING1, rural medicine, kallikrein, C1 inhibitor, immunodeficiency, Immunologic diseases. Allergy, RC581-607

Abstract

Hereditary angioedema due to C1 inhibitor deficiency (HAE) is a rare inborn error of immunity that presents with episodic swelling. Management is multifaceted and includes on-demand treatment of swelling episodes, short-term prophylaxis to prevent swelling episodes from procedures, and long-term prophylaxis (LTP) to prevent angioedema on an ongoing basis. All approved on-demand therapies are parenteral, necessitating patient training for home administration, particularly intravenous C1 inhibitor. These complexities can result in care gaps for rural HAE patients. We conducted a cross-sectional study at our Angioedema Center of Reference and Excellence to assess the care provided to urban and rural patients. The proportion of patients receiving LTP, proportion of patients diagnosed as children, and disease control measured using the Angioedema Control Test (AECT) were collected. Logistic and Poisson regression models adjusted for age and sex were used to compare the two groups. The proportion using LTP was similar at 62% and 61% in urban and rural patients, respectively (odds ratio [OR] 1.01 (CI 95% 0.34-2.99)). Among urban patients, 52% were diagnosed as children compared to 60% among rural residents (1.43 (0.37-5.56)). The mean (IQR) AECT score was 14.0 (8.5-15.5) in urban patients and 13.0 (10.0-14.0) in rural patients (Poisson β -0.001 (-0.23-0.23). These data indicate that rural patients received similar high-quality care. We attribute these findings to the centralized care model employed in which HAE patients in the region are seen at a single comprehensive care clinic.

Published

2024

17. An LNP-CRISPR gene editing drug demonstrates efficacy and safety in patients with hereditary angioedema following in vivo administration.

Author

Pardi, Norbert and Ivics, Zoltán

Published

2024

18. New Findings on Blood Coagulation Factors Described by Investigators at Chinese Academy of Sciences (The Plasma Kallikrein-kinin System: a Hematological Target for Environmental Contaminants)

Subjects

Kallikrein, Physical fitness, Health, Chinese Academy of Sciences

Abstract

2024 JUN 8 (NewsRx) -- By a News Reporter-Staff News Editor at Obesity, Fitness & Wellness Week -- Current study results on Hematology - Blood Coagulation Factors have been published. [...]

Published

2024

19. Berotralstat in hereditary angioedema due to C1 inhibitor deficiency: first real-world evidence from a Canadian center.

Author

Srinivasan, Cindy, Ritchie, Bruce, and Adatia, Adil

Subjects

ANGIONEUROTIC edema, PATIENT satisfaction, PATIENT experience, URTICARIA, LIKERT scale, DISEASE management

Abstract

Background: Hereditary angioedema due to C1 inhibitor deficiency is a rare genetic condition that causes recurrent swelling with consequent functional impairment and decreased quality of life. Long-term prophylaxis (LTP) to prevent angioedema episodes is a key component of disease management. Berotralstat, an oral, once-daily plasma kallikrein inhibitor, was approved for LTP by Health Canada in 2022. Methods: We conducted a retrospective, real-world study investigating the effectiveness and adverse effects of berotralstat. Data on angioedema frequency, disease control, and adverse events were tabulated. Patient satisfaction with treatment was scored on a 5-point Likert scale, with 1 representing very unsatisfied and 5 representing very satisfied with therapy. Results: From June, 2022 and May, 2023, 8 patients with HAE type 1 or type 2 received berotralstat. Effectiveness data were available for 7 patients who continued the drug for at least 3 months, 4 of whom switched to berotralstat from plasma-derived C1 inhibitor LTP. In these 7 patients, the average number of attacks per month decreased from 3.3 to 1.6 (p<0.05), representing a ~52% reduction in attack frequency. Median angioedema control test score numerically improved from 8 to 13 (p=0.0781). Of the 8 patients who received berotralstat, 3 reported no adverse effects and 5 experienced gastrointestinal side effects, which were mild and transient in 3 and led to discontinuation in 1. Average treatment satisfaction was between satisfied and very satisfied at 4.3. Conclusion: Berotralstat is an effective agent for long-term prophylaxis in HAE. Most patients experienced no adverse effects or mild, transient gastrointestinal symptoms. [ABSTRACT FROM AUTHOR]

Published

2024

20. Proteolytic Activation of the Epithelial Sodium Channel (ENaC): Its Mechanisms and Implications.

Author

Aufy, Mohammed, Hussein, Ahmed M., Stojanovic, Tamara, Studenik, Christian R., and Kotob, Mohamed H.

Subjects

*SODIUM channels, *REGULATION of blood pressure, *WATER-electrolyte balance (Physiology), *SERINE proteinases, *SODIUM ions, *TISSUES

Abstract

Epithelial sodium channel (ENaC) are integral to maintaining salt and water homeostasis in various biological tissues, including the kidney, lung, and colon. They enable the selective reabsorption of sodium ions, which is a process critical for controlling blood pressure, electrolyte balance, and overall fluid volume. ENaC activity is finely controlled through proteolytic activation, a process wherein specific enzymes, or proteases, cleave ENaC subunits, resulting in channel activation and increased sodium reabsorption. This regulatory mechanism plays a pivotal role in adapting sodium transport to different physiological conditions. In this review article, we provide an in-depth exploration of the role of proteolytic activation in regulating ENaC activity. We elucidate the involvement of various proteases, including furin-like convertases, cysteine, and serine proteases, and detail the precise cleavage sites and regulatory mechanisms underlying ENaC activation by these proteases. We also discuss the physiological implications of proteolytic ENaC activation, focusing on its involvement in blood pressure regulation, pulmonary function, and intestinal sodium absorption. Understanding the mechanisms and consequences of ENaC proteolytic activation provides valuable insights into the pathophysiology of various diseases, including hypertension, pulmonary disorders, and various gastrointestinal conditions. Moreover, we discuss the potential therapeutic avenues that emerge from understanding these mechanisms, offering new possibilities for managing diseases associated with ENaC dysfunction. In summary, this review provides a comprehensive discussion of the intricate interplay between proteases and ENaC, emphasizing the significance of proteolytic activation in maintaining sodium and fluid balance in both health and disease. [ABSTRACT FROM AUTHOR]

Published

2023

21. Association of Kallikrein Related Peptidase 3 (KLK3) gene with dermatophytosis in the UK biobank cohort.

Author

Lehrer, Steven and Rheinstein, Peter H.

Subjects

*RINGWORM, *GENOME-wide association studies, *PROSTATE-specific antigen, *PEPTIDASE, *KALLIKREIN, *LOCUS (Genetics)

Abstract

Background: In a previous genome wide association study (GWAS) of UK Biobank (UKB) data, we identified one susceptibility locus, tubulointerstitial nephritis antigen (TINAG), with genome wide significance for dermatophytosis. We used genotype calls from file UKB22418. These data are derived directly from Affymetrix DNA microarrays but are missing many genotype calls. Using computationally efficient approaches, UKB has entered imputed genotypes into a second dataset, UKB22828, increasing the number of testable variants by over 100‐fold to 96 million variants. Methods: In the current study, we used UKB imputed genotypes in UKB22828 to identify dermatophytosis susceptibility loci. To identify cases of dermatophytosis, we used ICD10 code B35, which covers tinea barbae, tinea capitis, tinea unguium, tinea manuum, tinea pedis, tinea corporis, tinea imbricata, tinea cruris, other dermatophytoses and dermatophytosis, unspecified. We used PLINK, a whole‐genome association analysis toolset, to analyse the UKB22828 chromosome files. Results: GWAS summary (Manhattan) plot of the meta‐analysis association statistics highlighted two susceptibility loci, TINAG and Kallikrein Related Peptidase 3 (KLK3), with genome wide significance for dermatophytosis. KLK3, also known as prostate specific antigen (PSA), belongs to a subclass of serine proteases with a variety of physiological functions. Conclusion: KLK3 may be a dermatophytosis susceptibility gene. KLK3 could affect risk of dermatophytosis, since kallikreins are necessary for normal homeostasis of the skin. [ABSTRACT FROM AUTHOR]

Published

2023

22. Recessive SERPING1 Variant Leads to Kinin–Kallikrein System Control Failure in a Consanguineous Brazilian Family with Hereditary Angioedema.

Author

Maia, Luana Sella Motta, Burger, Bettina, Ghannam, Arije, Nunes, Fernanda Leonel, Ferriani, Mariana Paes Leme, Dias, Marina Mendonça, Arruda, Luisa Karla, Drouet, Christian, and Cichon, Sven

Subjects

*SYSTEM failures, *ANGIONEUROTIC edema, *GENETIC variation, *MISSENSE mutation, *URTICARIA, *KALLIKREIN, *ECULIZUMAB

Abstract

Background: Hereditary angioedema (HAE) is a severe and potentially life-threatening disease. The most common forms are caused by variants in SERPING1, resulting in C1-inhibitor (C1-INH) deficiency (HAE-C1-INH). C1-INH is a serine protease inhibitor (SERPIN) that regulates multiple proteases pathways, including the kallikrein–kinin system (KKS) and its complement. In HAE-C1-INH patients, C1-INH deficiencies affect KKS control, resulting in the development of kallikrein activity in plasma and the subsequent release of bradykinin (BK). While the overwhelming majority of disease-causing SERPING1 variants are dominant, very few recessive variants have been described. We present a large Brazilian HAE-C1-INH family with a recessive form of HAE-C1-INH. Methods: Blood samples of family members were investigated for protein levels of C1-INH, C4, C1q, and C1-INH function. The SERPING1 gene was sequenced. Results: In two severely affected sisters, we identified a homozygous missense variant in SERPING1 (NM_000062.3:c.964G>A;p.Val322Met). Fourteen family members were asymptomatic heterozygous carriers of the variant. Data regarding C1-INH function in the plasma showed that homozygous p.Val322Met strongly impacts C1-INH function to inhibit C1s and kallikrein (PKa). When heterozygously expressed, it affects the C1-INH control of C1s more than that of PKa. Conclusions: These studies of the variant's effects on the structure–function relationship reinforce prior observations suggesting that C1-INH deficiency is a conformational disease. [ABSTRACT FROM AUTHOR]

Published

2023

23. Preanalytical impact on the accuracy of measurements of glucagon, GLP-1 and GIP in clinical trials.

Author

Rasmussen, Christine, Richter, Michael M., Jensen, Nicole J., Heinz, Niklas, Hartmann, Bolette, Holst, Jens J., Kjeldsen, Sasha A. S., and Wewer Albrechtsen, Nicolai J.

Subjects

*GLUCAGON, *CLINICAL trials, *INTRAVENOUS therapy, *KALLIKREIN, *PROTEASE inhibitors

Abstract

Plasma concentrations of glucagon, GLP-1 and GIP are reported in numerous clinical trials as outcome measures but preanalytical guidelines are lacking. We addressed the impact of commonly used blood containers in metabolic research on measurements of glucagon, GLP-1 and GIP in humans. Seventeen overweight individuals were subjected to an overnight fast followed by an intravenous infusion of amino acids to stimulate hormonal secretion. Blood was sampled into five containers: EDTA-coated tubes supplemented with DMSO (control), a neprilysin inhibitor, aprotinin (a kallikrein inhibitor) or a DPP-4 inhibitor, and P800 tubes. Plasma was kept on ice before and after centrifugation and stored at −80 Celsius until batch analysis using validated sandwich ELISAs or radioimmunoassays (RIA). Measures of fasting plasma glucagon did not depend on sampling containers, whether measured by ELISA or RIA. Amino acid-induced hyperglucagonemia was numerically higher when blood was collected into P800 tubes or tubes with aprotinin. The use of p800 tubes resulted in higher concentrations of GLP-1 by RIA compared to control tubes but not for measurements with sandwich ELISA. Plasma concentrations of GIP measured by ELISA were higher in control tubes and negatively affected by P800 and the addition of aprotinin. The choice of blood containers impacts on measurements of plasma concentrations of glucagon, GLP-1 and GIP, and based on this study, we recommend using EDTA-coated tubes without protease inhibitors or P800 tubes for measurements of glucagon, GLP-1 and GIP in clinical trials. [ABSTRACT FROM AUTHOR]

Published

2023

24. Investigation of a Serine Protease Inhibitor Active in the Infectious Stage of the Human Liver Fluke Opisthorchis viverrini

Author

Rosnanee Salang, Wansika Phadungsil, Amornrat Geadkaew-Krenc, and Rudi Grams

Subjects

Opisthorchis viverrini, serine protease inhibitor, serpins, chymotrypsin, kallikrein, thrombin, Medicine

Abstract

Serine protease inhibitors (serpins) participate in the regulation of inflammation, blood coagulation, and complement activation in humans. This research aimed to identify and characterize such inhibitors of the human liver fluke Opisthorchis viverrini. Parasite proteins that might contribute to the modulation of host physiology are of particular interest, especially as chronic opisthorchiasis increases the risk of developing biliary cancer. BLAST was used to find hypothetical serpins predicted from the parasite genome data. RNA extraction and reverse transcriptase PCR were used to isolate a serpin cDNA and to determine developmental transcript abundance. The evolutionary relation to other trematode serpins was revealed by phylogenetic analysis. Recombinant serpin was expressed in Escherichia coli and used to test the immunoreactivity of human opisthorchiasis sera and the inhibition of human serine proteases. A substantial serpin family with high sequence divergence among the members was found in the genus Opisthorchis. A serpin, different from previously analyzed trematode serpins, was cloned. The transcript was only detected in metacercariae and newly excysted juveniles. Human opisthorchiasis sera showed statistically significant reactivity to recombinant serpin. The serpin caused moderate inhibition of thrombin and low inhibition of kallikrein and chymotrypsin. This parasite serpin could be further evaluated as a diagnostic tool for early infection. Kallikrein and thrombin are involved in fibrinolysis; therefore, further research should explore the effects of the parasite serpin on this process.

Published

2024

25. Exploring Periodontal Conditions, Salivary Markers, and Systemic Inflammation in Patients with Cardiovascular Diseases

Author

Carmen Silvia Caloian, Petra Șurlin, Andreea Ciurea, Dana Pop, Bogdan Caloian, Daniel Corneliu Leucuța, Adrian Bogdan Țigu, Giulio Rasperini, Iulia Cristina Micu, Alina Stanomir, Andrada Soancă, and Alexandra Roman

Subjects

periodontitis, atherosclerotic cardiovascular disease, atherosclerosis, atrial fibrillation, S100A8/A9, kallikrein, Biology (General), QH301-705.5

Abstract

(1) Background: This cross-sectional investigation appreciated the role of serum C-reactive protein (CRP), several hematologic-cell markers, and salivary inflammation-related molecules [calprotectin (S100A8/A9), interleukin-1β (IL-1β), kallikrein] to predict periodontitis in patients with atherosclerotic cardiovascular disease (ACVD), arrhythmia, or both. Also, we appreciated the relationship between the inflammatory burden and periodontal destruction with the type of cardiac pathology. (2) Methods: Demographic, behavioral characteristics, periodontal indicators, blood parameters, and saliva samples were collected. (3) Results: All 148 patients exhibited stage II or III/IV periodontitis. Stage III/IV cases exhibited significantly increased S100A8/A9 levels (p = 0.004). A positive correlation between S100A8/A9 and IL-1β [0.35 (

Published

2024

26. Vasoactive Factors and Blood Pressure in Children

Author

Yosypiv, Ihor V., Ingelfinger, Julie R., Section editor, Flynn, Joseph T., editor, Ingelfinger, Julie R., editor, and Brady, Tammy M., editor

Published

2023

27. Efficacy and Safety of Garadacimab in Combination with Standard of Care Treatment in Patients with Severe COVID-19

Author

Papi, Alberto, Stapleton, Renee D., Shore, Paul M., Bica, Mihai Alexandru, Chen, Younan, Larbig, Michael, and Welte, Tobias

Subjects

United States. National Institute of Allergy and Infectious Diseases -- Standards, Blood -- Medical examination, Medical research, Medicine, Experimental, Mortality, Anticoagulants (Medicine) -- Complications and side effects, Immunoglobulin G, Monoclonal antibodies -- Complications and side effects, Kallikrein, Health

Abstract

Background Garadacimab, a fully human IgG4 monoclonal antibody, inhibits the kallikrein-kinin pathway at a key initiator, activated coagulation factor XII (FXIIa), and may play a protective role in preventing the progression of COVID-19. This phase 2 study evaluated the efficacy and safety of garadacimab plus standard of care (SOC) versus placebo plus SOC in patients with severe COVID-19. Methods Patients hospitalised with COVID-19 were randomised (1:1) to a single intravenous dose of garadacimab (700 mg) plus SOC or placebo plus SOC. Co-primary endpoint was incidence of endotracheal intubation or death between randomisation and Day 28. All-cause mortality, safety and pharmacokinetic/pharmacodynamic parameters were assessed. Results No difference in incidence of tracheal intubation or death (p = 0.274) or all-cause mortality was observed (p = 0.382). Garadacimab was associated with a lower incidence of treatment-emergent adverse events (60.3% vs 67.8%) and fewer serious adverse events (34 vs 45 events) versus placebo. No garadacimab-related deaths or bleeding events were reported, including in the 45.9% (n = 28/61) of patients who received concomitant heparin. Prolonged activated partial thromboplastin time (aPTT), and increased coagulation factor XII (FXII) levels were observed with garadacimab versus placebo to Day 14, whilst FXIIa-mediated kallikrein activity (FXIIa-mKA) was suppressed to Day 28. Conclusion In patients with severe COVID-19, garadacimab did not confer a clinical benefit over placebo. Transient aPTT prolongation and suppressed FXIIa-mKA showed target engagement of garadacimab that was not associated with bleeding events even with concomitant anticoagulant use. The safety profile of garadacimab was consistent with previous studies in patients with hereditary angioedema. ClinicalTrials. gov Identifier NCT04409509. Date of registration: 28 May, 2020., Author(s): Alberto Papi [sup.1], Renee D. Stapleton [sup.2], Paul M. Shore [sup.3], Mihai Alexandru Bica [sup.4], Younan Chen [sup.5], Michael Larbig [sup.6], Tobias Welte [sup.7] Author Affiliations: (1) grid.8484.0, 0000 [...]

Published

2023

28. Berotralstat in hereditary angioedema due to C1 inhibitor deficiency: first real-world evidence from a Canadian center

Author

Cindy Srinivasan, Bruce Ritchie, and Adil Adatia

Subjects

hereditary angioedema, berotralstat, kallikrein, C1 inhibitor, immunodeficiency, Immunologic diseases. Allergy, RC581-607

Abstract

BackgroundHereditary angioedema due to C1 inhibitor deficiency is a rare genetic condition that causes recurrent swelling with consequent functional impairment and decreased quality of life. Long-term prophylaxis (LTP) to prevent angioedema episodes is a key component of disease management. Berotralstat, an oral, once-daily plasma kallikrein inhibitor, was approved for LTP by Health Canada in 2022.MethodsWe conducted a retrospective, real-world study investigating the effectiveness and adverse effects of berotralstat. Data on angioedema frequency, disease control, and adverse events were tabulated. Patient satisfaction with treatment was scored on a 5-point Likert scale, with 1 representing very unsatisfied and 5 representing very satisfied with therapy.ResultsFrom June, 2022 and May, 2023, 8 patients with HAE type 1 or type 2 received berotralstat. Effectiveness data were available for 7 patients who continued the drug for at least 3 months, 4 of whom switched to berotralstat from plasma-derived C1 inhibitor LTP. In these 7 patients, the average number of attacks per month decreased from 3.3 to 1.6 (p

Published

2024

29. A novel approach to enhance the performance of kallikrein 6 enzyme using Pichia pastoris GS115 as a host.

Author

Mahmoodi, Fatemeh, Bakherad, Hamid, Mogharrab, Navid, and Rabbani, Mohammad

Subjects

*PICHIA pastoris, *KALLIKREIN, *AMINO acid sequence, *ENTEROKINASE, *ENZYMES

Abstract

Background and purpose: Enzyme engineering is the process of raising enzyme efficiency and activity by altering amino acid sequences. Kallikrein 6 (KLK6) enzyme is a secreted serine protease involved in a variety of physiological and pathological activities. The increased expression of KLK6 plays a key role in various diseases. Instability and spontaneous activation and deactivation are major challenges in the study of this enzyme. This study aimed to create a stable pro-KLK6 enzyme by enzyme engineering, designing a specific cleavage site for enterokinase, and using Pichia pastoris GS115 as a host cell. Then, recombinant pro-KLK6 was used to introduce a novel inhibitor for it. Experimental approach: An engineered pro-KLK6 gene was cloned into the pPICZα A expression vector. Then, it was expressed in P. pastoris GS115 and purified by Ni-NTA chromatography. An inactive engineered pro-KLK6 gene was cleaved by enterokinase and converted to an active KLK6. The KLK6 enzyme activity and its kinetic parameters were measured using N-benzoyl-L-arginine ethyl ester (BAEE) substrates. Findings/Results: The secretory form of the pro-KLK6 was expressed at about 11 mg/L in P. pastoris (GS115). Before activation with enterokinase, pro-KLK6 was inactive and did not activate spontaneously. The kinetic parameters, including Km and Vmax, were estimated at 113.59 µM and 0.432 µM/s, respectively. Conclusion and implications: A stable pro-KLK6 enzyme was produced using P. pastoris (GS115) as the host cell and a specific cleavage site for enterokinase. Additionally, this study assessed the kinetic parameters of the KLK6 enzyme using the BAEE substrate for the first time. [ABSTRACT FROM AUTHOR]

Published

2023

30. Bioinformatics analysis of human kallikrein 5 (KLK5) expression in metaplastic triple‐negative breast cancer.

Author

Song, Yue, Bai, Guiying, Li, Xiaoqing, Zhou, Liyan, Si, Yiran, Liu, Xiaohui, Deng, Yilin, and Shi, Yehui

Subjects

*TRIPLE-negative breast cancer, *GENE expression, *KALLIKREIN, *EPITHELIAL-mesenchymal transition, *BREAST cancer

Abstract

Background: Metaplastic breast carcinoma (MBC) is a rare breast cancer subtype; most cases are triple‐negative breast cancers (TNBCs) and are poorly responsive to conventional systemic therapy. Few potential diagnostic and prognostic markers for distinguishing between metaplastic TNBC and nonmetaplastic TNBC have been discovered. We performed bioinformatic analysis to explore the underlying mechanism by which metaplastic TNBC differs from nonmetaplastic TNBC and provides potential pathogenic genes of metaplastic TNBC. Methods: Differentially expressed genes (DEGs) in metaplastic tumors and nonmetaplastic tumors from TNBC patients were screened using GSE165407. The GSE76275 data set and The Cancer Genome Atlas (TCGA) database were used to screen DEGs in TNBC and non‐TNBC. Metascape and DAVID were used for the Kyoto Encyclopedia of Genes and Genomes (KEGG) enrichment analysis and Gene Ontology (GO) analysis of DEGs. Online databases, including UALCAN, GEPIA, HPA, Breast Cancer Gene‐Expression Miner, and quantitative PCR and western blot, were used to examine KLK5 messenger RNA and protein expression in breast cancer. Analysis of KLK5‑associated genes was performed with TCGA data, and the LinkedOmics database was used to detect the genes co‐expressed with KLK5. STRING (Search Tool for the Retrieval of Interacting Genes) and Cytoscape were used to screen for hub genes. Kaplan‑Meier plotter was used for survival analysis. Results: KLK5 was identified among the DEGs in nonmetaplastic TNBC and metaplastic TNBC. The KLK5 gene was overexpressed in nonmetaplastic TNBC but downregulated in metaplastic TNBC. KEGG and GO analyses revealed that epithelial‐to‐mesenchymal transition was a pathogenic mechanism in metaplastic TNBC and an important pathway by which KLK5 and its associated genes DSG1 and DSG3 influence metaplastic TNBC progression. Prognosis analysis showed that only low expression of KLK5 in metaplastic TNBC had clinical significance. Conclusion: Our research indicated that KLK5 may be a pivotal molecule with a key role in the mechanism of tumorigenesis in metaplastic TNBC. [ABSTRACT FROM AUTHOR]

Published

2023

31. Human plasma kallikrein: roles in coagulation, fibrinolysis, inflammation pathways, and beyond.

Author

Motta, Guacyara, Juliano, Luiz, and Ribeiro Chagas, Jair

Subjects

KALLIKREIN, MEMBRANE proteins, SERINE proteinases, FIBRINOLYSIS, BLOOD proteins

Abstract

Human plasma kallikrein (PKa) is obtained by activating its precursor, prekallikrein (PK), historically named the Fletcher factor. Human PKa and tissue kallikreins are serine proteases from the same family, having high- and low-molecular weight kininogens (HKs and LKs) as substrates, releasing bradykinin (Bk) and Lys-bradykinin (Lys-Bk), respectively. This review presents a brief history of human PKa with details and recent observations of its evolution among the vertebrate coagulation proteins, including the relations with Factor XI. We explored the role of Factor XII in activating the plasma kallikrein-kinin system (KKS), the mechanism of activity and control in the KKS, and the function of HK on contact activation proteins on cell membranes. The role of human PKa in cell biology regarding the contact system and KSS, particularly the endothelial cells, and neutrophils, in inflammatory processes and infectious diseases, was also approached. We examined the natural plasma protein inhibitors, including a detailed survey of human PKa inhibitors' development and their potential market. [ABSTRACT FROM AUTHOR]

Published

2023

32. Assessing the performance of docking, FEP, and MM/GBSA methods on a series of KLK6 inhibitors.

Author

Lima Silva, Wemenes José and Ferreira de Freitas, Renato

Subjects

*DRUG discovery, *BINDING energy, *DRUG target, *KALLIKREIN, *NEUROLOGICAL disorders

Abstract

Kallikrein 6 (KLK6) is an attractive drug target for the treatment of neurological diseases and for various cancers. Herein, we explore the accuracy and efficiency of different computational methods and protocols to predict the free energy of binding (ΔGbind) for a series of 49 inhibitors of KLK6. We found that the performance of the methods varied strongly with the tested system. For only one of the three KLK6 datasets, the docking scores obtained with rDock were in good agreement (R2 ≥ 0.5) with experimental values of ΔGbind. A similar result was obtained with MM/GBSA (using the ff14SB force field) calculations based on single minimized structures. Improved binding affinity predictions were obtained with the free energy perturbation (FEP) method, with an overall MUE and RMSE of 0.53 and 0.68 kcal/mol, respectively. Furthermore, in a simulation of a real-world drug discovery project, FEP was able to rank the most potent compounds at the top of the list. These results indicate that FEP can be a promising tool for the structure-based optimization of KLK6 inhibitors. [ABSTRACT FROM AUTHOR]

Published

2023

33. European Commission Grants Orphan Medicinal Product Designation for Navenibart, Astria Therapeutics' Investigational Therapy for the Treatment of Hereditary Angioedema

Subjects

Monoclonal antibodies, Kallikrein, Angioneurotic edema -- Drug therapy, Business, Business, international, European Union. European Commission

Abstract

BOSTON -- Astria Therapeutics, Inc. (Nasdaq:ATXS), a biopharmaceutical company focused on developing life-changing therapies for allergic and immunologic diseases, today announced that the European Commission (EC) has granted Orphan Medicinal [...]

Published

2024

34. Astria Therapeutics Receives FDA Orphan Drug Designation for Navenibart (STAR-0215) for the Treatment of Hereditary Angioedema

Subjects

United States. Food and Drug Administration, Biological products, Orphan drugs, Monoclonal antibodies, Kallikrein, Angioneurotic edema -- Drug therapy, Business, Business, international

Abstract

BOSTON -- Astria Therapeutics, Inc. (Nasdaq:ATXS), a biopharmaceutical company focused on developing life-changing therapies for allergic and immunologic diseases, today announced that navenibart (STAR-0215) has been granted Orphan Drug Designation [...]

Published

2024

35. KalVista Announces the Submission of Additional Marketing Authorization Applications for Sebetralstat for the Oral On-Demand Treatment of Hereditary Angioedema

Subjects

United States. Food and Drug Administration, Marketing, Kallikrein, Angioneurotic edema -- Drug therapy, Business, Business, international

Abstract

- Submissions support KalVista's mission of building a global footprint for sebetralstat to address the significant unmet need for people with HAE worldwide - - If approved, sebetralstat will be [...]

Published

2024

36. KalVista Announces FDA Acceptance of New Drug Application for Sebetralstat for Oral On-Demand Treatment of Hereditary Angioedema

Subjects

United States. Food and Drug Administration, Drugs -- Prescribing, Children -- Health aspects, Kallikrein, Angioneurotic edema -- Drug therapy, Business, Business, international

Abstract

- If approved, sebetralstat will be the first, oral on-demand treatment for HAE - - FDA PDUFA goal date of June 17, 2025 - CAMBRIDGE, Mass. & SALISBURY, England -- [...]

Published

2024

37. Discovery of Teleost Plasma Kallikrein/Coagulation Factor XI-Like Gene from Channel Catfish (Ictalurus punctatus) and the Evidence that the Protein Encoded by it Acts as a Lectin.

Author

Tsutsui, Shigeyuki, Yoshimura, Asuka, Iwakuma, Yoshiharu, and Nakamura, Osamu

Subjects

*CHANNEL catfish, *KALLIKREIN, *TANDEM mass spectrometry, *TIME-of-flight mass spectrometry, *GEL permeation chromatography, *BLOOD coagulation factors, *HEPATOCYTE growth factor

Abstract

Mammalian plasma kallikrein (PK) and coagulation factor XI (fXI) are serine proteases that play in the kinin–kallikrein cascade and in the blood clotting pathway. These proteases share sequence homology and have four apple domains (APDs) and a serine protease domain (SPD) from their N-terminus to C-terminus. No homologs of these proteases are believed to be present in fish species, except for lobe-finned fish. Fish, however, have a unique lectin, named kalliklectin (KL), which is composed of APDs only. In the present study, we found genomic sequences encoding a protein with both APDs and SPD in a few cartilaginous and bony fishes, including the channel catfish Ictalurus punctatus, using bioinformatic analysis. Furthermore, we purified two ~ 70 kDa proteins from the blood plasma of the catfish using mannose-affinity and gel filtration chromatography sequentially. Using de novo sequencing with quadrupole time-of-flight tandem mass spectrometry, several internal amino acid sequences in these proteins were mapped onto possible PK/fXI-like sequences that are thought to be splicing variants. Exploration of APD-containing proteins in the hagfish genome database and phylogenetic analysis suggested that the PK/fXI-like gene originated from hepatocyte growth factor, and that the gene was acquired in a common ancestor of jawed fish. Synteny analysis provided evidence for chromosomal translocation around the PK/fXI-like locus that occurred in the common ancestor of holosteans and teleosts after separation from the lobe-finned fish lineage, or gene duplication into two chromosomes, followed by independent gene losses. This is the first identification of PK/fXI-like proteins in teleosts. [ABSTRACT FROM AUTHOR]

Published

2023

38. Effects of a Peptide Derived from the Primary Sequence of a Kallikrein Inhibitor Isolated from Bauhinia bauhinioides (pep-BbKI) in an Asthma–COPD Overlap (ACO) Model.

Author

Silva, Luana Laura Sales da, Barbosa, Jéssica Anastácia Silva, João, Juliana Morelli Lopes Gonçalves, Fukuzaki, Silvia, Camargo, Leandro do Nascimento, dos Santos, Tabata Maruyama, Campos, Elaine Cristina de, Costa, Arthur Silva, Saraiva-Romanholo, Beatriz Mangueira, Bezerra, Suellen Karoline Moreira, Lopes, Fernanda Tenório Quirino dos Santos, Bonturi, Camila Ramalho, Oliva, Maria Luiza Vilela, Leick, Edna Aparecida, Righetti, Renato Fraga, and Tibério, Iolanda de Fátima Lopes Calvo

Subjects

*PEPTIDES, *BAUHINIA, *KALLIKREIN, *OVALBUMINS, *ELASTASES, *MATRIX metalloproteinases, *INTERLEUKIN-17

Abstract

(1) There are several patients with asthma–COPD overlap (ACO). A peptide derived from the primary sequence of a kallikrein inhibitor isolated from Bauhinia bauhinioides (pep-BbKI) has potent anti-inflammatory and antioxidant effects. Purpose: To investigate the effects of pep-BbKI treatment in an ACO model and compare them with those of corticosteroids. (2) BALB/c mice were divided into groups: SAL (saline), OVA (ovalbumin), ELA (elastase), ACO (ovalbumin + elastase), ACO-pep-BbKI (treated with inhibitor), ACO-DX (dexamethasone treatment), ACO-DX-pep-BbKI (both treatments), and SAL-pep-BbKI (saline group treated with inhibitor). We evaluated: hyperresponsiveness to methacholine, bronchoalveolar lavage fluid (BALF), exhaled nitric oxide (eNO), IL-1β, IL-4, IL-5, IL-6, IL-10, IL-13, IL-17, IFN-γ, TNF-α, MMP-9, MMP-12, TGF-β, collagen fibers, iNOS, eNO, linear mean intercept (Lm), and NF-κB in airways (AW) and alveolar septa (AS). (3) ACO-pep-BbKI reversed ACO alterations and was similar to SAL in all mechanical parameters, Lm, neutrophils, IL-5, IL-10, IL-17, IFN-γ, TNF-α, MMP-12 (AW), collagen fibers, iNOS (AW), and eNO (p > 0.05). ACO-DX reversed ACO alterations and was similar to SAL in all mechanical parameters, Lm, total cells and differentials, IL-1β(AS), IL-5 (AS), IL-6 (AS), IL-10 (AS), IL-13 (AS), IFN-γ, MMP-12 (AS), TGF-β (AS), collagen fibers (AW), iNOS, and eNO (p > 0.05). SAL was similar to SAL-pep-BbKI for all comparisons (p > 0.05). (4) Pep-BbKI was similar to dexamethasone in reducing the majority of alterations of this ACO model. [ABSTRACT FROM AUTHOR]

Published

2023

39. Mise au point sur les angiœdèmes héréditaires et leurs nouvelles thérapeutiques.

Author

Launay, D., Bouillet, L., Boccon-Gibod, I., Trumbic, B., Gobert, D., and Fain, O.

Abstract

Les angiœdèmes héréditaires, avec ou sans déficit en C1-inhibiteur, sont des maladies rares caractérisées par des crises récurrentes d'œdème non inflammatoire sous-cutané et/ou sous-muqueux. Elles peuvent menacer le pronostic vital et impacter substantiellement la qualité de vie. Les crises peuvent être spontanées ou provoquées, dans un contexte de stress émotionnel, par les infections ou les traumatismes physiques en particulier. Le médiateur-clé étant la bradykinine, ces angiœdèmes ne répondent pas aux thérapeutiques usuelles des angiœdèmes mastocytaires (antihistaminiques, corticoïdes, adrénaline), beaucoup plus fréquents. La prise en charge thérapeutique des angiœdèmes héréditaires consiste d'abord à traiter les crises sévères par un antagoniste sélectif du récepteur B2 de la bradykinine ou un concentré de C1-inhibiteur. Les concentrés de C1-inhibiteur ou un androgène atténué (danazol) peuvent être utilisés en prophylaxie à court terme. Les options thérapeutiques classiquement proposées pour la prévention des crises à long terme (danazol, antifibrinolytiques [acide tranexamique], concentré de C1-inhibiteur) sont d'efficacité variable et/ou posent des problèmes de tolérance ou de facilité d'emploi. La mise à disposition récente de molécules innovantes de la classe des inhibiteurs de la kallicréine comme traitement de fond (lanadelumab sous-cutané, bérotralstat oral) constitue une avancée thérapeutique importante dans la prophylaxie à long terme des crises d'angiœdème héréditaire. L'arrivée de ces nouvelles molécules s'accompagne d'une nouvelle ambition pour les patients : obtenir le contrôle optimal de la maladie pour limiter au maximum son retentissement sur la qualité de vie du patient. Hereditary angioedema, with or without deficient C1 inhibitor level or function, is a rare disease characterized by recurrent attacks of noninflammatory subcutaneous and/or submucosal edema. It may be life-threatening and substantially affects quality of life. Attacks may be spontaneous or induced, in a setting of emotional stress, by infections or physical trauma, in particular. As the key mediator is bradykinin, this angioedema does not respond to the usual treatments of mast cell-mediated angioedema (antihistamines, corticosteroids, adrenaline), which is much more frequent. Therapeutic management of hereditary angioedema first consists in treating severe attacks with a selective B2 bradykinin receptor antagonist or a C1 inhibitor concentrate. The latter or an attenuated androgen (danazol) can be used for short-term prophylaxis. Therapeutic solutions conventionally proposed for long-term prophylaxis (danazol, antifibrinolytics [tranexamic acid], C1 inhibitor concentrate) vary in efficacy and/or pose problems of safety or ease of use. Kallikrein inhibitors (subcutaneous lanadelumab, oral berotralstat) recently made available as disease-modifying treatment constitute an important advance in long-term prophylaxis of hereditary angioedema attacks. The advent of these new drugs is accompanied by a new ambition for patients: optimize control of the disease and thereby minimize its impact on quality of life. [ABSTRACT FROM AUTHOR]

Published

2023

40. Mechanisms involved in hereditary angioedema with normal C1-inhibitor activity.

Author

Shamanaev, Aleksandr, Dickeson, S. Kent, Ivanov, Ivan, Litvak, Maxim, Mao-Fu Sun, Kumar, Sunil, Quifang Cheng, Srivastava, Priyanka, He, Tracey Z., and Gailani, David

Subjects

ANGIONEUROTIC edema, ZYMOGENS, EDEMA, PLASMINOGEN, PLASMIN, LYSINE, GLUTAMIC acid

Abstract

Patients with the inherited disorder hereditary angioedema (HAE) suffer from episodes of soft tissue swelling due to excessive bradykinin production. In most cases, dysregulation of the plasma kallikrein-kinin system due to deficiency of plasma C1 inhibitor is the underlying cause. However, at least 10% of HAE patients have normal plasma C1 inhibitor activity levels, indicating their syndrome is the result of other causes. Two mutations in plasma protease zymogens that appear causative for HAE with normal C1 inhibitor activity have been identified in multiple families. Both appear to alter protease activity in a gain-of-function manner. Lysine or arginine substitutions for threonine 309 in factor XII introduces a new protease cleavage site that results in formation of a truncated factor XII protein (Δfactor XII) that accelerates kallikrein-kinin system activity. A glutamic acid substitution for lysine 311 in the fibrinolytic protein plasminogen creates a consensus binding site for lysine/arginine side chains. The plasmin form of the variant plasminogen cleaves plasma kininogens to release bradykinin directly, bypassing the kallikrein-kinin system. Here we review work on the mechanisms of action of the FXII-Lys/Arg309 and Plasminogen-Glu311 variants, and discuss the clinical implications of these mechanisms. [ABSTRACT FROM AUTHOR]

Published

2023

41. Predictive value of kallikrein forms and β-microseminoprotein in blood from patients with evidence of detectable levels of PSA after radical prostatectomy.

Author

Pellegrino, Francesco, Sjoberg, Daniel D., Tin, Amy L., Benfante, Nicole E., Briganti, Alberto, Montorsi, Francesco, Scardino, Peter T., Eastham, James A., Vickers, Andrew J., Lilja, Hans, and Laudone, Vincent P.

Subjects

*RADICAL prostatectomy, *PROSTATE-specific antigen, *KALLIKREIN, *GLEASON grading system, *PROSTATE cancer patients

Abstract

Purpose: To determine whether β-microseminoprotein or any of the kallikrein forms in blood-free, total or intact PSA or total hK2-predict metastasis in patients with evidence of detectable levels of PSA in blood after radical prostatectomy. Method: We determined marker concentrations in blood from 173 men treated with radical prostatectomy and evidence of detectable levels of PSA in the blood (PSA ≥ 0.05) after surgery between 2014 and 2015 and at least 1 year after any adjuvant therapy. We used Cox regression to determine whether any marker was associated with metastasis using both univariate and multivariable models that included standard clinical predictors. Results: Overall, 42 patients had metastasis, with a median follow-up of 67 months among patients without an event. The levels of intact and free PSA and free-to-total PSA ratio were significantly associated with metastasis. Discrimination was highest for free PSA (c-index: 0.645) and free-to-total PSA ratio (0.625). Only free-to-total PSA ratio remained associated with overall metastasis (either regional or distant) after including standard clinical predictors (p = 0.025) and increased discrimination from 0.686 to 0.697. Similar results were found using distant metastasis as an outcome (p = 0.011; c-index increased from 0.658 to 0.723). Conclusion: Our results provide evidence that free-to-total PSA ratio can risk stratifying patients with evidence of detectable levels of PSA in blood after RP. Further research is warranted on the biology of prostate cancer markers in patients with evidence of detectable levels of PSA in blood after radical prostatectomy. Our findings on the free-to-total ratio for predicting adverse oncologic outcomes need to be validated in other cohorts. [ABSTRACT FROM AUTHOR]

Published

2023

42. Safety Aspects and Rational Use of Lanadelumab Injections in the Treatment of Hereditary Angioedema (HAE): Clinical Insights

Author

Petkova E, Yordanova V, Staevska M, and Valerieva A

Subjects

hereditary angioedema, c1 inhibitor, bradykinin, kallikrein, lanadelumab, drug safety, Medicine (General), R5-920

Abstract

Elena Petkova, Vanya Yordanova, Maria Staevska, Anna Valerieva Department of Allergology, Medical University of Sofia, University Hospital “Alexandrovska”, Sofia, BulgariaCorrespondence: Anna Valerieva, Email anna.valerieva@gmail.comAbstract: Hereditary angioedema (HAE) is a rare genetic disorder characterized by recurrent episodes of skin/mucosal swelling, and/or attacks of severe abdominal pain when it affects the gastrointestinal tract. The disease might be unexpectedly fatal when the upper airways are compromised. HAE clinical presentation, disease course and prognosis are associated with significant disease burden and severely impaired quality of life. Lanadelumab is a breakthrough therapy for the prevention of attacks in HAE type 1 and 2 patients. This revolutionary approach to administer a single subcutaneous injection (once every two to four weeks) and achieve complete disease control has dramatically improved patient care resulting in significant change in the life of affected families. Current data support the drug’s tolerability in adult and adolescent patients without notable safety concerns in both clinical research and real-world settings. Rational use of prophylactic treatments of HAE searches for a socio-economic balance, taking into account the life-long course of the disease, the public health funds who pay the monetary price, and the patients who might need to receive the therapy for a period longer than investigated during the development program. In this review, we address the current evidence on lanadelumab’s tolerability, highlighting aspects of the drug’s rationale use in clinical practice. Further studies need to investigate whether this therapy might be appropriate in other forms of angioedema, such as idiopathic primary angioedema and HAE with normal C1 inhibitor. Future efforts must focus to improve modern drugs’ accessibility in more countries. Although modern prophylactic options lessen the risk of fatal laryngeal attacks, patients must be equipped with reliable on-demand therapies and be trained how to use them as such a risk cannot be fully diminished with potentially life-threatening attacks occurring even in subjects with successful and stable long-term prophylaxis. Notwithstanding, further studies are needed to identify early responders from non-responders and develop therapies for the latter.Keywords: hereditary angioedema, C1 inhibitor, bradykinin, kallikrein, lanadelumab, drug safety

Published

2022

43. Donidalorsen Reduces Attacks in Patients With Hereditary Angioedema

Author

Park, Brian

Subjects

Kallikrein, Angioneurotic edema -- Drug therapy -- Complications and side effects, Health

Abstract

Topline results were announced from a phase 3 study evaluating the efficacy and safety of donidalorsen in patients with hereditary angioedema (HAE). Donidalorsen is an investigational ligand-conjugated antisense (LICA) drug [...]

Published

2024

44. Proteomics of fibrin amyloid microclots in long COVID/post-acute sequelae of COVID-19 (PASC) shows many entrapped pro-inflammatory molecules that may also contribute to a failed fibrinolytic system

Author

Arneaux Kruger, Mare Vlok, Simone Turner, Chantelle Venter, Gert Jacobus Laubscher, Douglas B. Kell, and Etheresia Pretorius

Subjects

Long COVID, Microclots, Platelet hyperactivation, von Willebrand factor, Kallikrein, Platelet factor 4, Diseases of the circulatory (Cardiovascular) system, RC666-701

Abstract

Abstract Background Post-acute sequelae of COVID-19 (PASC), also now known as long COVID, has become a major global health and economic burden. Previously, we provided evidence that there is a significant insoluble fibrin amyloid microclot load in the circulation of individuals with long COVID, and that these microclots entrap a substantial number of inflammatory molecules, including those that might prevent clot breakdown. Scientifically, the most challenging aspect of this debilitating condition is that traditional pathology tests such as a serum CRP (C-reactive protein) may not show any significant abnormal inflammatory markers, albeit these tests measure only the soluble inflammatory molecules. Elevated, or abnormal soluble biomarkers such as IL-6, D-Dimer or fibrinogen indicate an increased risk for thrombosis or a host immune response in COVID-19. The absence of biomarkers in standard pathology tests, result in a significant amount of confusion for patients and clinicians, as patients are extremely sick or even bed-ridden but with no regular identifiable reason for their disease. Biomarkers that are currently available cannot detect the molecules present in the microclots we identified and are therefore unable to confirm their presence or the mechanisms that drive their formation. Methods Here we analysed the protein content of double-digested microclots of 99 long COVID patients and 29 healthy controls. The patients suffering from long COVID reported their symptoms through a questionnaire completed by themselves or their attending physician. Results Our long COVID cohort’s symptoms were found to be in line with global findings, where the most prevalent symptoms were constant fatigue (74%,) cognitive impairment (71%) and depression and anxiety (30%). Our most noteworthy findings were a reduced level of plasma Kallikrein compared to our controls, an increased level of platelet factor 4 (PF4) von Willebrand factor (VWF), and a marginally increased level of α-2 antiplasmin (α-2-AP). We also found a significant presence of antibodies entrapped inside these microclots. Conclusion Our results confirm the presence of pro-inflammatory molecules that may also contribute to a failed fibrinolysis phenomenon, which could possibly explain why individuals with long COVID suffer from chronic fatigue, dyspnoea, or cognitive impairment. In addition, significant platelet hyperactivation was noted. Hyperactivation will result in the granular content of platelets being shed into the circulation, including PF4. Overall, our results provide further evidence of both a failed fibrinolytic system in long COVID/PASC and the entrapment of many proteins whose presence might otherwise go unrecorded. These findings might have significant implications for individuals with pre-existing comorbidities, including cardiovascular disease and type 2 diabetes.

Published

2022

45. Genetic Ablation and Pharmacological Blockade of Bradykinin B1 Receptor Unveiled a Detrimental Role for the Kinin System in Chagas Disease Cardiomyopathy.

Author

Oliveira, Ana Carolina, Vicentino, Amanda Roberta Revoredo, Andrade, Daniele, Pereira, Isabela Resende, Saboia-Vahia, Leonardo, Moreira, Otacílio da Cruz, Carvalho-Pinto, Carla Eponina, Mota, Julia Barbalho da, Maciel, Leonardo, Vilar-Pereira, Glaucia, Pesquero, João B., Lannes-Vieira, Joseli, Sirois, Pierre, Campos de Carvalho, Antônio Carlos, and Scharfstein, Julio

Subjects

*CHAGAS' disease, *BRADYKININ receptors, *CARDIOMYOPATHIES, *PARASITIC diseases, *HEART fibrosis, *BLUNT trauma, *TRICHOMONIASIS

Abstract

Chagas disease, the parasitic infection caused by Trypanosoma cruzi, afflicts about 6 million people in Latin America. Here, we investigated the hypothesis that T. cruzi may fuel heart parasitism by activating B1R, a G protein-coupled (brady) kinin receptor whose expression is upregulated in inflamed tissues. Studies in WT and B1R−/− mice showed that T. cruzi DNA levels (15 days post infection—dpi) were sharply reduced in the transgenic heart. FACS analysis revealed that frequencies of proinflammatory neutrophils and monocytes were diminished in B1R−/− hearts whereas CK-MB activity (60 dpi) was exclusively detected in B1R+/+ sera. Since chronic myocarditis and heart fibrosis (90 dpi) were markedly attenuated in the transgenic mice, we sought to determine whether a pharmacological blockade of the des-Arg9-bradykinin (DABK)/B1R pathway might alleviate chagasic cardiomyopathy. Using C57BL/6 mice acutely infected by a myotropic T. cruzi strain (Colombian), we found that daily treatment (15–60 dpi) with R-954 (B1R antagonist) reduced heart parasitism and blunted cardiac injury. Extending R-954 treatment to the chronic phase (120–160 dpi), we verified that B1R targeting (i) decreased mortality indexes, (ii) mitigated chronic myocarditis, and (iii) ameliorated heart conduction disturbances. Collectively, our study suggests that a pharmacological blockade of the proinflammatory KKS/DABK/B1R pathway is cardioprotective in acute and chronic Chagas disease. [ABSTRACT FROM AUTHOR]

Published

2023

46. Peptides Derived from a Plant Protease Inhibitor of the Coagulation Contact System Decrease Arterial Thrombus Formation in a Murine Model, without Impairing Hemostatic Parameters.

Author

De Souza, Daniel Alexandre, Salu, Bruno Ramos, Nogueira, Ruben Siedlarczyk, de Carvalho Neto, José Carlos Sá, Maffei, Francisco Humberto de Abreu, and Oliva, Maria Luiza Vilela

Subjects

*PEPTIDES, *PROTEASE inhibitors, *PLANT proteins, *BLOOD platelet aggregation, *THROMBOSIS, *TRYPSIN, *SERINE proteinases

Abstract

Several plant protein inhibitors with anticoagulant properties have been studied and characterized, including the Delonix regia trypsin inhibitor (DrTI). This protein inhibits serine proteases (trypsin) and enzymes directly involved in coagulation, such as plasma kallikrein, factor XIIa, and factor XIa. In this study, we evaluated the effects of two new synthetic peptides derived from the primary sequence of DrTI in coagulation and thrombosis models to understand the mechanisms involved in the pathophysiology of thrombus formation as well as in the development of new antithrombotic therapies. Both peptides acted on in vitro hemostasis-related parameters, showing promising results, prolonging the Partially Activated Thromboplastin Time (aPTT) and inhibited platelet aggregation induced by adenosine diphosphate (ADP) and arachidonic acid. In murine models, for arterial thrombosis induced by photochemical injury, and platelet-endothelial interactions monitored by intravital microscopy, both peptides at doses of 0.5 mg/kg significantly extended the time of artery occlusion and modified the platelet adhesion and aggregation pattern with no changes in bleeding time, demonstrating the high biotechnological potential of both molecules. [ABSTRACT FROM AUTHOR]

Published

2023

47. Human plasma kallikrein: roles in coagulation, fibrinolysis, inflammation pathways, and beyond

Author

Guacyara Motta, Luiz Juliano, and Jair Ribeiro Chagas

Subjects

bradykinin, kininogen, kallikrein, proteolysis, cell biology, inflammation, Physiology, QP1-981

Abstract

Human plasma kallikrein (PKa) is obtained by activating its precursor, prekallikrein (PK), historically named the Fletcher factor. Human PKa and tissue kallikreins are serine proteases from the same family, having high- and low-molecular weight kininogens (HKs and LKs) as substrates, releasing bradykinin (Bk) and Lys-bradykinin (Lys-Bk), respectively. This review presents a brief history of human PKa with details and recent observations of its evolution among the vertebrate coagulation proteins, including the relations with Factor XI. We explored the role of Factor XII in activating the plasma kallikrein–kinin system (KKS), the mechanism of activity and control in the KKS, and the function of HK on contact activation proteins on cell membranes. The role of human PKa in cell biology regarding the contact system and KSS, particularly the endothelial cells, and neutrophils, in inflammatory processes and infectious diseases, was also approached. We examined the natural plasma protein inhibitors, including a detailed survey of human PKa inhibitors’ development and their potential market.

Published

2023

48. 'Anti-Plasma Kallikrein Antibody Dosing Regimens For Treating Hereditary Angioedema' in Patent Application Approval Process (USPTO 20240343829)

Subjects

Intellectual property, Lanadelumab -- Intellectual property, Kallikrein, Patient compliance, Amino acids -- Intellectual property, Biological products -- Intellectual property

Abstract

2024 NOV 4 (NewsRx) -- By a News Reporter-Staff News Editor at Pharma Business Week -- A patent application by the inventors Chung, Jou-Ku (Brookline, MA, US); Morabito, Christopher John [...]

Published

2024

49. Patent Issued for Human plasma kallikrein inhibitors (USPTO 12116346)

Subjects

BioCryst Pharmaceuticals Inc. -- Intellectual property, Intellectual property, Kallikrein, Pharmaceutical industry -- Intellectual property

Abstract

2024 NOV 4 (NewsRx) -- By a News Reporter-Staff News Editor at Hematology Week -- According to news reporting originating from Alexandria, Virginia, by NewsRx journalists, a patent by the [...]

Published

2024

50. Researchers Submit Patent Application, 'Evaluation, Assays And Treatment Of Pkalmediated Disorders', for Approval (USPTO 20240310377)

Subjects

Bradykinin, Enzymes -- Intellectual property, Kallikrein, Pharmaceutical industry -- Intellectual property, Takeda Pharmaceutical Company Ltd. -- Intellectual property

Abstract

2024 OCT 11 (NewsRx) -- By a News Reporter-Staff News Editor at Angiogenesis Weekly -- From Washington, D.C., NewsRx journalists report that a patent application by the inventors Joseph, Kusumam [...]

Published

2024