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	<id>https://wiki.mininuniver.ru/index.php?action=history&amp;feed=atom&amp;title=~Delete_31202</id>
	<title>~Delete 31202 - История изменений</title>
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	<updated>2026-04-21T04:43:19Z</updated>
	<subtitle>История изменений этой страницы в вики</subtitle>
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	<entry>
		<id>https://wiki.mininuniver.ru/index.php?title=~Delete_31202&amp;diff=467036&amp;oldid=prev</id>
		<title>Moderator: Moderator переименовал страницу The Capabilities and Positive aspects of LY2228820 в ~Delete 31202: Spam</title>
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		<updated>2025-12-26T16:04:50Z</updated>

		<summary type="html">&lt;p&gt;Moderator переименовал страницу &lt;a href=&quot;/index.php/The_Capabilities_and_Positive_aspects_of_LY2228820&quot; class=&quot;mw-redirect&quot; title=&quot;The Capabilities and Positive aspects of LY2228820&quot;&gt;The Capabilities and Positive aspects of LY2228820&lt;/a&gt; в &lt;a href=&quot;/index.php/~Delete_31202&quot; title=&quot;~Delete 31202&quot;&gt;~Delete 31202&lt;/a&gt;: Spam&lt;/p&gt;
&lt;table class=&quot;diff diff-contentalign-left&quot; data-mw=&quot;interface&quot;&gt;
				&lt;tr class=&quot;diff-title&quot; lang=&quot;ru&quot;&gt;
				&lt;td colspan=&quot;1&quot; style=&quot;background-color: #fff; color: #222; text-align: center;&quot;&gt;← Предыдущая&lt;/td&gt;
				&lt;td colspan=&quot;1&quot; style=&quot;background-color: #fff; color: #222; text-align: center;&quot;&gt;Версия 16:04, 26 декабря 2025&lt;/td&gt;
				&lt;/tr&gt;&lt;tr&gt;&lt;td colspan=&quot;2&quot; class=&quot;diff-notice&quot; lang=&quot;ru&quot;&gt;&lt;div class=&quot;mw-diff-empty&quot;&gt;(нет различий)&lt;/div&gt;
&lt;/td&gt;&lt;/tr&gt;&lt;/table&gt;</summary>
		<author><name>Moderator</name></author>
		
	</entry>
	<entry>
		<id>https://wiki.mininuniver.ru/index.php?title=~Delete_31202&amp;diff=467035&amp;oldid=prev</id>
		<title>Moderator: Spam cleanup</title>
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		<updated>2025-12-26T16:04:47Z</updated>

		<summary type="html">&lt;p&gt;Spam cleanup&lt;/p&gt;
&lt;table class=&quot;diff diff-contentalign-left&quot; data-mw=&quot;interface&quot;&gt;
				&lt;col class=&quot;diff-marker&quot; /&gt;
				&lt;col class=&quot;diff-content&quot; /&gt;
				&lt;col class=&quot;diff-marker&quot; /&gt;
				&lt;col class=&quot;diff-content&quot; /&gt;
				&lt;tr class=&quot;diff-title&quot; lang=&quot;ru&quot;&gt;
				&lt;td colspan=&quot;2&quot; style=&quot;background-color: #fff; color: #222; text-align: center;&quot;&gt;← Предыдущая&lt;/td&gt;
				&lt;td colspan=&quot;2&quot; style=&quot;background-color: #fff; color: #222; text-align: center;&quot;&gt;Версия 16:04, 26 декабря 2025&lt;/td&gt;
				&lt;/tr&gt;&lt;tr&gt;&lt;td colspan=&quot;2&quot; class=&quot;diff-lineno&quot; id=&quot;mw-diff-left-l1&quot; &gt;Строка 1:&lt;/td&gt;
&lt;td colspan=&quot;2&quot; class=&quot;diff-lineno&quot;&gt;Строка 1:&lt;/td&gt;&lt;/tr&gt;
&lt;tr&gt;&lt;td class='diff-marker'&gt;−&lt;/td&gt;&lt;td style=&quot;color: #222; font-size: 88%; border-style: solid; border-width: 1px 1px 1px 4px; border-radius: 0.33em; border-color: #ffe49c; vertical-align: top; white-space: pre-wrap;&quot;&gt;&lt;div&gt;&lt;del class=&quot;diffchange diffchange-inline&quot;&gt;INTRODUCTION:&lt;/del&gt;&lt;/div&gt;&lt;/td&gt;&lt;td class='diff-marker'&gt;+&lt;/td&gt;&lt;td style=&quot;color: #222; font-size: 88%; border-style: solid; border-width: 1px 1px 1px 4px; border-radius: 0.33em; border-color: #a3d3ff; vertical-align: top; white-space: pre-wrap;&quot;&gt;&lt;div&gt;&lt;ins class=&quot;diffchange diffchange-inline&quot;&gt;Content removed&lt;/ins&gt;&lt;/div&gt;&lt;/td&gt;&lt;/tr&gt;
&lt;tr&gt;&lt;td class='diff-marker'&gt;−&lt;/td&gt;&lt;td style=&quot;color: #222; font-size: 88%; border-style: solid; border-width: 1px 1px 1px 4px; border-radius: 0.33em; border-color: #ffe49c; vertical-align: top; white-space: pre-wrap;&quot;&gt;&lt;div&gt;&lt;del class=&quot;diffchange diffchange-inline&quot;&gt;P38 MAPK when activated causes the increased manufacturing of cytokines by inhibiting the degradation of their messenger RNA. On the opposite, if the p38 MAPK inhibition is suppressed, the cytokine creation is also inhibited. These are the cytokines which may probably make the osteoclastic action and increased bone decline in multiple myeloma [1, two and 3].&lt;/del&gt;&lt;/div&gt;&lt;/td&gt;&lt;td colspan=&quot;2&quot;&gt; &lt;/td&gt;&lt;/tr&gt;
&lt;tr&gt;&lt;td class='diff-marker'&gt;−&lt;/td&gt;&lt;td style=&quot;color: #222; font-size: 88%; border-style: solid; border-width: 1px 1px 1px 4px; border-radius: 0.33em; border-color: #ffe49c; vertical-align: top; white-space: pre-wrap;&quot;&gt;&lt;div&gt;&lt;del class=&quot;diffchange diffchange-inline&quot;&gt;LY2228820 WHY Essential?&lt;/del&gt;&lt;/div&gt;&lt;/td&gt;&lt;td colspan=&quot;2&quot;&gt; &lt;/td&gt;&lt;/tr&gt;
&lt;tr&gt;&lt;td class='diff-marker'&gt;−&lt;/td&gt;&lt;td style=&quot;color: #222; font-size: 88%; border-style: solid; border-width: 1px 1px 1px 4px; border-radius: 0.33em; border-color: #ffe49c; vertical-align: top; white-space: pre-wrap;&quot;&gt;&lt;div&gt;&lt;del class=&quot;diffchange diffchange-inline&quot;&gt;It must really be remembered that bone loss and destruction is incredibly common in numerous myeloma and hence a individual may possibly nicely experience from bone discomfort, a lot of bone fractures, hypocalcaemia and bad substantial high quality of life [4]. LY2228820 is generally a powerful p38 MAPK inhibitor, which in change decreases the generation of several cytokines within the physique which are dependable for bone loss and destruction, specifically in many myeloma. The cytokines in the bone marrow microenvironment as effectively as the direct cell to mobile get in contact with generates the proliferation, molecular resistance and survival in various myeloma cells in addition to the differentiation and activation of osteoclasts [5].&lt;/del&gt;&lt;/div&gt;&lt;/td&gt;&lt;td colspan=&quot;2&quot;&gt; &lt;/td&gt;&lt;/tr&gt;
&lt;tr&gt;&lt;td class='diff-marker'&gt;−&lt;/td&gt;&lt;td style=&quot;color: #222; font-size: 88%; border-style: solid; border-width: 1px 1px 1px 4px; border-radius: 0.33em; border-color: #ffe49c; vertical-align: top; white-space: pre-wrap;&quot;&gt;&lt;div&gt;&lt;del class=&quot;diffchange diffchange-inline&quot;&gt;LY2228820 Effectiveness AND STRENGHT:&lt;/del&gt;&lt;/div&gt;&lt;/td&gt;&lt;td colspan=&quot;2&quot;&gt; &lt;/td&gt;&lt;/tr&gt;
&lt;tr&gt;&lt;td class='diff-marker'&gt;−&lt;/td&gt;&lt;td style=&quot;color: #222; font-size: 88%; border-style: solid; border-width: 1px 1px 1px 4px; border-radius: 0.33em; border-color: #ffe49c; vertical-align: top; white-space: pre-wrap;&quot;&gt;&lt;div&gt;&lt;del class=&quot;diffchange diffchange-inline&quot;&gt;LY2228820 modulates the bone marrow microenvironment of numerous myeloma cells, and inhibits the osteoclastogenesis. LY2228820 is usually a powerful and particular molecule that inhibits the kinase activities of MAPK at a extremely lower focus. The study studies have shown that fifty% inhibitory concentration of LY2228820 for p38a and p38b MAPK is just 7 nm and three nm respectively. Even so, the 50% inhibitory focus for other kinases like p38d MAPK, p38c MAPK, and so on is additional than 20 LM.&lt;/del&gt;&lt;/div&gt;&lt;/td&gt;&lt;td colspan=&quot;2&quot;&gt; &lt;/td&gt;&lt;/tr&gt;
&lt;tr&gt;&lt;td class='diff-marker'&gt;−&lt;/td&gt;&lt;td style=&quot;color: #222; font-size: 88%; border-style: solid; border-width: 1px 1px 1px 4px; border-radius: 0.33em; border-color: #ffe49c; vertical-align: top; white-space: pre-wrap;&quot;&gt;&lt;div&gt;&lt;del class=&quot;diffchange diffchange-inline&quot;&gt;LY2228820 Functions AND Actions:&lt;/del&gt;&lt;/div&gt;&lt;/td&gt;&lt;td colspan=&quot;2&quot;&gt; &lt;/td&gt;&lt;/tr&gt;
&lt;tr&gt;&lt;td class='diff-marker'&gt;−&lt;/td&gt;&lt;td style=&quot;color: #222; font-size: 88%; border-style: solid; border-width: 1px 1px 1px 4px; border-radius: 0.33em; border-color: #ffe49c; vertical-align: top; white-space: pre-wrap;&quot;&gt;&lt;div&gt;&lt;del class=&quot;diffchange diffchange-inline&quot;&gt;LY2228820 exhibits specific activity by down streaming the targets of p38 MAPK every single in MM mobile traces and LT-BMSCs. The molecule also delivers phosphorylation of MAPKAPK2 and HSP27. LY2228820 does not create immediate toxicity, every in human MM mobile lines and individuals MM cells.&lt;/del&gt;&lt;/div&gt;&lt;/td&gt;&lt;td colspan=&quot;2&quot;&gt; &lt;/td&gt;&lt;/tr&gt;
&lt;tr&gt;&lt;td class='diff-marker'&gt;−&lt;/td&gt;&lt;td style=&quot;color: #222; font-size: 88%; border-style: solid; border-width: 1px 1px 1px 4px; border-radius: 0.33em; border-color: #ffe49c; vertical-align: top; white-space: pre-wrap;&quot;&gt;&lt;div&gt;&lt;del class=&quot;diffchange diffchange-inline&quot;&gt;Another effect of LY2228820 is that it considerably raises the cytotoxicity and apoptosis created by bortezomib. For that cause, the mixture of LY2228820 alongside with bortezomib dramatically down regulates the expression of bortezomib made HSP27. That's why LY2228820 augments the cytotoxicity of bortezomib [6].&lt;/del&gt;&lt;/div&gt;&lt;/td&gt;&lt;td colspan=&quot;2&quot;&gt; &lt;/td&gt;&lt;/tr&gt;
&lt;tr&gt;&lt;td class='diff-marker'&gt;−&lt;/td&gt;&lt;td style=&quot;color: #222; font-size: 88%; border-style: solid; border-width: 1px 1px 1px 4px; border-radius: 0.33em; border-color: #ffe49c; vertical-align: top; white-space: pre-wrap;&quot;&gt;&lt;div&gt;&lt;del class=&quot;diffchange diffchange-inline&quot;&gt;Suppression of osteoclastogenesis by implies of LY2228820 has been verified more by the pit development assay that correlates utilizing the capabilities of osteoclastic routines. These are the benefits that show that p38 MAPK pathway also operates for the differentiation of osteoclasts from human CD14 cells by sRANKL and M-CSF. It actually is noteworthy that the inhibitory effects of bortezomib on osteoclastogenesis, which come about to be documented recently [7] might nicely be enhanced by using LY2228820 together with it.&lt;/del&gt;&lt;/div&gt;&lt;/td&gt;&lt;td colspan=&quot;2&quot;&gt; &lt;/td&gt;&lt;/tr&gt;
&lt;tr&gt;&lt;td class='diff-marker'&gt;−&lt;/td&gt;&lt;td style=&quot;color: #222; font-size: 88%; border-style: solid; border-width: 1px 1px 1px 4px; border-radius: 0.33em; border-color: #ffe49c; vertical-align: top; white-space: pre-wrap;&quot;&gt;&lt;div&gt;&lt;del class=&quot;diffchange diffchange-inline&quot;&gt;Summary:&lt;/del&gt;&lt;/div&gt;&lt;/td&gt;&lt;td colspan=&quot;2&quot;&gt; &lt;/td&gt;&lt;/tr&gt;
&lt;tr&gt;&lt;td class='diff-marker'&gt;−&lt;/td&gt;&lt;td style=&quot;color: #222; font-size: 88%; border-style: solid; border-width: 1px 1px 1px 4px; border-radius: 0.33em; border-color: #ffe49c; vertical-align: top; white-space: pre-wrap;&quot;&gt;&lt;div&gt;&lt;del class=&quot;diffchange diffchange-inline&quot;&gt;In conclusion, LY2228820 is a terrific molecule that could probably be utilised to suppress the osteoclastogenesis action in numerous myeloma cells. This molecule may be used in addition to bortezomib towards MM cells and that's why in this way, the motion may well be enhanced more. LY2228820 apart from creating outcomes for modulating the osteoclast development can display the inhibitory impacts in osteoclastogenesis in a SCID-hu MM design. Nevertheless, even more investigation should be accomplished to be able to good numerous other benefits of this molecule to ensure that it can be utilized for outstanding end result and reducing the impacts of illness on the human entire body.&lt;/del&gt;&lt;/div&gt;&lt;/td&gt;&lt;td colspan=&quot;2&quot;&gt; &lt;/td&gt;&lt;/tr&gt;
&lt;tr&gt;&lt;td class='diff-marker'&gt;−&lt;/td&gt;&lt;td style=&quot;color: #222; font-size: 88%; border-style: solid; border-width: 1px 1px 1px 4px; border-radius: 0.33em; border-color: #ffe49c; vertical-align: top; white-space: pre-wrap;&quot;&gt;&lt;div&gt; &lt;/div&gt;&lt;/td&gt;&lt;td colspan=&quot;2&quot;&gt; &lt;/td&gt;&lt;/tr&gt;
&lt;tr&gt;&lt;td class='diff-marker'&gt;−&lt;/td&gt;&lt;td style=&quot;color: #222; font-size: 88%; border-style: solid; border-width: 1px 1px 1px 4px; border-radius: 0.33em; border-color: #ffe49c; vertical-align: top; white-space: pre-wrap;&quot;&gt;&lt;div&gt;&lt;del class=&quot;diffchange diffchange-inline&quot;&gt;[http://www.entertainermedia.com/blogs/197441/311980/new-discoveries-in-cancer-treatm New Discoveries in Cancer Treatments Offer More Options], [http://www.purevolume.com/carrot67alloy/posts/4192374/New+Discoveries+in+Cancer+Treatments+Offer+More+Options Crizotinib, Dasatinib, Erlotinib], [http://beta.truck.net/blogs/325716/381969/new-discoveries-in-cancer-treatm Crizotinib, Dasatinib, Erlotinib]&lt;/del&gt;&lt;/div&gt;&lt;/td&gt;&lt;td colspan=&quot;2&quot;&gt; &lt;/td&gt;&lt;/tr&gt;
&lt;/table&gt;</summary>
		<author><name>Moderator</name></author>
		
	</entry>
	<entry>
		<id>https://wiki.mininuniver.ru/index.php?title=~Delete_31202&amp;diff=133634&amp;oldid=prev</id>
		<title>Heart96soy: Новая: INTRODUCTION: P38 MAPK when activated causes the increased manufacturing of cytokines by inhibiting the degradation of their messenger RNA. On the opposite, if the p38 MAPK inhibition is...</title>
		<link rel="alternate" type="text/html" href="https://wiki.mininuniver.ru/index.php?title=~Delete_31202&amp;diff=133634&amp;oldid=prev"/>
		<updated>2013-05-09T07:55:40Z</updated>

		<summary type="html">&lt;p&gt;Новая: INTRODUCTION: P38 MAPK when activated causes the increased manufacturing of cytokines by inhibiting the degradation of their messenger RNA. On the opposite, if the p38 MAPK inhibition is...&lt;/p&gt;
&lt;p&gt;&lt;b&gt;Новая страница&lt;/b&gt;&lt;/p&gt;&lt;div&gt;INTRODUCTION:&lt;br /&gt;
P38 MAPK when activated causes the increased manufacturing of cytokines by inhibiting the degradation of their messenger RNA. On the opposite, if the p38 MAPK inhibition is suppressed, the cytokine creation is also inhibited. These are the cytokines which may probably make the osteoclastic action and increased bone decline in multiple myeloma [1, two and 3].&lt;br /&gt;
LY2228820 WHY Essential?&lt;br /&gt;
It must really be remembered that bone loss and destruction is incredibly common in numerous myeloma and hence a individual may possibly nicely experience from bone discomfort, a lot of bone fractures, hypocalcaemia and bad substantial high quality of life [4]. LY2228820 is generally a powerful p38 MAPK inhibitor, which in change decreases the generation of several cytokines within the physique which are dependable for bone loss and destruction, specifically in many myeloma. The cytokines in the bone marrow microenvironment as effectively as the direct cell to mobile get in contact with generates the proliferation, molecular resistance and survival in various myeloma cells in addition to the differentiation and activation of osteoclasts [5].&lt;br /&gt;
LY2228820 Effectiveness AND STRENGHT:&lt;br /&gt;
LY2228820 modulates the bone marrow microenvironment of numerous myeloma cells, and inhibits the osteoclastogenesis. LY2228820 is usually a powerful and particular molecule that inhibits the kinase activities of MAPK at a extremely lower focus. The study studies have shown that fifty% inhibitory concentration of LY2228820 for p38a and p38b MAPK is just 7 nm and three nm respectively. Even so, the 50% inhibitory focus for other kinases like p38d MAPK, p38c MAPK, and so on is additional than 20 LM.&lt;br /&gt;
LY2228820 Functions AND Actions:&lt;br /&gt;
LY2228820 exhibits specific activity by down streaming the targets of p38 MAPK every single in MM mobile traces and LT-BMSCs. The molecule also delivers phosphorylation of MAPKAPK2 and HSP27. LY2228820 does not create immediate toxicity, every in human MM mobile lines and individuals MM cells.&lt;br /&gt;
Another effect of LY2228820 is that it considerably raises the cytotoxicity and apoptosis created by bortezomib. For that cause, the mixture of LY2228820 alongside with bortezomib dramatically down regulates the expression of bortezomib made HSP27. That's why LY2228820 augments the cytotoxicity of bortezomib [6].&lt;br /&gt;
Suppression of osteoclastogenesis by implies of LY2228820 has been verified more by the pit development assay that correlates utilizing the capabilities of osteoclastic routines. These are the benefits that show that p38 MAPK pathway also operates for the differentiation of osteoclasts from human CD14 cells by sRANKL and M-CSF. It actually is noteworthy that the inhibitory effects of bortezomib on osteoclastogenesis, which come about to be documented recently [7] might nicely be enhanced by using LY2228820 together with it.&lt;br /&gt;
Summary:&lt;br /&gt;
In conclusion, LY2228820 is a terrific molecule that could probably be utilised to suppress the osteoclastogenesis action in numerous myeloma cells. This molecule may be used in addition to bortezomib towards MM cells and that's why in this way, the motion may well be enhanced more. LY2228820 apart from creating outcomes for modulating the osteoclast development can display the inhibitory impacts in osteoclastogenesis in a SCID-hu MM design. Nevertheless, even more investigation should be accomplished to be able to good numerous other benefits of this molecule to ensure that it can be utilized for outstanding end result and reducing the impacts of illness on the human entire body.&lt;br /&gt;
&lt;br /&gt;
[http://www.entertainermedia.com/blogs/197441/311980/new-discoveries-in-cancer-treatm New Discoveries in Cancer Treatments Offer More Options], [http://www.purevolume.com/carrot67alloy/posts/4192374/New+Discoveries+in+Cancer+Treatments+Offer+More+Options Crizotinib, Dasatinib, Erlotinib], [http://beta.truck.net/blogs/325716/381969/new-discoveries-in-cancer-treatm Crizotinib, Dasatinib, Erlotinib]&lt;/div&gt;</summary>
		<author><name>Heart96soy</name></author>
		
	</entry>
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