Dating Apps – Does Your Teen Talk to Strangers?

Lack of affection often leads teens to dating sites and apps. They find strangers with whom they can share their insecurities. Many online dating apps for teens are popping up these days, which already has increased the parent’s concern. Teens find it interesting to meet new people and explore the personality of the new friend or partner. But every online user is not what it seems. Many groups prey on teens and make them involve in commercial sexual abuse or drug. In this post, we will share a list of dating apps and a solution that is known as parental control app.

Dating Apps – Ensure Your Teen is not Using!

Skout

Its recent update allows teens age 13-17 to create an account on Skout. Such news raises the eyebrows of the audience as they do not want the kids and teens to use such dating sites and apps. It allows people to find strangers online and leads to in-person meetings. The user can enter fake birth dates and interact with older people.

Tinder

Tinder lets the users match the profile through browsing the photos around the current location. A user should swipe right to like and swipe left to dislike. When mutually users like each other profiles, the app will allow them to message. Teens visit many accounts and develop an interest in vulgar content.

MyLOL

MyLOL is an app where a user can create a profile older than 13. But it does not let the user above 19 be on its app. Teens meet here with other same-age members and often develop bonding in real-life too. This app has terms and conditions against sharing sexual propositions. Any underage kid can create a profile here and share personal stuff with strangers.

MeetMe

To know the nearby people, MeetMe has come with its advanced features. A user should purchase credits to be in the top position so more nearby users can see the profile and get more chances to meet the new people. There is no age verification feature, and much live streaming promotes drug or alcohol consumption.

Kik

It is a well-designed app that does not involve a mobile number to log in. A user can sign in and can have a conversation with friends or even with strangers. It also allows its users to attach every video or multimedia files for sharing online. There are many public groups where your kid can go and get involved in drug consumption or pornography.

What’s A Better Solution to Prevent Teens from Using Dating Apps?

The parental control app is the top method to track the screen of the kids. Parents can manage the installed apps on their phones and uninstall them instantly without touching the mobile. Once the end-user downloads the app on the target device (from the official website), the next step is to start monitoring without blinking the eye. The most successful android parental control app in the market is TheWiSpy, which offers multiple features for kid’s monitoring. A parent can manage the installed apps in android phone and activities remotely. After its setup, the end-user can capture the screen and find out if the teens are meeting with strangers in person. It also gives access to the chats that will clear if they are sexting or not.

Wrapping Up

Dating apps are becoming common among teens. If your child is not aware of such sites, then one of his/her friends can share the experience. It will raise their interest in talking with strangers, and they will not think about the consequences. All you need is to find a reliable source for parental control apps and prevent a teen from using such an app. These sites are like the open gates to criminals that target the youth and make them do unlawful things. TheWiSpy is the best way to capture the screen and restrict access to adult content.

Sensual Health: Is a Taste of Mint Good or Bad?

Men who are concerned about appropriate male organ care – and every man should be – want to make sure they do all they can to ensure premium sensual health. But the world of sensual health matters is littered with all sorts of misinformation, old wives tales and myths. One of the recurring ones concerns the use of mint as it relates to the male member. According to some sources, mint can be a fine sensual aid, but other sources insist there are dangers to sensual health in the overuse of mint. So what is a guy to believe?

Mint

It seems as if mint is everywhere around us. Spearmint is a popular flavor of chewing gum. Peppermint candies are a treat for kids and adults alike. The range of mint teas seems to have grown exponentially. As menthol, mint is found in several brands of cigarettes and cough drops. And “minty fresh” has become synonymous with toothpastes and other oral hygiene products. It’s even used in some environmentally friendly pesticides in place of toxic chemicals.

There are well over a dozen different kinds of mint plants, and they grow across most of the inhabited continents (although not so often in South America). This popular herb can grow all year long in the appropriate conditions.

The male organ connection

So why should mint have any connection with the male organ? Certainly, anything that is ingested has the potential to affect parts of the body, including the manhood.

One of the more common theories associated with mint is that it has the effect of numbing the member naturally. According to this theory, performing oral sensual activity on a firm male organ after sucking on a mint cough drop will temporarily de-sensitize the member so it can stay harder for a longer period of time during sensual activity. A variant on this theory recommends using mint oil on a firm male organ for the same purpose.

There is a little scientific reasoning to back up this claim. Parts of the body contain a protein with a long scientific name, more generally known as TRPM8. When mint comes into contact with TRPM8, it sends a signal to the brain that says “Experience this sensation as cold.” So although mint itself is not cold, it makes the body think it is. And so the theory is that getting mint on a firm male organ will numb it sufficiently that it acts as a kind of “delay spray.” However, there are no studies to prove that mint applied to the manhood will indeed result in longer-lasting coupling.

Male hormone

And in fact, some people believe mint could have a negative effect on sensual health and function. Some men have claimed that mint depresses their sensual drive. A 2004 study involving mint tea given to male rats seemed to back this up. The intake of mint tea was associated with both an increase in female hormones and a decrease in male hormone.

A study in women with high male hormone levels later found the same thing – that mint caused their male hormone levels to drop and their female hormone levels to rise.

Since male hormone in men is associated with an increased sensual drive, the studies suggest that too much mint could indeed cause an effect. But more studies would be needed to definitively prove this.

Whether or not mint affects a man’s sensual health, it pays to keep his male member in excellent form. Daily use of a first-rate male organ health crème (health professionals recommend Man1 Man Oil, which is clinically proven mild and safe for skin) is a big aid in this regard. Choose a crème that contains the amino acid L-arginine, which is key to the development of nitric oxide. This in turn keeps male organ blood vessels open and receptive to increased blood flow. The best creme will also include a wide range of essential vitamins, such as A, B5, C, D and E.

Visit http://www.menshealthfirst.com for additional information on most common manhood health issues, tips on improving male organ sensitivity and what to do to maintain a healthy member. John Dugan is a professional writer who specializes in men’s health issues and is an ongoing contributing writer to numerous websites.

MDM2 degraders turned out to degrade p53?

PROTACs, fully known as Proteolysis-Targeting Chimeras, or proteolytically targeted chimeras, are a new drug type different from antibodies and traditional small molecule inhibitors and consist of three parts: target protein binder, linker, and E3 ubiquitin ligase binder. That is, one end of the PROTAC molecule binds to the target protein and the other end binds to the E3 ubiquitin ligase. E3 ubiquitin ligases, on the other hand, can label small proteins called ubiquitin as defective or damaged proteins by attaching them to target proteins. Afterwards, the cell’s protein crusher (i.e., proteasome) recognizes and degrades labeled target proteins.

In recent years, as a new way to regulate proteostasis, PROTAC has received much attention from academia and industry, and many teams are actively developing protein-degrading agents based on PROTAC technology. In terms of target proteins, it is statistically stated that there are currently more than 100 popular targets targeted by PROTAC, and the fastest progressing ones include AR-PROTAC, ER-PROTAC, BTK-PROTAC, etc.; in terms of E3 ubiquitin ligases, there are currently two most commonly used for PROTAC development, which are von Hippel Lindau (VHL) and cereblon (CRBN).

CRBN is part of the CRL4 E3 ubiquitin ligase that recognizes substrate proteins as substrate receptors (SRs), thereby initiating the degradation process. CRLs, the largest family of E3 ubiquitin ligases, form over 250 CRLs by assembling substrate acceptor and adapter proteins around different cullin backbones.

Simply put, molecular gel-degrading agents are a class of small molecules that can induce novel interactions between E3 ubiquitin ligase substrate receptors (e.g., CRBN) and target proteins, which lead to target protein degradation. Thalidomide, lenalidomide, and pondolamine small molecule immunomodulators are a remarkable example of molecular glues that redirect CRBN, thereby polyubiquitinating transcription factors IKZF1 and IKZF3, resulting in IKZF1 and IKZF3 degradation by the proteasome. Analogously, the anticancer sulfonamide indisulam also guides the interaction between the E3 ubiquitin ligase DCAF15 and RBM39 and promotes the degradation of RBM39. In conclusion, the development of molecular glue and PROTAC technology provides a new strategy for targeting pathogenic proteins, including many proteins targeted using traditional methods.

A team of scientists from the University of Wisconsin-Madison announced their development of a new type of MDM2 degradant in a paper published in the European Journal of Medicinal Chemistry.

MDM2, fully known as mouse double minute 2, is a key negative regulator of p53 (a powerful tumor suppressor, the most frequently mutated gene in human cancer), which is highly expressed in tumors and plays an important role in tumor development and progression. Previous studies have shown that MDM2 can not only bind to p53 to block its tumor suppressor transactivation domain, the protein itself is an E3 ligase that labels p53 for degradation by the proteasome. Since the wild-type p53 gene is retained in about 50% of human cancers, but the tumor suppressor function of these p53 is weakened by signaling molecules such as MDM2, the researchers hope that patients carrying wild-type p53 can restore the tumor suppressor activity of p53 by developing small molecule inhibitors or degradation agents to block the interaction between p53 and MDM2.

In August 2019, the team of scientists reported that they had developed a highly effective MDM2-PROTAC, WB156, which consists of a nutlin derivative linked to the CRBN ligand lenalidomide. In leukemia cells, WB156 is able to efficiently deplete MDM2 and activate wild-type p53, which in turn induces apoptosis. However, although WB156 is able to effectively degrade MDM2, induce p53 activation, and show anti-proliferative effects, this molecule can only act in a limited number of leukemia cell lines.

To overcome the bottleneck, scientists envision that fusion of different MDM2 ligands may enable MDM2 degraders to act in a wider range of cancers. In this newly published new study, they first prepared ligands for the development of MDM2 degraders by performing a four-component Ugi reaction using “MDM2 ligand 1″ and “MDM2 ligand 2″, and then used these ligands as binders of MDM2 to construct active MDM2 degraders. After extensive optimization, WB214 was identified as the most effective antiproliferative agent in various leukemia cell lines.

Surprisingly, mechanistic studies showed that this novel WB214 degrader did not activate p53, and conversely, WB214 induced the degradation of p53, which is completely opposite to the MDM2 degrader WB156 previously reported by the team.

Scientists have conducted a series of experiments to investigate the potential mechanisms of action behind this effect. The results showed that WB214-mediated degradation of the MDM2-p53 complex was achieved through the ubiquitin-proteasome system; p53 was a bystander in the MDM2 degradation process because it was directly associated with MDM2, thus producing a “bystander degradation effect”; and the WB214-CRBN complex did not bind MDM2 at the p53-binding site (in contrast, either MDM2 ligand 1 or WB13 bound MDM2 at the p53-binding site).

Since ternary complex formation is a prerequisite for proteasomal degradation, the researchers further analyzed WB214-induced ternary complex formation and confirmed that WB214 was able to effectively induce ternary complex formation in a dose-dependent manner and that WB214 induced a stronger CRBN-MDM2 interaction than WB156. These data suggest that unlike WB156 (bona fide MDM2 PROTAC), WB214 does not degrade MDM2 via the classical PROTAC mechanism. The mechanism of action of WB214 is more consistent with molecular glue. In other words, WB214 simply leads to binding to MDM2 by interacting with its CRBN. The authors state that MDM2 was first discovered to act as a new substrate (neo-substrate) for CRBN.