生殖細胞負責遺傳信息的時代傳遞，那么基因組的完整性對于生殖細胞至關重要。而在真核生物精細胞中，有許多外來侵入的轉座子、逆轉座子等移動型遺傳元件。這些自私的遺傳元件在染色體不同位點間跳躍，造成基因突變和基因組損傷。在生殖細胞中，轉座子的跳躍可能會導致不育。PiRNA/Piwi能夠高效的阻止轉座子等元件對基因組的損傷。研究發現，piRNA起源于反轉座子、重復序列等區域，與Piwi蛋白形成piRNA/Piwi機器，沉默轉座子、反轉座子等。此外，piRNA還可以發揮類似于siRNA的功能，參與調控生殖細胞中編碼基因的表達。

方法：

研究人員發現無精子癥患者體內Piwi（Hiwi）生殖突變會阻止其泛素化和降解。為了了解其中的作用機制，研究人員構建了Piwi（Miwi）突變敲入小鼠模型，證明了這種遺傳缺陷直接導致了男性不育癥。具體來說，研究人員發現MIWI能以一種對立于Piwi作用RNA（piRNA）的方式，與組蛋白泛素連接酶RNF8結合，并在晚期精子細胞的細胞質中穩定螯合RNF8，從而導致精子異常，引起組蛋白滯留，形態異常和活性嚴重受損，而這可以通過RNF8-N阻斷精子細胞中RNF8-MIWI的相互作用，逆轉功能。

結果1：

研究人員篩查了413例臨床無精、弱精癥患者Piwi基因上控制Piwi蛋白泛素化修飾降解的關鍵元件D-box，發現有3例病人在此元件中存在雜合性基因突變，且發現此類突變可來源于基因自發突變，也可從母親遺傳獲得。為鑒定此類突變是否是造成這些患者發生無精/少弱精的原因，研究人員將其中的一組突變條件型敲入小鼠Piwi基因，在小鼠模型中研究此類突變對精子發生的作用。他們發現， Piwi D-box雜合突變小鼠均出現雄性不育，精子表型也與患者*。深入研究發現，Miwi D-box雜合突變小鼠精子發生阻滯在延長型精子細胞發育階段，盡管能產生少量精子，但精子形態異常、細胞核結構疏松、無活力。

結果2：

機制研究揭示， PIWI蛋白具有將RNF8“扣留”于細胞核外的功能。正常小鼠體內PIWI蛋白會在精子發育后期被自然降解，RNF8進入細胞核內開啟“組蛋白-魚精蛋白轉換”，幫助精子發育完成。而Piwi蛋白突變導致其在后期不能被正常代謝，大量RNF8因此被“扣留”在細胞核外，魚精蛋白與組蛋白交換受阻，zui終造成精子發育受阻。將RNF8-N端導入突變小鼠的精子細胞后，可有效阻斷Piwi基因蛋白產物對RNF8的“扣留”，恢復精子的正常形態及游動能力，提示該策略對臨床治療此類無精、弱精癥具有重要理論參考價值。

Reproductive cells are responsible for the transmission of genetic information, then the integrity of the genome is crucial to the germ cells. In eukaryote, there are many intruded transposons, reverse transposons, and other genetic elements. These selfish genetic elements jump between chromosomal locations, causing gene mutations and genome damage. In the germ cells, the leaping of the transposon may lead to infertility. PiRNA/Piwi can effectively prevent the damage to the genome by the components of the transposon. It is found that piRNA originates in the retrotransposon, repeat sequence and other regions, and forms the piRNA/Piwi machine with the Piwi protein, silencing the transposon, and the retrotransposon. In addition, piRNA can also play a role similar to siRNA and participate in the regulation of the expression of encoded genes in the germ cells.

Method：

The researchers found that Piwi (Hiwi) mutagenesis in the body of azoospermia prevents its ubiquitination and degradation. In order to understand the mechanism, the researchers constructed a Piwi (Miwi) in mouse model of mutation, proved the genetic defects directly lead to male infertility. Specifically, the researchers found that MIWI in a Piwi RNA (piRNA) in the way of combination with histone RNF8 ubiquitin ligase, and stable chelate RNF8 in advanced sperm cell cytoplasm, resulting in abnormal sperm, cause protein retention, abnormal morphology and activity severely damaged, this can be done by RNF8-N blocking the interaction of RNF8-MIWI in sperm cells, reverse function.

Results 1:

The key element of D-box researchers screened 413 cases of azoospermia and weak sperm Piwi in patients with Piwi gene controlling protein ubiquitination and degradation, discovered the existence of heterozygous mutations in 3 patients in this element, and found that these mutations can be derived from spontaneous mutation gene can be inherited from his mother. For the identification of such mutations is the cause of azoospermia / little weak sperm occurred in these patients, the researchers will be a group of mutant type Piwi gene knock in mouse condition which, in a mouse model of such mutations on spermatogenesis function. They found that the Piwi D-box heterozygous mutant mice were male sterility, and the sperm phenotype was also consistent with the patient. Further studies showed that Miwi D-box heterozygous mutant mice had spermatogenesis arrest at the extended stage of spermatogenesis, although they produced a small amount of sperm, but the sperm morphology was abnormal, the nuclear structure was loose and inactive.

Results 2:

The mechanism studies have revealed that PIWI protein has the function of "withholding" RNF8 outside the nucleus. In normal mice, PIWI protein will be degraded naturally in the late stage of sperm development. RNF8 will enter into the nucleus and start the histone protamine transformation to help sperm development. However, the mutation of Piwi protein causes it to not be metabolize in the late stage. A large number of RNF8 is therefore "arrested" outside the nucleus. The exchange of protamine and histone is hindered, resulting in the development of sperm is blocked. After introducing the RNF8-N terminal into the spermatozoa of the mutant mice, it can effectively block the retention of Piwi protein products to RNF8 and restore the normal morphology and swimming ability of the sperm, suggesting that this strategy has important theoretical reference value for the clinical treatment of such azoospermia and asthenospermia.

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